Homo sapiens diseases - Quantitative alterations in white blood cells (WBCs)

HOMO SAPIENS DISEASES - QUANTITATIVE ALTERATIONS IN WHITE BLOOD CELLS (WBCs)

Table of contents :

lymphopenia

granulocytopenia

agranulocytosis

neutropenia

eosinopenia

basophilopenia

monocytopenia

granulocytosis

neutrophilia

eosinophilia

basophilia

mastocytosis

monocytosis / histiocytosis

lymphocytosis

plasmacytosis

lymphohistiocytosis

hypoplasias (leukopenia (< 4 ^.10³ / mL) : granulocytopenia (neutropenia + eosinopenia + basophilopenia) + lymphopenia)

hyponeocytosis : leukopenia with immature forms of leukocytes present in the blood
hypo-orthocytosis : leukopenia in which the proportion of the various forms of leukocytes is normal

lymphocytes (lymphopenia / lymphocytopenia (< 1.5 ^.10³ / mL in adults or < 3 ^.10³ / µL in children < 2 yr))

Aetiology

sarcoidosis
systemic lupus erythematosus (SLE)
autoimmune lymphopenia
immunodeficiencies
Salmonella typhi
influenzavirus
B lymphopenia
T lymphopenia : apoptosis of T lymphocytes in vitro, linked to transient T cell loss in vivo, is a consequence of certain viral infections, including lymphocytic choriomeningitis^ref and vaccinia^ref in mice and EBV^ref in humans. It has also been reported in association with HIV-1^{ref1,
ref2} in humans, although whether or not direct HIV infection is required for this effect, and its specificity for CD4⁺ T cells, are subjects of debate^ref

Aetiology

thoracoscopic talc poudrage ^ref.
CD4⁺ lymphopenia

Aetiology

neoplasia
HIV-1
type II BLS / class II MHC deficiency
idiopathic CD4⁺ lymphocytopenia (ICL) / severe unexplained HIV-seronegative immune suppression (SUHIS) : CD4⁺ count <300 cells/ml or a CD4⁺ count that is <20% of the total T cell count on 2 occasions, with no evidence of retroviral infections (HIV-1 or -2, HTLV-1 or -2) on testing, and absence of any defined immunodeficiency or therapy that depresses the levels of CD4⁺ T cells (unaccompanied by increased CD8⁺ T lymphocytes and hypergammaglobulinemia) either alone (ICL according to CDC, 1992^ref) or accompanied by clinical signs and symptoms of cellular immune deficiency (SUHIS according to WHO^ref). Cases have been identified since 1983^ref. It is likely that others could have been identified much earlier; however, the determination of CD4⁺ T-cell counts has been routine only since the early to mid-1980s and the beginning of the HIV epidemic. ICL differs from HIV infection by stable levels of CD4⁺ T cell counts in contrast to the progressive loss of this subpopulation observed in the course of HIV disease^{ref1,
ref2,
ref3}. Anyway recently a subset of ICL patients mimicking HIV disease has been reported: severe, prolonged decrement in peripheral CD4⁺ T cells with progressive decline in such counts documented in some; CD4/CD8 T cell ratios <= 1; and a history of opportunistic infections^{ref1,
ref2}. Moreover, a great heterogeneity in the symptomatology and the T cell phenotypic abnormalities have been reported among patients with ICL.

Epidemiology

^{ref1,
ref2,
ref3}

HIV-1

Aetiology

Although several genetic etiologies including MHC class II deficiency1 or mutations in RAG1,2 MST1,3 or LCK4although Laurence et al.^ref and Gupta et al.^ref suggested in 1992 that ICL could be due to a new retrovirus distinct from HIV-1 and HIV-2 (a human intracisternal A-type retrovirus, HIAP-II, was detected in a subset of patients with ICL : most of them were also ANA positive^ref), epidemiologic studies showed no evidence for a transmissible agent : all close contacts and sexual partners who were studied were clinically well, including 31 sexual partners^{ref1,
ref2,
ref3} in whom serologic, immunologic, and virologic studies for HIV were negative. Indeed, ICL can be diagnosed with the onset of opportunistic infections or among autoimmune disorders, whereas it remains asymptomatic in other patients^{ref1,
ref2,
ref3,
ref4}. In addition to the CD4⁺ lymphocytopenia, several patients also display a CD8⁺ lymphocytopenia while low B or NK cell counts have also been reported in others^{ref1,
ref2,
ref3}. The heterogeneity of ICL does not favor the hypothesis of a unique cause^ref (Moore, J. P. and Ho, D. D. 1992. HIV-negative AIDS. Lancet 340:475). CD4 cell counts of < 500 cells/ml were, however, associated with subsequent HIV seroconversion^ref. A subset of patients has anyway antibodies against retroviral proteins and nuclear antigens^ref . Low CD4⁺ counts are rare among anti-HIV-1-negative volunteer blood donors and are generally associated with transient illnesses. If any unknown virus progresses similarly to HIV-1, CD4⁺ count donor screening would be a poor surrogate for its detection^ref. There is also no epidemiologic evidence to suggest that a transmissible microbe is involved. The cases of idiopathic CD4⁺ T-lymphocytopenia were widely dispersed, with no clustering.
several genetic etiologies including :

MHC class II deficiency^ref
mutations in RAG1^ref, MST1^ref, LCK^ref, and ITK^ref

some authors have suggested ICL to be classified among common variable immunodeficiency ^ref. Similarly, a case of ICL associated with recurrent opportunistic infections could be attributed to a primary immunodeficiency disorder^ref
ICL was found in 16% of anti-SSA seropositive primary Sjogren's syndrome patients^ref. Anti-CD4 antibodies were observed more frequently in patients with Sjögren's syndrome (12.6%) as compared with the control groups (0.6%), and at a level similar to that seen among the HIV-1 patients (13.0%). However, no correlation was found between the presence of anti-CD4 antibodies and CD4+ T lymphocytopenia in the Sjögren patients^ref.
2 familial cases have been reported^{ref1,
ref2}
a recent study of "normal" persons reported a substantial proportion of subjects with CD4⁺ T lymphocytopenia, suggesting that this condition may occur as a result of the inherent variability in the measurement of T lymphocyte subsets^ref
it is hypothesised that CD4⁺ T lymphocytopenia represents the tail end of natural statistical variation in CD4⁺ cell counts^ref

Pathogenesis

increased spontaneous and activation-induced apoptosis

enhanced expression of Fas and FasL

^ref

Antihistone autoantibodies

^{ref1,
ref2}

^ref

⁺

in vitro

^{ref1,
ref2}

in vivo

^ref

proliferative T cell defects to mitogens or antigens

^{ref1,
ref2,
ref3,
ref4}

^ref

Abnormality of the PTK p56^Lck in CD8⁺ T cells

^Lck

⁺

^ref

⁺

^Lck

^{Fynref1,
ref2,
ref3,
ref4}

Symptoms & signs

dementia and encephalopathy^ref
viral infections :

3 cases of PML have been reported in ICL^{ref1, ref2,
ref3}
EBV and CMV coinfection of the central nervous system^ref
empyema thoracis and cytomegaloviral retinitis^ref
cutaneous infections by papillomavirus, relapsing generalized herpes zoster^ref and Candida albicans^ref
juvenile laryngeal papillomatosis (JLP)^ref

bacterial infections :

chronic mucocutaneous candidiasis (CMC), recurrent abscesses, and relapsing aphthous and ulcerous lesions. In addition to ICL the patient frequently showed a panlymphocytopenia. An increased percentage of gd⁺ T lymphocytes and IgD⁺ IgM⁺ B lymphocytes, and a decreased percentage of CD21⁺ B lymphocytes, were observed. In vitro assays showed normal T-cell responses to candidin and T-cell mitogens, but impaired B-cell responses to PWM. B-cell maturation after stimulation with Staphylococcus aureus Cowan I (SAC) and IL-2 was nearly normal^ref.
chronic severe mycobacterial disease^ref and disseminated infection with Mycobacterium avium^ref

fungal infections :

pleural effusion due to Histoplasma capsulatum^{ref1,
ref2}
cryptococcal infections :

pulmonary cryptococcosis and lung cancer^ref
cryptococcal meningitis^{ref1,
ref2,
ref3}

recurrent oral candidiasis who subsequently developed cryptococcal meningitis^ref

active intestinal tuberculosis with esophageal candidiasis^ref
episodic erythematous candidiasis, persistent angular cheilitis, lingua exfoliativa areata, and teleangiectasia of facial skin and buccal mucosa^ref
Pneumocystis carinii and Hemophillus influenzae pneumonia^ref

protozoal infections :

toxoplasmic myositis^ref

cancers : 6 cases with NHL, including 1 with primary leptomeningeal lymphoma^ref
epilepsy^ref
intracranial haemorrhage^ref

selective IgA deficiency

^ref

Therapy

IL-2

^{ref1,
ref2}

antimicrobials

^ref

Prognosis

CD8⁺ lymphopenia

Aetiology

type I BLS / class I MHC deficiency

^ref

⁺

^ref

⁺

^ref

⁺

^ref

⁺

^ref

^ref

⁺

^{ref1,
ref2,
ref3}

⁺

^ref

^{ref1,
ref2}

^ref

Transient changes may also be seen after severe physical or psychological stress. In one study of 15 healthy persons^ref [27], cognitive stressors caused elevations in heart rate and blood pressure, without affecting serum cortisol or catecholamine levels or absolute T-lymphocyte subsets (Table 1). Physical stress (ergometry), leading to elevation in heart rate, blood pressure, and serum adrenaline and noradrenaline, has been associated with a concomitant increase in the absolute number of CD8⁺ T cells relative to CD4⁺ T cells, resulting in a decrease in the CD4:CD8 ratio (Table 1). Splenectomy has also been linked to a stable increase in the percentage, but not the absolute count, of CD4⁺ cells; an increase in absolute CD8⁺ cells; and a decrease in the CD4:CD8 ratio Table 1^ref [28].

Other medical conditions accompanied by severe stress may have immediate effects on peripheral T-cell subsets without long-lasting sequelae. The most dramatic changes have been reported after acute myocardial infarction. In one study^ref [29], although absolute CD4 and CD8 counts did not differ statistically between infarct and control groups, a decrease in CD4:CD8 ratios was noted among infarct patients, with these low values typically persisting for 3 or more days after the event. The CD4:CD8 ratios among the 11 infarct patients (0.83 ± 0.43) differed from both control (2.12 ± 1.13, P = 0.001) and acute sepsis cases (1.76 ± 1.05, P = 0.004); however, no statistical difference was seen in ratios between the control and acute sepsis groups [29].
Ranges for T-Lymphocyte Subsets in "Normal Controls"

Table 2 shows studies of unselected, asymptomatic adults that provided means, standard deviations, and ranges or 95% CIs for absolute CD4 and CD8 counts. All but three included screening for HIV-1 infection by enzyme-linked immunosorbent assay (ELISA). The largest studies^{ref1,
ref2,
ref3} [14, 30, 31] specified that attention was paid to the time of day at which blood was drawn, with duplicate determinations and quality control measures in place; all participants were HIV seronegative. The smaller studies usually did not provide specific information about analytic or biologic variables for controls; these data are included for comparison with the more established normal ranges and as specific controls for the studies listed in Tables 3 and 4. (When HIV serologies were not done in these latter instances, a notation has been included in the appropriate table.) Companion data are given for HIV-seronegative pregnant women as well as for HIV-seronegative controls from the two major risk groups for HIV infection: homosexual men and intravenous drug abusers.

Miscellaneous conditions associated with changes in T-lymphocyte subsets :

The means for CD4⁺ and CD8⁺ T-cell counts presented in each of these reports are remarkably similar, despite differences in sex and the broad age groups included as adults. In one study^ref [14], a small number of these ostensibly healthy persons had stable but very low CD4 counts during a 5-year period, technically fulfilling the criteria for idiopathic CD4⁺ T lymphocytopenia. Clearly, other phenomena must be considered when evaluating CD4⁺ T-cell counts below the lowest limits of normal. The homeostatic control of peripheral T lymphocytes is susceptible to the various internal and environmental influences described above and conditioned by circulating hormones, cytokines, and other lymphocyte products^ref [46]. In addition, the total number of peripheral T cells appears to be independent of cellular input. In experimental systems, in the absence of either the CD4⁺ or CD8⁺ T-cell population, cell loss is routinely compensated for by the remaining subset^ref [46]. This phenomenon is also seen in patients with HIV, given that throughout much of the clinical course the total T-cell levels (CD3⁺) remain constant in the face of declining CD4 cells, secondary to CD8⁺ T lymphocytosis^ref [47]. Regulation of these T-cell populations is rapid and flexible, adapting to environmental changes through selection and amplification of appropriate T-lymphocyte clonal specificities. In adults, T cells are replaced primarily by cell proliferation at the periphery. Although > 30% of such cells are renewed every 3 days, total numbers are relatively fixed, with lymphocytes at varying stages of differentiation having different probabilities of survival, modulated by the environment^ref [46]. Evaluation of T-cell population kinetics, with documentation of stability in absolute values and attention to the subset ratio, is thus important in defining "normal" fluctuations in T-cell counts. Unlike HIV, which involves a progressive decline in CD4 counts that is typically accompanied by a depressed CD4:CD8 ratio, combined changes of "physiologic" CD4⁺ T lymphopenia (low CD4 percentage and absolute counts <400/ml), and an inverted ratio occurred in only 0.6% of 500 persons enrolled in one large study^ref [14], and even these markedly depressed values were stable during a 5-year period. This observation has been supported by other studies: only 1 of 275 healthy blood donors had a CD4 count < 300/ml (CD4:CD8 ratio not reported)^ref[48], and none of 2284 HIV-seronegative homosexual men had CD4 counts of less than 300/ml with multiple determinations during a 10-year period^ref [49]. It has been suggested that such persons with an absolute CD4 count physiologically "set" significantly below the means outlined in Table 2, if infected with HIV, might be expected to progress to a clinical definition of the AIDS at a more rapid rate than a patient whose baseline CD4 counts were significantly greater than the mean^ref [13]. Some anecdotal data support this contention^ref [50], but no evidence exists that these persons are otherwise compromised immunologically. Unless long-term stability of CD4 counts < 95% CI and CD4:CD8 ratios > 1.0 are documented, such persons with low CD4 cell counts warrant further evaluation. Indeed, before the identification of HIV-1 and HIV-2 as the primary etiologic agents of AIDS, the possibility of segregating healthy homosexual men from those at potential risk for disease, using a combination of depressed absolute CD4 counts and CD4:CD8 ratio, was suggested^ref [34]. One blood center even conducted a T-lymphocyte subset analysis as an interim screening procedure for a putative "AIDS agent"^ref [51]. Nearly 2% of 8715 consecutive volunteer blood donors between 17 and 77 years old had CD4:CD8 ratios < 0.85, and blood from these persons was not used for clinical purposes. Most had concomitant low CD4 values, and follow-up showed that some belonged to AIDS risk populations, despite denials at the time of donation^ref [51]. Other studies examining persons at high risk for HIV who were repeatedly seronegative for HIV by ELISA and immunoblotting but who had HIV-1 proviral DNA detectable by polymerase chain reaction^{ref1,
ref2} [35, 52], support the use of CD4 counts in conjunction with the CD4:CD8 ratio. Similarly, among male homosexual couples discordant for HIV-1 antibodies, those without evidence for HIV infection by polymerase chain reaction amplification of proviral DNA had stable CD4⁺ T-cell counts and CD4:CD8 ratios > 1, regardless of the absolute number of cells in these subsets^ref [53]. This finding further supports our recommendation that all persons with a CD4 count < 400/ml and a CD4:CD8 ratio < 1.0 should be investigated for HIV, as well as for other causes of immune deficiency, and that the definition of ICL/SUHIS be restricted to patients with < 300 to 400 CD4⁺ cells/ml, an inverted ratio, and evidence of a progressive decline in CD4⁺ cells. A similar approach, together with the aggressive tracing of donors and recipients, has been recommended within the transfusion community to investigate cases of idiopathic CD4⁺ T lymphocytopenia^ref [54] and is further discussed here.
T-lymphocyte subsets in infectious disease : as reported in Table 3, common pathogenic and opportunistic bacterial, viral, parasitic, and fungal diseases can cause transient alterations in T-lymphocyte subsets. These changes may be superimposed on various functional immune defects associated with such infections^ref [68] as well as on ill-defined syndromes of putative infectious etiology sometimes linked to decrements in CD4 counts, such as the chronic fatigue syndrome^ref [69]. Even immunizations may affect absolute numbers of T-cell subsets, transiently but significantly depressing CD4:CD8 ratios to < 1.0 in 25% of cases in one study^ref [70]. 2 risk factors for HIV, intravenous drug abuse (see Table 2) and clotting disorders (see Table 4), are not necessarily associated with significant alterations in absolute peripheral CD4+ or CD8⁺ T-cell counts, despite the fact that chronic antigenic exposure might have been expected to render these patients particularly susceptible to lymphocyte subset alterations. Infections linked to at least transient depression in CD4 counts (including tuberculosis, hepatitis B, and EBV-associated mononucleosis) are usually associated with a CD4:CD8 ratio > 1.0, even if it is statistically lower than control ratios. This finding also appears to be typical of other opportunistic infections seen in patients with HIV, including toxoplasmosis and P. carinii pneumonia (see Table 3). For oral candidiasis^{ref1,
ref2} [64, 65] and cryptococcosis^{ref1,
ref2} [66, 67], the numbers of HIV-seronegative patients studied are still too small to permit definitive conclusions. The major exception to the generalization that infectious disorders do not cause a low CD4 count in conjunction with a CD4:CD8 ratio of less than 1.0 is acute cytomegalovirus infection, in which depression of CD4 counts is typically accompanied by a marked increase in CD8 values (see Table 3). Both usually return to baseline after resolution of cytomegalovirus disease, with no statistical difference in absolute CD4+ or CD8+ T-cell counts in cytomegalovirus-seropositive compared with seronegative persons (see Table 2). Human T-cell lymphotropic virus type II (HTLV-II) occurs in a substantial portion of intravenous drug abusers and some homosexual men at risk for HIV and is capable of altering CD4 counts for prolonged periods. In HTLV-II-positive persons whose T cells do not exhibit spontaneous proliferation in vitro, T-cell subsets do not differ from those of normal controls^ref [61]. Among most HTLV-II- positive persons whose cells do exhibit such spontaneous growth, however, a significant increase in both CD4+ and CD8+ T-cell subsets, without alteration in CD4:CD8 ratio, has been reported (see Table 3). Lymphopenia, with artificial lowering of absolute counts, affects T-cell phenotype in the presence of certain infectious diseases or congenital disorders. Reference ranges for analysis of disease-related variations by T-cell subset percentages may be more appropriate in this setting^{ref1,
ref2} [17, 71], but these results do not alter our approach to assessing T-cell changes. Transient alterations in CD4 values in infectious diseases also occur in HIV-seropositive persons. These changes may have clinical relevance, although their pathophysiologic nature is incompletely understood. For example, primary cytomegalovirus infection in HIV⁺ persons may initiate a more rapid and substantial decline in CD4⁺ T-cell counts than in HIV⁺ controls not exposed to cytomegalovirus^ref [72]. The risk for advanced HIV disease in cytomegalovirus-seropositive persons was 2.5 times that of a similar cytomegalovirus-negative cohort^ref [72].
Congenital conditions that may be recognized late in life : common variable immunodeficiency may lead to altered CD4 counts recognized in later life. It is an important exclusion criterion for ICL/SUHIS^{ref1,
ref2} [4, 8]. Although progressive decreases in CD4⁺ T cells were not documented during a 2-year follow-up of HIV-seronegative and culture-negative patients with CVID^ref [73], including those with low baseline CD4 values^ref [39], initial absolute counts may be substantially less than the usual mean. Although CD4: CD8 ratios < 1.0 are unusual in common variable immunodeficiency^ref [73], they have been reported^{ref1,
ref2} [39, 74], unfortunately, in the absence of documentation of HIV serostatus. In these cases, CD4⁺ T-cell subset analysis may be illuminating because decrements in CD4 count appear to be secondary to a dramatic deficit in those cells that induce CD8⁺ suppressor cells, the CD4+ CD45RA⁺ population (126 ± 91 compared with 384 ± 142 in controls; P < 0.001), whereas the CD4⁺ CD29+ "memory" subset, which induces helper cells, remains unaffected^ref [39]. All of these analyses beg the issue of qualitative defects in CD4⁺ T-cell function occurring in the absence of quantitative changes. Such alterations are seen in the early stages of HIV infection^ref [75] and may underlie increased susceptibility to opportunistic infections occurring in the absence of changes in absolute CD4 count. They are beyond the scope of this review.
Importance of biologic variability in assessing CD4⁺ T lymphocytopenia and severe unexplained HIV-negative immunosuppression : because myriad factors can affect T-cell subsets, changes in CD4⁺ T-cell counts should be investigated over time, together with the CD4:CD8 ratio, particularly in the context of intercurrent disease. This is especially important in evaluating patients with ICL/SUHIS and should aid in refining its definition. For example, case 5 from 5 reports of idiopathic CD4⁺ T lymphocytopenia^ref [3] was a sexually active homosexual man, negative for HIV by serologic testing and DNA amplification by polymerase chain reaction, who had pulmonary tuberculosis, a persistent but stable CD4 count < 300/ml, and a CD4: CD8 ratio < 1.0. 6 months after successful therapy for his tuberculosis, his CD4 counts increased to > 600/ml, making the diagnosis of ICL/SUHIS untenable. Indeed, in all of the few patients with ICL/SUHIS investigated by reverse transcriptase measurements in viral cultures^{ref1,
ref2} [4, 6], no evidence for retroviral activity has been found. These patients have not shown progressive declines in their CD4 counts, however, and thus have been accurately described as not having an "HIV-like" immunologic picture. It has been estimated recently that > 300,000 persons in the USA alone would meet the current definition of idiopathic CD4⁺ T lymphocytopenia, with the possible involvement of a novel agent(s) lost within this mixture of uncertain lower truncation point for CD4 distribution and statistical variations^ref [76]. Thus, the failure to detect a lymphocytopathic or retrovirus or other micro-organisms should not discourage a thorough analysis of that subset of ICL/SUHIS patients with T-cell changes more characteristic of HIV. They should undergo extensive evaluation for HIV or other recognized or novel infectious causes of immune deficiency^{ref1,
ref2} [3, 77]. Such patients represent a very small fraction of the total cases reported to the Centers for Disease Control and Prevention and the World Health Organization^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6} [3-8]. I believe that it is these persons, however, for whom pneumocystis prophylaxis should be considered after CD4 counts decrease to < 200/ml, regardless of whether a retrovirus or other infectious agent has been identified. In the absence of clear epidemiologic support for a transmissible agent, however, any recommendation concerning ICL/SUHIS must be presented with great reserve. For example, a "novel retrovirus" was reported to have been isolated from two HIV-seronegative patients with CVID^ref [78] who, unlike the typical cases summarized here, had very low CD4 counts as well as depressed CD4:CD8 ratios. Follow-up showed that these patients were actively infected with HIV-1, even if incompetent to mount a serologic response to it^ref [73]. Finally, apart from T-cell subset analyses, AIDS in the "pre-AIDS era" had been described^ref [79] before recognition of ICL/SUHIS, but in only 1 of these 19 patients with opportunistic infections were CD4 counts measured. Indeed, my colleagues and I had previously documented P. carinii pneumonia in patients with normal CD4 counts and CD4:CD8 ratios^ref [63], and similar reports of AIDS-linked illnesses in patients with normal CD4 counts and T-cell subset ratios have been published^ref [80]. It is only through careful follow-up of patients screened in the manner suggested here, using historical knowledge of the effects of various infectious diseases and conditions on immunophenotyping, that complex issues such as physiologic CD4⁺ lymphopenia, ICL/SUHIS, requirements for institution of prophylactic antibiotics, and potential new infectious agents associated with alterations in T-cell subsets can be assessed.

granulocytes (granulocytopenia)

agranulocytosis / agranulocytic or neutropenic angina / malignant or pernicious leukopenia / Schultz's angina or syndrome / idiopathic or malignant neutropenia : any condition involving greatly decreased numbers of granulocytes

Aetiology

sensitization to drugs

type II hypersensitivity to sulfonamide

chemicals

vesnarinone is an important new drug that significantly decreases mortality rates in severe congestive heart failure; however, its use is associated with a relatively high incidence (approximately 1%) of agranulocytosis^ref

radiation affecting the bone marrow and depressing granulopoiesis

Symptoms & signs

neutropenia : absolute neutrophil count (ANC) < 2s below the age-related mean

peripheral neutropenia : decrease in the number of neutrophils in the circulating blood.

Grading

mild neutropenia : ANC = 1000-1500/mm³
moderate neutropenia : 500-1000/mm³
severe neutropenia : < 500/mm³

Epidemiology

Onset

congenital neutropenia (CN) / chronic hypoplastic neutropenia : former names for infantile genetic agranulocytosis. The 2 mains forms of hereditary neutropenia are cyclic neutropenia, also known as cyclic hematopoiesis, and severe congenital neutropenia (SCN), sometimes referred to as Kostmann syndrome. Other syndromes can feature neutropenia as a component :

syndrome	inheritance	gene	clinical features	animal model	animal model phenotype
cyclic neutropenia	autosomal dominant	ELA2	alternate 21 day cycling of neutrophils and monocytes	mouse knock-out	no neutropenia resistance to smoking-induced COPD vulnerability to infection
severe congenital neutropenia (SCN)	autosomal dominant	ELA2 (35–84%)	static neutropenia MDS and AML	mouse knock-in (V72M)	no obvious phenotype
	autosomal dominant	Gfi1 (rare)	static neutropenia circulating myeloid progenitors lymphopenia	mouse knock-out	resembles human Gfi1 deficiency
	sex-linked	wASP (rare)	neutropenic variant of Wiskott-Aldrich syndrome	mouse knock-out	lymphopenia thrombocytopenia colitis
	autosomal dominant	G-CSFR (rare)	G-CSF refractory neutropenia no documented MDS or AML	mouse knock-out	moderate neutropenia decreased progenitors in bone marrow increased apoptosis in circulating neutrophils
Kostmann syndrome	autosomal recessive	unknown	static neutropenia without MDS or AML
Hermansky-Pudlak syndrome , type 2	autosomal recessive	AP3B1	SCN platelet dense body defects oculocutaneous albinism	gray collie syndrome of dogs	14-day cycles of pancytopenia coat and eye color changes
Hermansky-Pudlak syndrome , type 2	autosomal recessive	AP3B1	SCN platelet dense body defects oculocutaneous albinism	mouse pearl mutation mouse knockout	no documented neutropenia platelet dense body defects coat and eye color changes
Chediak-Higashi syndrome	autosomal recessive	LYST	neutropenia oculocutaneous albinism giant lysosomes lymphohistiocytic infiltration impaired platelet function	blue-smoke Persian cat	neutropenia coat and eye color changes giant lysosomes lymphohistiocytic infiltration impaired platelet function
Chediak-Higashi syndrome	autosomal recessive	LYST		mouse beige mutation cattle Aleutian mink	no neutropenia coat and eye color changes giant lysosomes lymphohistiocytic infiltration impaired platelet function
Barth syndrome	sex-linked	TAZ	neutropenia, often cyclic dilated cardiomyopathy methylglutaconic-aciduria
Cohen syndrome	autosomal recessive	COH1	mental retardation neutropenia dysmorphism

Aetiology

cyclic or periodic neutropenia / cyclic hematopoiesis / gray collie syndrome

Aetiology

ELA2

^ref

Symptoms & signs

Laboratory examinations

^ref

chronic myelogenous leukemia (CML)

large granular lymphocytosis (LGL)

hypereosinophilic syndrome

Prognosis

^ref

Therapy

G-CSF

^ref

Kostmann congenital agranulocytosis neutropenia / infantile genetic agranulocytosis / severe congenital neutropenia (SCN)^ref

Epidemiology

Aetiology

autosomal dominant

heterozygous ELA2 mutations are present in DNA extracted from the peripheral blood of 35–84% of SCN cases^ref, leading to increased SHP-1 and SHP-2 in neutrophils. SCN is genetically heterogeneous, and most cases seem to arise sporadically, consistent with its transmission as an often lethal, autosomal dominant disorder. A rare case of sex-linked recessive inheritance has been described and constitutes an allelic variant of the Wiskott-Aldrich syndrome ^ref. Most cases are sporadic, but ELA2 mutations segregate with multigenerational transmission of the disease in several pedigrees where there are multiple affected family members, thus indicating that the mutations, at least in familial cases, occur constitutionally in the germline. The possibility of somatic ELA2 mutations, similar to the case for G-CSFR, remains unexplored. Mutations causing SCN are generally distinct from those responsible for cyclic neutropenia. The genotypes and phenotypes can overlap^{ref1,
ref2}, however, and the mutation P110L appears roughly equally among both cyclic neutropenia and SCN patient populations. Chain terminating nonsense and frameshift mutations near the carboxyl terminus are the most common SCN mutations. SCN patients whose disease is the result of ELA2 mutations represent a subset with worse disease: lower neutrophil counts, requirement for higher doses of G-CSF to achieve a response, and higher rate of neoplastic progression^ref. Some ELA2 mutations are particularly severe. G185R occurs in 4 SCN patients known in the French neutropenia registry^ref and each of whom has failed G-CSF treatment and has developed MDS or AML
homozygous mutation of ELA2 is unknown, and this gene would be an unlikely candidate for the recessive syndrome first reported by Kostmann, where the responsible gene remains unidentified.

Symptoms & signs

Acute myeloid leukemia

Laboratory examinations

static ANC < 500/mm³, monocytosis and eosinophilia => normal TLC
mild anemia may be present from chronic inflammation
hypergammaglobulinemia
normal complementemia, no ANCA
cytomorphology : bone marrow aspiration or biopsy reveals an arrest of neutrophil precursor maturation at the promyelocyte or myelocyte level
immunophenotype : neutrophils are CD16 / FcgRII^low and CD64 / FcgRI^high
normal ROS generation and intracellular killing of bacteria
decreased intracellular calcium mobilization in response to fMLP or IL-8
cytogenetic analysis typically reveals a normal bone marrow karyotype

Differential diagnosis

Chediak-Higashi syndrome

Therapy

prophylactic antibiotics may be considered but are not usually required
steroids and testosterone is not effective.
drain abscess as needed.
splenectomy is not effective
G-CSF (at higher doses than those used to treat cyclic neutropenia^ref) remains a highly efficacious therapy to prevent serious infections^ref : 29% of patients who receive G-CSF for 10 years will either die from sepsis (8%) or develop MDS /AML (21%)^ref. Those who receive a daily G-CSF dose greater than 8 µg/kg yet show neutrophil counts that are below the mean for the entire group have a cumulative incidence of either fatal sepsis or myeloid leukemia of 55%. Importantly, the myeloid malignancies that develop in patients with SCN show adverse biologic features such as chromosome 7 deletions. Mutations of G-CSFR , the gene encoding the G-CSF receptor, which almost exclusively occur in SCN, were initially reported as causative of some SCN cases^{ref1,
ref2}. Later, it was appreciated that G-CSFR mutations represent acquired, nonheritable, somatic events in the bone marrow, accumulating as SCN progresses to MDS and AML, although the mutations do not invariantly occur in AML and may also appear in the absence of neoplasia^{ref1,
ref2} : Lyn and Hck as key negative regulators of granulopoiesis and raise the possibility that loss of Src-family kinase activation by the d715 truncation mutation in G-CSFR may contribute to its hyperproliferative phenotype^ref. This potentially lifesaving treatment should not be withheld from newly diagnosed patients due to the risk of leukemia later in life. Leukemia in SCN may also show acquired monosomy 7, trisomy 21, and ras mutations. Subsequently, there have been reports of 2 sporadic SCN patients, resistant to G-CSF therapy, with constitutional heterozygous G-CSFR mutations that do appear to represent new pathogenetic germline mutations. The possibility of somatic ELA2 mutations in MDS or AML arising in the absence of hereditary neutropenia has not been addressed.
allogeneic HSCT is the preferred treatment for patients with CN who have a matched sibling donor, are unresponsive to therapy with G-CSF or in those with leukemic transformation

Web resources

Severe Chronic Neutropenia International Registry (SCNIR)

Gänsslen familial neutropenia
Hitzig chronic benign familial neutropenia : a rare familial type of peripheral neutropenia, probably transmitted as an autosomal dominant trait, related to but less severe than agranulocytosis. It is usually seen in children and is characterized by recurrent infections with eventual spontaneous remission, but in a few cases it has persisted into adulthood
reticular dysgenesia
Shwachman-Diamond syndrome (SDS)
Whim syndrome : myelokathexis (the occurrence of neutropenia and retention of bone marrow neutrophils has been called myelokathexis (kathexis = retention)), combination of chronic papillomavirus and bacterial sinopulmonary infections, low immunoglobulin levels.

Pathogenesis

^ref

₁

^ref

Chediak-Higashi syndrome

^ref

gray collie syndrome

Hermansky-Pudkak syndrome

^ref

in vitro

^ref

^ref

nonimmune chronic idiopathic neutropenia of adults (NI-CINA)

^ref

trans

^ref

Chediak-Higashi syndrome

^ref

Laboratory examinations

Therapy

G-CSF

acquired neutropenia : is a relatively rare disorder

immune neutropenia

Aetiology

alloimmune or isoimmune neonatal neutropenia (AINN) : neutropenia in the newborn due to in utero incompatibility between its paternal neutrophil antigens and those of the mother's blood; the mother's blood produces IgG antineutrophil antibodies that cross the placenta and sensitize fetal neutrophils. Affected infants may have fever, pneumonia, septicemia, and other infections that can be fatal. The condition eventually resolves itself as the infant's immunoglobulin replaces that from the mother. Newborns develop transient neutropenia that recovers spontaneously after an average of 11 weeks. In general, infectious complications are minor, and most series report no septic deaths^ref. When necessary, patients respond well to G-CSF ^ref. The majority of patients with AINN develop neutropenia in response to antibodies directed against antigens of HNA-1. The HNA antigens are located FcgIIIb (CD16). Pan-FcgRIIIb antibodies can arise in individuals who lack the receptor altogether as the result of a gene deletion; this is a rare cause of AINN^ref. Although FcgRIII deficiency was first discovered in the evaluation of patients who had newborns with AINN, the incidence of the development of antineutrophil antibodies was actually quite low. For example, in a study of 21 patients with FcgRIIIb deficiency, among 3 patients with 10 at-risk pregnancies, there were no newborns with neutropenia^ref. Interestingly, the incidence of AINN appears to be lower than the incidence of detectable granulocyte-specific antibodies in the population. In one survey of over 1000 postpartum women, 1.1% demonstrated granulocyte-specific antibodies, but no newborns had neutropenia^ref. Whether the detected antibodies were false positives inherent in the test or whether relative clinical silence reflects the biology of antineutrophil antibodies is unknown
autoimmune neutropenia (AIN)

primary AIN is a rare disorder. It occurs predominantly in early childhood: one study of 143 patients with AIN demonstrated that of 101 patients with primary AIN, 76 patients were under age 3^ref. The average age of onset is 6–12 months, and patients develop a moderate to severe chronic neutropenia. Infections are usually mild to moderate, and serious infections are unusual. Spontaneous remission occurs in 95% of childhood AIN patients over the course of 2 years^ref, with one group suggesting that the level of detected antibody is predictive of both infectious complications and time to remission^ref. Treatment with prophylactic antibiotics ameliorates infectious complications. Although patients are almost uniformly responsive to G-CSF , chronic administration is usually unnecessary and should be reserved for recurrent or severe infections^ref. Tests for antineutrophil antibodies in AIN are nearly always detected by GIFT, but in about 3% of cases may be positive only by GAT. Antibodies are uniformly IgG, and are directed primarily against HNA1 and 2, with rarer cases associated with antibodies to CD11b (HNA-5a) or pan-FcgIIIb (CD16)^{ref1,
ref2}. This is in contrast to secondary AIN, where pan-FcgRIIIb antibodies are frequently detected. Primary AIN is rare in adults, where autoimmune neutropenia is more often secondary to underlying rheumatologic syndromes. In adults, infectious complications are also frequently absent or mild, although the disease is usually chronic and spontaneous recovery is unusual^ref. Again, since symptoms may be minimal, treatment should be based on the patient’s clinical course rather than on the absolute level of the neutrophil count
secondary AIN : secondary AIN in adults is usually associated with systemic autoimmune disease, predominantly rheumatoid arthritis (RA) and SLE^ref. Neutropenia in RA is usually attributable to :

Felty’s syndrome (FS) typically occurs in patients with longstanding RA associated with end-organ manifestations of RA, including pulmonary fibrosis, vasculitis, rheumatoid nodules, and splenomegaly. Patients may also have Sjögren’s syndrome. Patients may have considerable morbidity from bacterial infection and may in rare cases succumb to overwhelming sepsis^ref. Laboratory evaluation of patients with FS demonstrates high levels of rheumatoid factor, circulating immune complexes, and hypergammaglobulinemia. In addition, many patients may be antinuclear antibody (ANA)⁺. 90% of patients with FS are HLA-DR4⁺
T-LGL leukemia : interestingly, patients with LGL leukemia share this incidence of HLA-DR4. This and other pathophysiologic features of the disease have prompted some investigators to suggest that FS and LGL leukemia represent a spectrum of the same disease process^ref.
SLE -associated neutropenia : neutropenia occurs in approximately half of patients with SLE. It is rarely severe and serves more as a marker of disease activity than as a clinically important complication. Neutropenia has little impact on the course of the disease and does not appear to predispose to an increase in infectious complications. The incidence of infectious complications is more reflective of immunosuppressive therapy than the height of the neutrophil count^ref. Neutropenia in SLE has been attributed to neutrophil-specific antibodies, to increased apoptosis of neutrophils, and to decreased marrow neutrophil production. All of these effects appear to be antibody-mediated. Increased neutrophil-associated IgG has been detected in half of patients diagnosed with SLE, but not all patients are neutropenic^ref. This further supports the observation that interpretation of increased neutrophil-associated IgG is especially difficult in the presence of immune complex disease. Both immune complexes and neutrophil antigen-specific antibodies have been implicated in the pathogenesis of SLE-associated neutropenia, but the correlation between laboratory testing and clinical neutropenia is poor. Some investigators have hypothesized that antinuclear antibodies may crossreact with neutrophil surface antigens, either because of crossreactive epitopes or because the nuclear antigens themselves are expressed on the cell surface. Neutropenia in SLE has been hypothesized to be pathogenetically related to the presence of anti-SSA (Ro) and anti-SSB (La) antibodies. Anti-Ro antibodies have been shown to bind a crossreacting antigen on the neutrophil cell surface and to fix complement. In another study^ref, immunoscreening of a leukocyte expression library identified La as an antigen bound by antineutrophil-positive sera from patients with SLE; this too was demonstrated to increase neutrophil apoptosis, as well as decreasing phagocytosis and increasing IL-8 production^ref. Finally, some antibodies have been demonstrated to be reactive against early myeloid progenitors, leading to decreased neutrophil production^ref
secondary AIN in childhood is rare and may be associated with autoimmune lymphoproliferative syndrome (ALPS). This disorder is caused by heterozygous mutations in the fas gene, leading to abnormalities of lymphoid apoptosis. ALPS is associated with autoimmune cytopenias in association with adenopathy and splenomegaly. Patients have increased numbers of circulating double negative (CD4^–, CD8^–) T cells. ALPS is associated with a markedly increased incidence of non-Hodgkin’s lymphoma ^ref

Pathogenesis

^ref

^{ref1,
ref2,
ref3,
ref4}

^ref

antigens	previous nomenclature	glycoprotein	allele frequency (%)
HNA-1a allele	NA1	FcgIIIb (CD16)	58
HNA-1b allele	NA2	FcgIIIb (CD16)	58
HNA-1c allele	SH, NA3	FcgIIIb (CD16)	8-38
HNA-2a	NB1	CD177(gp50-64)	94
HNA-3a	5b	Gp70-95	97
HNA-4a	MART	CD11a	99
HNA-5a	OND	CD11b	96
SSB/La			may play a role in the secondary autoimmune neutropenia seen in patients with systemic lupus erythematosus (SLE)

Laboratory examinations

most widely performed

granulocyte agglutination test (GAT) : incubation of granulocytes with patient sera (as in indirect Coombs test) and microscopic evaluation of agglutination. Results with this assay are reported to have widely varied rates of sensitivity, depending on the procedures used.
granulocyte immunofluorescence test (GIFT) : detection of neutrophil-bound antibody (as in direct Coombs test) by binding of glutaraldehyde-fixed patient neutrophils to fluorescently labeled anti-human IgG. Glutaraldehyde fixation prevents spontaneous fluorescence of neutrophils, which can confound interpretation of the test. The assay can be performed directly on patient neutrophils, although this may be difficult if the patient is profoundly neutropenic. Direct assay for the presence of antibody bound to neutrophils, either on patient neutrophils or on heterologous neutrophils incubated with patient serum or plasma, is fraught with difficulty^ref. Because neutrophils have abundant Fc receptors, false positive results may complicate interpretation of any of these studies, especially in the presence of high levels of circulating antibodies (as in myeloma or HIV infection) or in the setting of immune complex disease. Furthermore, neutrophils are fragile, tend to aggregate spontaneously in vitro, and often lyse upon manipulation, complicating interpretation of direct assays further. The degree to which these difficulties are estimated to complicate the interpretation of the assays varies among investigators. However, it may explain the presence of detectable antibodies in certain nonneutropenic study populations as well as the lack of correlation between the level of detected antibody and the degree of neutropenia reported by most investigators.

granulocyte indirect immunofluorescence test (GIIFT) (as in indirect Coombs test) : detection of serum antibody by incubation with glutaraldehyde-fixed heterologous normal neutrophils with patient serum with subsequent staining with fluorescently labeled anti-human IgG. This can be further adapted by using typed neutrophils homozygous for known neutrophil antigens, allowing identification of the target antigen of the patient’s antibody. Fluorescence can be detected by inspection under a microscope or by flow cytometry
enzyme linked immunoassays (ELISA) : detection of antibody in serum by binding to glutaraldehyde-fixed normal neutrophils on microtiter plates with detection by conjugated anti-human IgG
monoclonal antibody-specific immobilization of granulocyte antigens (MAIGA) : simultaneous incubation of neutrophils with defined antigen specificity with patient serum and monoclonal antibodies directed against neutrophil-specific antigens. Antigens are then immobilized on column coated with anti-mouse ab, and assayed for presence of human antibody^ref. This allows for the direct and simultaneous determination of antibody specificity directed at a variety of antigens. Tests of neutrophil antibodies are less widely performed and are more difficult to interpret than comparable tests on erythrocytes.

primary splenic neutropenia / hypersplenic neutropenia : a syndrome characterized by splenomegaly , hypercellular bone marrow, profound leukopenia and neutropenia, and susceptibility to infection, occasionally with anemia and thrombocytopenia
drug-induced neutropenia is an idiosyncratic reaction that results in profound neutropenia or agranulocytosis^ref. Unlike the chronic immune neutropenias, which have a surprisingly low rate of morbidity and mortality, drug-induced neutropenia is associated with a high rate of infectious complications and has a mortality rate of approximately 10%^{ref1,
ref2}. The most common drugs associated with agranulocytosis are antithyroid medications and sulfonamides. The most common mechanisms are immunological (formation of antibodies destructive to neutrophils or of immune complexes that bind to neutrophils), followed by inhibition of granulopoiesis and direct damage to bone marrow or precursor cells of the granulocytic series.

antithyroid medications :

antibiotics :

anticonvulsants :

antiplatelet agents
antivirals :

zidovudine
acyclovir (at high doses)

antibacterials :

NSAIDs

sulphasalazine

antipsychotics

clozapine ^ref : the usual recommendation is to discontinue treatment with the drug when the peripheral neutrophil count drops < 1,500/ml. The therapeutic procedures described (symptomatic treatment of neutropenia by co-administration of lithium or G-CSF , management of the adjunctive medication) seem to be efficient strategies that allow continuation of clozapine treatment despite the occurrence of neutropenia^ref.

anticancer drugs
SSRI : fluoxetine ^ref
immunomodulators :

^ref

Graves’ disease

thyroid-stimulating hormones (TSH)

^ref

antineutrophil cytoplasm antibodies (ANCA)

^ref

Clozapine

^ref

^{ref1,
ref2}

nonimmune chronic idiopathic neutropenia (NI-CINA) : a subset of patients with chronic neutropenia has no evidence of immune-mediated disease. NI-CINA is an acquired syndrome associated with chronic neutropenia, normal marrow cytogenetics, and no evidence for underlying autoimmune disease, nutritional deficiency, or myelodysplasia^ref. The marrow findings are variable, ranging from a hypoplastic to a hyperplastic myeloid series. The clinical course is usually quite benign, and many of these patients are diagnosed by examination of routine laboratory tests in the absence of any history of infection or other symptoms^ref. The pathogenesis of NI-CINA is poorly understood. The pathophysiology of the disease has been hypothesized to reflect decreased neutrophil production, excessive neutrophil margination, and increased peripheral neutrophil destruction. There has been a suggestion that patients with this syndrome have an undiagnosed underlying inflammatory illness, with increased production of inflammatory cytokines. A recent study by Papadaki et al concentrated on those patients with myeloid hypoplasia on marrow examination. Investigation of marrow progenitors and colony forming unit–granulocyte macrophage (CFU-GM) production documented a selective decrease in CD34⁺/CD33^– myeloid progenitors, with evidence for increased fas-mediated apoptosis as the cause for the reduction in CFU-GM. In addition, they demonstrated that stromal cell layers produced increased amounts of TNF^{ref1,
ref2}. Finally, the same group has previously demonstrated that increased risk of developing NI-CINA may be related to HLA phenotype^ref. It should be noted that the TNF locus lies within the HLA cluster, and the apparent HLA predilection for the development of clonazapine-induced agranulocytosis actually was more tightly linked to TNF microsatellite polymorphisms^ref. Hence, it is tempting to speculate that perhaps a predisposition to NI-CINA is also linked to polymorphisms of the same locus. Finally, 2 patients with NI-CINA have been found to have heterozygous mutations in Gfi-1^ref.
anticancer drugs

Prophylaxis

oral antibiotic therapy :

levofloxacin 500 mg 1 cps/day 4-5 days before expected onset of severe neutropenia and until hematological recovery (ANC > 1,000); no prophylaxis in patients with quinolone allergy; it is an effective and well-tolerated way of preventing febrile episodes and other relevant infection-related outcomes in patients with cancer and profound and protracted neutropenia. The long-term effect of this intervention on microbial resistance in the community is not known^ref
cotrimoxazole 960 mg 2 times a day for 3 consecutive days a week until end of therapy

oral antifungal therapy : itraconazole (oral solution or caps) 200 mg 2 times a day (alternatively fluconazole 200 mg/day)
hygiene and prophylaxis of oral cavity :

nystatin (oral suspension) 2 tablespoons at meals (wash and swallow)
clorhexidine (wash without swallowing)

G-CSF (only for non-myeloid malignancies)

for weekly chemotherapy : 150 mg/m²/day for 4 days in the interval
for monthly chemotherapy : 150 mg/m²/day since day + 5 of end of therapy until nadir of ANC (generally 4-7 days)

copper deficiency (associated with macrocytic anemia, normal platelet count, and elevated serum ferritin and EPO levels)^ref
folic acid deficiency
vitamin B₁₂ deficiency
hairy cell leukemia
ethanol
aplastic anemia
MDS

Therapy

G-CSF

^{ref1,
ref2}

^ref

pseudo-neutropenia

myeloperoxidase deficiency that occurs when the automated instrument employs a peroxidase reaction for the identification of neutrophils, eosinophils, and monocytes
neutrophil or platelet clumping
platelet satellitism.

Symptoms & signs

Staphylococcus epidermidis

Escherichia coli

Pseudomonas spp.

Candida spp

Aspergillus spp.

Therapy

G-CSF
hematopoietic stem cell transplantation (HSCT)
fluoroquinolones are highly effective in preventing Gram-negative infections in neutropenic cancer patients, but offer inadequate coverage for Gram-positive infections. Considering the lack of cut-clear benefit on some parameters of morbidity and mortality, routine use of Gram-positive prophylaxis is not advisable. This strategy, however, should be particularly valuable in subgroups of patients at high risk of streptococcal infection (eg, those with severe and prolonged neutropenia or mucositis, and those receiving cytarabine). Problems of tolerability and the potential for the emergence of resistant microorganisms should be considered when prescribing prophylaxis with enhanced Gram-positive activity to neutropenic patients.

Prognosis

eosinopenia : abnormal deficiency of eosinophils in the blood

Aetiology

acute bacterial infection (Simon's septic factor : decrease of eosinophils and increase of neutrophils in the blood in pyogenic infections)
GR agonists
hairy cell leukemia

basophilopenia / basophilic leukopenia : abnormal reduction in the number of basophils in the blood

Aetiology

hypothyroidism
stress
a few other conditions

monocytopenia : abnormal reduction in the number of monocytes in the blood

Aetiology

hairy cell leukemia

hyperplasias (leukocytosis (> 10 ^.10³ / mL))

hyperleukocytosis :
absolute leukocytosis : increase in the total number of leukocytes in the blood
relative leukocytosis : increase in the proportion of just one type of leukocyte in the blood, without increase of the total number of leukocytes.
physiologic leukocytosis : that caused by nonpathologic factors such as strenuous exercise
pathologic leukocytosis : that occurring as the result of some morbid condition, such as infections , inflammation, fever , trauma or hemorrhage.

toxic leukocytosis : leukocytosis occurring in septicemia and other toxic conditions.
agonal or terminal leukocytosis : leukocytosis occurring just before death

granulocytes (granulocytosis)

neutrophilia / pure leukocytosis / neutrophilic leukocytosis

pseudoneutrophilia
masked neutrophilia

granulocytic leukemoid reactions : > 50,000 WBC/ml in peripheral blood, not related to bone marrow involvement; the LR during infancy has been defined as an ANC of >10 SD above the mean for gestational age or >30 x 10³/ml during the first week of life^{ref1,
ref2}. The differential count has a marked "left shift" evidenced by the presence of myelocytes, metamyelocytes (and rarely promyelocytes), and increased number of band forms in the peripheral blood. In the absence of lymphadenopathy, organomegaly, basophilia, or eosinophilia, a high LAP score initially favors diagnosis of a leukemoid reaction

Aetiology

drugs :

G-CSF
corticosteroids (betamethasone^ref)
lithium
ethylene glycole intoxication^ref

alcoholic hepatitis^{ref1,
ref2} : although a leukocytosis of 15,000-18,000 cells/ml is frequently seen in AH, LRs are rare in this context. AH-associated LRs are a sign of poor prognosis and have a high mortality^ref
infections :

bacterial infections :

Shigella dysenteriae ^{ref1,
ref2}
Clostridium difficile (poor prognosis^ref), also in HIV patients^ref
Mycobacterium tuberculosis : disseminated hepatosplenic mycobacterial infection^ref

protozoal infections :

systemic toxocariasis ^ref

mesenteric inflammatory pseudotumor ^ref
fulminant purpura^ref
retroperitoneal hemorrhage^ref
cancer : Asano S, Urabe A, Okabe T, Sato N, Kondo Y. Demonstration of granulopoietic factor(s) in the plasma of nude mice transplanted with a human lung cancer and in the tumor tissue. Blood 49: 845-852, 1977^ref

paraneoplastic incretion of G-CSF :

diffuse malignant mesothelioma of pleura^ref
undifferentiated sarcoma of the lung^ref
cervical carcinoma ^ref (response to chemotherapy and local radiotherapy^ref)
cutaneous angiosarcoma^ref

paraneoplastic incretion of GM-CSF :

case	age	gender	origin	WBC count (/µl)	eosinophil (%)	serum GM-CSF by ELISA (pg/ml)	other means of detection	outcome
1	65	M	lung SCC	90 500	31	3800 (pleural fluid)	biological activity of CFU-GM
2	68	M	lung adenocarcinoma	36 900	37	1000 (pleural fluid)	biological activity of CFU-GM
3	61	M	undifferentiated thyroid cancer	105 600	-	106.4	-	died 1 month after diagnosis
4	72	F	undifferentiated thyroid cancer	116 900	32	459	-	died 4 months after diagnosis
5	67	F	TCC of the renal pelvis	45 000	-	132	biological activity of CFU-GM	observed 7 months after curative resection
6	71	M	large cell carcinoma of the lung	48 300	38	112	IHC	died of progressive tumor growth within 2 months of admission

^ref

⁺

paraneoplastic IL-6 and TNF-a : bone marrow necrosis due to metastatic prostate cancer ^ref
unknown :

bladder carcinoma ^ref
hepatocellular carcinoma ^ref
transitional cell carcinoma^ref
undifferentiated ovarian carcinoma^ref
transitional cell carcinoma of the kidney^ref
lung carcinoma ^ref
laryngeal cancer ^ref
colorectal carcinoma (preceding diagnosis by 4 years^ref)
undifferentiated carcinoma of the nasopharynx^ref
dedifferentiated liposarcoma with an inflammatory malignant fibrous histiocytoma-like component^ref
epidermal squamous cell carcinoma ^ref

^ref

leukaemoid reaction in megaloblastic anemia during puerperium^ref
familial thrombocytosis^ref

^ref

corticosteroids

^ref

Down syndrome

^{ref1,
ref2}

bronchopulmonary dysplasia (BPD)

^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7,
ref8,
ref9}

^ref

^{ref1,
ref2}

^ref

Laboratory examinations

Differential diagnosis

eosinophilia / eosinophilic leukocytosis : the formation and accumulation of an abnormally large number of eosinophils in the blood (> 450 / mL; [eosinophil]_blood inversely relates with [cortisol ]_blood)

eosinophilic leukemoid reaction :

metastatic melanoma^ref

Aetiology

drugs :

type I hypersensitivities :

type III hypersensitivity :

serum sickness

autoimmune disease :

hypoadrenalism
infestations (expecially in patients with HIV-1 infection ) :

protozoa :

Isospora spp. (rarely)
Sarcocystis spp.(rarely)
Toxoplasma gondii (low and discontinous)

Aspergillus spp.
Coccidioides immitis
helminths (related to level of tissue spreading ; normal eosinophil concentration if the helminth persists in cysts or lumens)

Langerhans cell histiocytosis (LCH) / eosinophilic granuloma of bone
neoplasms :

Hodgkin's lymphoma (15%)
non-Hodgkin lymphomas (NHLs) (5%)

cholesterol embolization (e.g. renal atheroembolism )
radiation exposure
Job syndrome
chronic granulomatous disease (CGD)
eosinophilia-myalgia syndrome (EMS)
toxic oil syndrome (TOS)
hypereosinophilia : extreme eosinophilia

Symptoms & signs

Laboratory examinations :

₁₂

Therapy

GR agonists

basophilia / basophilism / basophilic leukocytosis : an abnormal increase of basophils in the blood (> 150 / mL)

Aetiology

mastocytosis
monocytosis / histiocytosis / mononuclear leukocytosis / mononucleosis (> 10³ / mL) : a condition marked by the abnormal appearance of histiocytes (macrophages) in the blood. Disorders arising from cells of histiocytic and dendritic derivation are the epitome of confusing medical terminology, incomplete disease definitions and partial biologic and immunologic understanding. They are among the most rare of disorders of the hematopoietic system and thus, among the most difficult to study. They comprise a spectrum from benign proliferations of unknown etiology to frankly malignant tumors. The scarcity of markers specific to histiocytes, the lack of consistent means for detection of monoclonality, and the clinocopathologic overlap with reactive and infectious proliferations further complicate understanding their pathogenesis. Formulating a classification that incorporates the heterogeneity of histiocytic disorders has been challenging. The classification adopted by the Histiocyte Society separates dendritic cell- and macrophage-related entities of varied biological behavior from those that are malignant^{ref1,
ref2}. A recent proposal expounded by the International Lymphoma Study Group classifies tumors of histiocyte and accessory dendritic cells into four groups based on their immunophenotype^ref:

histiocytic sarcoma
Langerhans cell tumor/sarcoma (LCH)
follicular dendritic cell tumor/sarcoma
interdigitating dendritic cell tumor/sarcoma

Aetiology

infective causes

recovery from neutropenia
autoimmune diseases :

chemical causes
malignant diseases :

leukemia
HD
NHL
carcinomas
malignant histiocytosis : a rare type of histiocytosis found accompanying malignancies such as acute myeloid leukemia ; it may be a malignant transformation of stem cells of the monocyte series. It usually affects children or young adults and has a poor prognosis. Histiocytes migrate into skin around vessels and adnexa. Now it seems clear that most cases of malignant histiocytosis represent anaplastic large cell lymphoma (ALCL) with Ki 1 expression, and they are not related to the monocyte/macrophage system. This conclusion is based on histopathologic and immunohistochemical findings, and more recently, on results from genotypic studies. Thus, malignant histiocytosis is a "vanishing disease"^ref.

Epidemiology

Symptoms & signs

Laboratory examinations

Prognosis

Therapy

after splenectomy
diabetes mellitus
burns
Wiskott-Aldrich syndrome
HIV-1
GR agonists
hereditary histiocytosis from lipid storage diseases (LSD)

Gaucher disease
sea-blue histiocyte disease or syndrome / sea-blue histiocytosis

Aetiology

primary : D409 apoE mutation
Niemann-Pick disease type B (NPB)

Symptoms & signs :

splenomegaly

Laboratory examinations

sea-blue histiocytes

unknown causes

type I histiocytosis / Langerhans cell histiocytosis (LCH) or granulomatosis / histiocytosis X (HX) / eosinophilic granuloma or granulomatosis of bone (EGB) (CD1a⁺)

Epidemiology

Aeiology

^ref

Pathogenesis

^ref

^ref

in vitro

^ref

⁺

^ref

⁺

^ref

LCH = malignancy? : a central controversy about LCH is whether this is a malignant or inflammatory disorder. Clonal expansion of LC, but not lesional T cells, was defined by the human androgen receptor (HUMARA) DNA assay as well as TcR analysis ^ref. These findings have led many aficionados of LCH to strongly state that it is a malignant proliferation. Clinical data that are considered supportive of this concept include the finding of familial cases and the higher than expected incidence of malignancies in LCH patients. Until recently there had been scant data on chromosome analysis. Now there are 2 papers in the literature showing molecular cytogenetic abnormalities in LCH by comparative genomic hybridization (CGH) and loss of heterozygosity (LOH) analysis^{ref1,
ref2}. The first study evaluated 7 bone lesions and found losses of DNA sequences on chromosomes 1p, 5, 6, 9, 16, and 22q^ref. There was gain of DNA copy number on 2q, 4q, and 12. The highest frequencies of LOH (3/7 cases) were found on chromosome 1p and chromosome 7 (4/7 cases). Allele loss occurred on chromosomes 9 (2 cases) and 22q (1 case). The authors noted that 1p35-p36.3 contains several putative tumor suppressor genes and 22q12 contains the NF2 gene. They hypothesized that gains of DNA at sites similar to those found in malignancies (4q and 12) could relate to presence of a proliferation sequence. The above CGH data seem supportive of the malignancy theory given that cells from bone lesions are clonal by the HUMARA assay. However, analysis of adult pulmonary LCH by HUMARA has determined that it is not a clonal proliferation. Dacic et al reported that by CGH/LOH analysis of pulmonary LCH there was allelic loss at 1 or more tumor suppressor gene loci in 80% of the nodules dissected from 14 patients using essentially the same polymorphic microsatellite markers as noted in the first CGH study^ref. Given similar CGH/LOH results from clonal versus nonclonal LCH, the controversy on the malignant nature of LCH seems far from settled.
LCH = inflammation? : for those who like the "inflammatory" disease label, the collection of morphologically normal LC along with other players in common inflammatory lesions (macrophages, lymphocytes, eosinophils) augur for a nonmalignant biology. Until recently there had been few data linking a specific viral infection to LCH. Glotzbecker et al found immunohistochemical evidence for HHV-6 in 71% of LCH biopsies^ref. However, there was no serologic evidence to show that a recent infection had occurred. Given the latent nature of herpes viruses and their propensity for reactivation, the link of HHV-6 and LCH is controversial. Another argument against a transformed LC phenotype is the fact that no one has been able to propagate these cells in vitro for more than a few days or successfully maintain LCH cells in immune-deficient mice. Furthermore, the generation of "clonal proliferations" does not always signal a malignancy. Clonal proliferation of T cells in the peripheral blood of normal individuals or those with cutaneous lymphomas have been termed "clonality of uncertain significance." The familial LCH cases are extraordinarily rare, and HLA data show that siblings of LCH patients who don’t have the disease share same HLA type^ref. A study of Scandinavian LCH patients revealed immunogenetic heterogeneity (as did the US study) with the HLA-DRB1*03 phenotype present in 38% of single-system LCH and only 3% of multisystem LCH^ref. It is well known that individuals with immune deficiencies have high rates of malignancies so it is difficult to use this data to argue that LCH is an a priori (pre)malignant condition. Strong TGFß receptor expression and heterogeneous staining for MDM2, p53, and p21 in LCH lesions are thought to be evidence of a normal cellular response, not of mutational damage^ref. Given the tumor suppressor actions of TGFß, p53, and p16 it seems unlikely that all of these would be functional in a truly malignant cell. High expression of Bcl-2 in LCH lesions has been reported by more than one group and is thought to enhance cell survival. A Danish group has evaluated the expression of p53, Fas and Fas-ligand in LCH and found strong expression of p53 and some cells co-expressing Fas/Fas-ligand creating an "autocrine apoptotic shortcut." This mechanism could possibly explain the spontaneous regression of some LCH lesions.

Symptoms & signs

unifocal LCH : occurring as a single osteolytic lesion, usually in a long or flat bone; it may be asymptomatic or may produce bone pain, tenderness, and swelling and, sometimes, pathologic fracture

floating tooth sign : on radiographic examination of the mandible, erosion of the bony alveoli around the teeth so that they seem to be floating in space; it occurs in some forms of histiocytosis X.

type II or multifocal LCH : erosive accumulations of proliferating Langerhans' cells, commonly within the medullary cavities of bones, but also affecting the skin, gingiva, lungs, and stomach. It most commonly affects children age 2-6 years and is accompanied by seborrheic eruptions,fever , frequent occurrences of otitis media , mastoiditis , and URT infection , often with sclerosing cholangitis, lymphadenitis and splenomegaly . When the triad of calvarial bone defects, exophthalmos , and diabetes insipidus is present (sometimes with accumulation of cholesterol), it is referred to as Hand-Schüller-Christian disease / chronic idiopathic xanthomatosis (Hand A. Jr. Polyuria and tuberculosis. Arch.Pediatri. 10:673-675 (1893); Schuller A. Uber eigenartige Schadel-defekte im Jugendalter. Fortschr.Rontgenstr. 23:12-18 (1915); Christian HA. Defects in membranous bone, exophthalmos and diabetes insipidus. Contribut.Med. Biol.Res., Hoeber Inc. 199 p.320)
acute disseminated LCH / Letterer-Siwe (L-S) disease (Letterer E. Aleukemische Retikulose (Ein beitraf zu den proliferativen Erkrankugen des Retikulo-endothelial Apparates). Zeitschr. Pathol. 30:377-394 (1924). Siwe SA. Die Reticulo-Endotheliosis. Ein neues Krankheitsbild unter den Heptosplenomegalien. Eur. J.Ped. 55:212-230 (1933))

Aetiology

Epidemiology

Symptoms & signs

seborrheic dermatitis

hepatosplenomegaly

Prognosis

reticuloendotheliosis / hemohistioblastic syndrome : hyperplasia of reticuloendothelial tissue.

Laboratory examinations

Custer cells

disseminated lipogranulomatosis

Laboratory examinations

in bone and chronic lymph node lesions, LCH cells have immature phenotype (CD1a⁺14⁺40⁺68⁺83^-86^-LAMP^-langerin⁺ IL-10⁺class II MHC intracellular) and function (poorly stimulate allogeneic T-cell proliferation in vitro, but treatment with CD40L induces the expression of membrane class II and CD86 and strongly increases LCH cell allostimulatory activity to a level similar to that of mature DCs)
in patients with self-healing and/or isolated cutaneous disease, LCH cells have more mature phenotype (CD14^-86⁺ IL-10^-)^ref
in florid (exudative and granulomatous) nonfibrotic lung LCH lesions, LC, particularly those in contact with lymphocytes, are S100⁺CD1a⁺4⁺11a⁺11c⁺16⁺25⁺54⁺, MHC Class II⁺. Lymphocytes around LC are CD3⁺25⁺45RO⁺HLA-DR⁺ with a "memory" phenotype^ref
eosinophilia
Touton giant cell : a large vacuolated cell with numerous nuclei surrounding a peripheral rim of foamy cytoplasm

jaw lesions can be divided into 2 types:

type I (alveolar type) : the bone was destroyed along the alveola. This type is seen more frequently in the disseminated cases than in the EGB, and the majority of the lesions in this type manifested as ulcerative lesions clinically
type II (jaw body type) : the mandibular body was destroyed in two ways which manifested as bony radiolucence with or without partitions. Most of the lesions had local swelling or massive manifestations clinically, and almost all lesions occurred in mandible, particularly in the cases of EGB.

Prognosis

congenital self-healing Langerhans cell histiocytosis or reticulohistiocytosis (CSHH / CSHRH / CSHLCH) / Hashimoto-Pritzker disease (CD1a/c⁺, CD1b^-, CD4^+/-, HLA-DR/DQ⁺, S-100⁺) : complete involution of the eruptions, leaving atrophic lesions in the sites corresponding to the initial findings^ref; consisting of precursor Langerhans cells ^ref; may contain a large number of mast cells, leading to confusion with mastocytosis expecially when accompanied by urticaria^ref
Lavin-Osband criteria : age of onset of the disease, number of involved organs, function of organs, characters of the traditional classification

Therapy

"low risk" sites: skin, bone, lymph nodes, and pituitary
"high risk" sites: lung, liver, bone marrow, and spleen.

smoking

central diabetes insipidus

parenchymal brain lesions

smoking cessation may be effective in some patients with lung disease, but they need to be monitored carefully since the insidious progression of cystic changes and fibrosis can rob the patient of vital lung function.
feroic surgery for jaw disease results in disfigurement and loss of teeth, whereas a 6-month course of vinblastine and prednisone can cure the disease and allow reformation of the bone with no loss of dentition.
painful and disturbing perineal ulcers of LCH in women are best treated with chemotherapy or thalidomide , not radiation.

^ref

etoposide

prednisone

acute promyelocytic leukemia (APL)

^ref

mercaptopurine

methotrexate

^ref

radiotherapy

central diabetes insipidus

IFN-a₂

^ref

Prognosis

^ref

Cladribine (2-CdA)

^ref

type II (non-Langerhans cell) histiocytosis

Erdheim-Chester disease (ECD) is a rare histiocytosis first described in 1930, histologically characterized by xanthogranulomatous infiltrates of foamy, lipid-laden histiocytes in all involved sites

Symptoms & signs

cystic medial necrosis / Edrheim's disease

^ref

Laboratory examinations

disseminated xanthoma / xanthoma disseminatum / xanthoma multiplex : a rare form of non-Langerhans histiocyte proliferation, described by Montgomery in 1938

Symptoms & signs

central diabetes insipidus

Therapy

^ref

Prognosis

sinus histiocytosis : a disorder of the lymph nodes in which the distended sinuses are completely, or nearly completely, filled by histiocytes, as a result of active multiplication of the littoral cells

sinus histiocytosis with massive lymphadenopathy (SHML) / Rosai-Dorfman-Destombes disease (RDD) is a rare disorder characterized by a nonmalignant proliferation of distinctive histiocytic/phagocytic cells within lymph node sinuses and lymphatics in extranodal sites. Much of what is known of SHML today was pioneered by 2 pathologists, Juan Rosai and Ronald Dorfman. They recognized SHML as a distinct clinicopathologic entity and established a registry to collect and catalogue cases of SHML worldwide such that this unusual disorder may be better studied^ref. This scholarly contribution is well recognized today by the popularity of the eponym Rosai-Dorfman disease (RDD), particularly to refer to the extranodal form of this disorder. Since its initial description in 1969, SHML remains a disorder defined primarily by its histopathologic features. Due to its rarity, neither community-based surveys nor systematic treatment studies have been undertaken. Although a few hundred publications related to SHML can be found in the literature, many are single case reports or descriptions of small series of patients, limiting comprehensive appraisal of the subject.

Epidemiology

^ref

Pathogenesis

^ref

In situ

HHV-6

^ref

follicular dendritic cells (FDC)

autoimmune lymphoproliferative syndrome (ALPS)

^ref

⁺

^{ref1,
ref2,
ref3}

Fas

familial hemophagocytic lymphohistiocytosis (FHL)

perforin

^ref

Symptoms & signs

^ref

lymph nodes (87%) : massive painless adenopathy: cervical most frequent (axillary, para-aortic, inguinal and mediastinal lymph nodes are also commonly affected), may be bilateral, occasionally accompanied by pain or tenderness and contain large numbers of histiocytes
extranodal disease (43%), in some without associated lymphadenopathy which may or may not develop later in the disease course^ref : sometimes with fever , anemia, neutrophilia, elevated ESR , and hypergammaglobulinemia.

skin and soft tissue (16%) : broad range of non-specific presentations: typically painless, maculopapular rash, yellow xanthomatous solitary or multiple, usually raised reddish or bluish lesions, scaly
subcutaneous nodules or soft tissue masses
nasal cavity/paranasal sinuses (16%) : mucosal thickening, nasal polyps (may be recurrent) or masses causing mild or complete nasal obstruction, epistaxis, displacement of septum, infiltrative mass extending into maxillary, ethmoid, or sphenoid sinuses
eye/orbit/ocular adnexa (11%) : eyelid or orbital mass with proptosis; may require enucleation
bone (11%) : bone pain with osteolytic lesions in any bone of the axial or appendicular skeleton; on radiography, may be purely lucent or mixed with sclerosis or exhibit irregular borders or a broad sclerotic rim
salivary gland (7%) : bilateral parotid enlargement or submandibular mass; may be associated with dry mouth
central nervous system (7%) : intracranial epidural or dural, single or multiple masses, spinal cord masses, associated lytic bone lesions in skull or spine, cranial or spinal nerve palsies, weakness, syncope, headache
oral cavity (4%) : infiltrative mass of soft or hard palate, diffuse mucosal thickening, papillomatosis, gingival swelling
kidney/genitourinary tract (3%) : unilateral or bilateral renal masses accompanied by obstruction: hydronephrosis, hydroureter, ureteral obstruction, glomerulonephritis, chronic pyelonephritis
testicular, scrotal or epididymal masses with intermittent penile or pubic edema
respiratory tract/larynx/lungs (3%) : laryngeal obstruction, thickening and fibrosis associated with hoarseness
liver (1%) : enlargement with congestion, milliary infiltrates, masses
tonsil (1%) : enlargement, may be accompanied by tonsillitis
breast (< 1%) : predominantly subcutaneous involvement, rarely involves breast parenchyma, associated axillary adenopathy
gastrointestinal tract (< 1%) : hyperplastic mucosal folds, single or multiple exophytic masses
heart (< 1%) : subendocardial or valvular infiltrates causing arrythmias

Langerhans cell histiocytosis

sarcoid

Erdheim-Chester disease

foreign-body giant cell reaction

aspiration pneumonia

giant cell myocarditis

granulomatous myocarditis

Laboratory examinations

clinical laboratory findings include hematologic abnormalities such as normocytic or microcytic anemia. Immunologic abnormalities are found in a significant number of patients and often lead to a clinically unfavorable disease course. Up to 90% of patients demonstrate an elevated erythrocyte sedimentation rate. The most frequent immune dysfunction is autoimmune hemolytic anemia , which leads to severe hemolysis or fatality in a subset of patients^{ref1,
ref2}. Polyarthralgia, rheumatoid arthritis , glomerulonephritis , atopic asthma and diabetes mellitus are also known to complicate SHML. Polyclonal hypergammaglobulinemia is found in 90% of patients. Rarely, patients exhibit rheumatoid factor , antinuclear antibodies , and a reversal of CD4/CD8 ratio among peripheral lymphocytes. A small subset of patients also has concurrent neoplasia including NHL , other histiocytic proliferations, multiple myeloma ,melanoma and carcinoma. Consistent serologic findings are lacking, although antibodies to pathogenic organisms including EBV and HHV-6 have been reported^{ref1,
ref2,
ref3}
surgically excised lymph nodes are yellow-white with frequent capsular and pericapsular fibrosis. Generally, normal lymph node architecture is preserved and effacement is only seen in patients with longstanding lymphadenopathy. Typically, the lymph node sinuses are expanded by a proliferation of distinctive histiocytes exhibiting enlarged round or oval vesicular nuclei with well-defined, delicate nuclear membranes and a single prominent nucleolus. Multilobulated nuclei, nuclei with multiple nucleoli and nuclear atypia are rare. Mitoses are infrequent, although increased mitotic activity can be apparent occasionally. The histiocytes possess abundant pale eosinophilic cytoplasm; however, on occasion numerous histiocytes with foamy cytoplasm may predominate the cellular milieu. The hallmark of the SHML histiocyte is the presence within the cytoplasm of variable numbers of intact lymphocytes, a phenomenon referred to as lymphophagocytosis or emperipolesis, defined as lymphocytic penetration of and movement within another cell, in this case, the histiocyte^ref. These lymphocytes are often housed within vacuoles and escape degradation during their transit through the histiocyte. Plasma cells, neutrophils and red blood cells may also occupy this unique intracytoplasmic niche. Associated with the histiocytic proliferation are numerous, morphologically typical plasma cells often aggregated around post-capillary venules. Eosinophils are not a salient feature of SHML as compared with LCH, classical Hodgkin or T-cell lymphoma. Collections of neutrophils, eosinophilic microabscesses and reactive germinal centers are occasionally seen but are not prominent findings in SHML. Rosai-Dorfman disease involving extranodal sites shows similar morphologic features to its nodal counterpart although more fibrosis and fewer histiocytes with emperipolesis are encountered.
the histologic differential diagnosis includes LCH, histiocytic sarcoma, storage disorders such as Gaucher’s disease , classical Hodgkin lymphoma , metastatic melanoma and carcinoma, and infections caused by Histoplasma and mycobacterial organisms involving the lymph node. In the nasal cavity, rhinoscleroma may morphologically resemble RDD but is distinguished by the identification of Klebsiella rhinoscleroma. Perhaps the most frequently faced histologic challenge is that of distinguishing SHML from reactive sinus histiocytic proliferations which occur as nonspecific responses to a variety of instigating agents. Emperipolesis is rare or absent in reactive histiocytic proliferations. Although erythrophagocytosis is seen in reactive and neoplastic histiocytic proliferations, including LCH, emperipolesis in a setting outside of SHML is extremely rare. The appearance of lymph node sinuses expanded by a histiocytic proliferation is a feature common to LCH and SHML. However, unlike SHML, Langerhans cells have smaller, frequently folded or grooved nuclei and are associated with eosinophilic microabscesses.
immunohistologic studies : the most useful immunohistologic marker for SHML histiocytes is the expression of the S100 protein^{ref1,
ref2}. In addition, SHML histiocytes express pan-macrophage antigens (CD68, HAM 56, CD14, CD64, CD15), antigens associated with phagocytosis (CD64 or Fc receptor for IgG), lysosomal activity (lysozyme, a₁-antitrypsin) and immune activation (transferring receptor, IL-2R). We have recently found that SHML histiocytes express CD163, a hemoglobin scavenger receptor and acute phase-regulated transmembrane protein found on tissue macrophages and monocytes^ref. These studies support the hypothesis that the effector cell in SHML is a functionally activated macrophage and is distinct from Langerhans cells, FDCs and interdigitating dendritic cells. While Langerhans cells stain for the S100 protein and CD1a, only rare CD1a⁺ cells are found in SHML. In addition, SHML histiocytes do not express CD21, CD23, or CD35 (markers of dendritic differentiation). The overlap in morphologic and immunophenotypic features among reactive and neoplastic histiocytic proliferations, especially in unusual nodal presentations or extranodal sites, can make the diagnosis of SHML particularly problematic.

Therapy

Partial removal of tumor masses

^ref

^ref

Prognosis

^ref

reticulohistiocytoma : a granulomatous proliferation of lipid-laden histiocytes and multinucleated giant cells with pale eosinophilic cytoplasm having a ground-glass appearance. It occurs in 2 clinically different but histologically indistinguishable forms

reticulohistiocytic granuloma / reticulohistiocytoma sensu strictu : a solitary reticulohistiocytoma, seen mainly in men, which is not associated with systemic involvement, as in multicentric reticulohistiocytosis
multicentric reticulohistiocytosis / lipid or lipoid dermatoarthritis : a rare systemic disease seen mainly in women, characterized by the formation of multiple reticulohistiocytomas, polyarthritis of the hands and large joints with non pruriginous and hyperchromic papulonodular rash in the skin, bone, and mucous and synovial membranes and sometimes soft cystic ganglialike swellings over the extensor and flexor surfaces of the wrists; there may be evidence of internal malignancy. It may become quiescent, leaving only crippling arthropathy and disfigured skin, or it may progress to multiple organ involvement and eventual death

Therapy

GR agonists

chloroquine

^ref

Pathogenesis

^ref

Web resources

Histiocytosis Association of America

lymphocytosis

polyclonal lymphocytosis

polyclonal B-cell lymphocytosis (PPBL) : 84 cases have been published since 1983 to 2000. This rare hematological disorder of unknown etiology is characterized by morphologically atypical lymphocytes, polyclonal IgM production in association with smoking, female gender, and HLA-DR7 phenotype. In contrast to normal B-cells, PPBL cells showed no response to IL-4 with regard to CD23 and HLA-DR expression. F2mu antibodies failed to co-stimulate IL-4-mediated CD23 expression. Crosslinking membrane IgM receptors by F2mu resulted in elevated HLA-DR expression but did not induce in vitro proliferation of PPBL cells. This indicates a different activation and differentiation status than normal B-cells^ref

Differential diagnosis

B-cell chronic lymphocytic leukaemia (CLL)

atypical lymphocytosis
acute infectious lymphocytosis : an acute, benign infectious disease of children characterized by an excess of normal small lymphocytes in the blood without lymphadenopathy or splenomegaly, and with varying degrees of clinical expression and constitutional response.

absolute large granular lymphocytosis (ALGL)
plasmacytosis

plasma cell leukemia
reactive plasmacytosis :

viral infections :

staphylococcal sepsis ^ref
inflammation ^ref
medication
serum sickness syndrome ^ref
acalculous cholecystitis ^ref
reactive plasmacytosis of the thyroid gland in a patient with disseminated tuberculosis ^ref
primary Sjogren's syndrome (skin^ref, lung^ref and bone marrow^{ref1,
ref2})
drug hypersensitivity

mucous membrane plasmacytosis is a rare, idiopathic condition consisting of a dense plasma-cell infiltrate of the mucous membranes. The phenomenon of plasma-cell infiltrate was first described by Zoon^ref in 1952 when he described balanitis plasma cellularis . Since then, plasma-cell infiltrates have been found on the vulva, buccal mucosa, palate, nasal aperture, gingiva, lips, tongue, epiglottis, larynx, and other orificial surfaces. These conditions have been described with a variety of different terms. During the late 1960s and early 1970s, cases of plasma-cell infiltrates of the lips, gums, and tongue were described primarily in the dental literature under the names atypical gingivostomatitis^{ref1,
ref2}, idiopathic gingivostomatitis^ref, and allergic gingivostomatitis^ref. The lesions were thought to be a result of a reaction to chewing gum, dentifrices, and other foreign substances^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7,
ref8}, although extensive allergy testing has been inconclusive^{ref1,
ref2}. Sherman (Schuermann H. Plasmacytosis circumorificialis. Dtsch Zahnarztl 1960; 15: 601-610) and Luders (Luders G. Plasmocytosis mucosae: Ein oft verkanntes neues Krankheitsbild. Munch ed Wochenschr 1972; 114: 8-12) simplified the nomenclature in 1960 and 1973, respectively, by grouping the infiltrates by anatomy under the titles plasmacytosis circumorificialis and plasmacytosis mucosae. However, additional terms have been used in the literature to describe plasma-cell infiltrates of the aerodigestive tract, such as plasma cell gingivitis ^{ref1,
ref2,
ref3,
ref4}, plasmacytosis of the gingival^ref, and plasma-cell cheilitis^{ref1,
ref2}. In 1986, White et al.^ref grouped all plasma-cell infiltrates of the aerodigestive tract under the name plasma-cell orificial mucositis because of the fact that all the cases reported had clinical and histologic findings that were indistinguishable from one another, eliminating the need for separate names for each anatomic area. Since that time, plasma-cell orificial mucositis, or variants of the name such as mucous membrane plasmacytosis and plasma-cell mucositis, have been used to describe benign plasmacytic lesions of the aerodigestive tract in the majority of cases reported^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6}. Clinically, the lesions of mucous membrane plasmacytosis may present with a variety of symptoms and morphologies depending on the area of the aerodigestive tract in which it occurs. When appearing on the lips and gums, patients complain of sore, swollen lips and gums. Examination reveals a well-circumscribed, soft, slightly elevated, edematous mass in which the surface is red and glistening but not ulcerated. When occurring in other parts of the aerodigestive tract, such as the larynx, pharynx, palate, buccal mucosa, trachea, and distal airways^ref, patients complain of oral pain, dysphonia, dysphasia and difficulty breathing. On examination the lesions typically appear cobblestone- or wart-like^ref. Several cases have been reported in which patients demonstrate simultaneous plasma-cell infiltrate lesions of the gingiva and the pharynx or larynx^{ref1,
ref2,
ref3,
ref4}. Histologically, the majority of lesions are described as having an acanthotic epidermis with narrow and elongated rete ridges, spongiosis and a dense subepithelial cellular infiltrate composed largely of mature plasma cells, but also including a few polymorphonuclear leukocytes and lymphocytes. Occasional Russell bodies (accumulation of immunoglobulin within cytoplasm of plasma cells) were occasionally noted^ref. The plasma cells do not show anaplasia or prominent nucleoli. In addition, there are reports of plasma-cell orificial mucositis that show epidermal atrophy (Luders G. Plasmocytosis mucosae: Ein oft verkanntes neues Krankheitsbild. Munch ed Wochenschr 1972; 114: 8-12) and eroded epidermis^{ref1,ref2,
ref3}. Immunoperoxidase staining show mixed population of k and l light chains and various heavy chains, demonstrating the polytypic and benign nature of the condition.

Differential diagnosis

fungal infection can mimic mucous membrane plasmacytosis but is usually distinguished by absence of fungal hyphae on microscopic examination, negative KOH preparation, no growth on culture, or a lack of response to treatment with nystatin. Histologic examination of the tissue can exclude carcinoma from the differential diagnosis.
mucous membrane lesions are present in one-third of patients with secondary syphilis, and histology can show superficial and deep perivascular infiltrate of plasma cells, lymphocytes and macrophages distributed in a bandlike pattern in the dermis, accompanied by psoriasiform epidermal hyperplasia and hyperkeratosis (Odom, RB, James, WD, Berger, TG. Andrew's Diseases of the Skin Clinical Dermatology, 9th Edition. Philadelphia: W.B. Saunders Co., 2000). However, negative serologic tests for syphilis and absence of spirochetes on a silver stain of tissue sections can rule out secondary syphilis as the cause for the mucous membrane lesions.
when lichen planus occurs on mucous membranes, these often painful lesions are usually white plaques, typically with a lacelike pattern. Other presentations of mucous membrane lichen planus include atrophy, erosions or ulcers, and bullae. Microscopically, lichen planus is characterized by a superficial, bandlike, lymphocytic infiltrate and occasionally hyperkeratosis, but no significant accumulation of plasma cells.
cicatricial pemphigoid (benign mucosal pemphigoid) can clinically resemble mucous membrane plasmacytosis. The oral mucosa of patients with cicatricial pemphigoid is almost always involved, including the nasal mucosa, nasopharynx, larynx, oropharynx, hypopharynx, and esophagus. Oral lesions are characterized by evanescent vesicles that quickly rupture and leave erosions and ulcers, as opposed to the raised and cobblestone-appearing lesions of mucous membrane plasmacytosis. Cicatricial pemphigoid typically affects middle-aged to elderly women whereas mucous membrane plasmacytosis tends to affect elderly men. Histologically, there is subepithelial disruption or ulceration but no psoriasiform changes or plasmacytosis as expected with mucous membrane plasmacytosis^ref (Odom, RB, James, WD, Berger, TG. Andrew's Diseases of the Skin Clinical Dermatology, 9th Edition. Philadelphia: W.B. Saunders Co., 2000)
allergic or irritant contact dermatitis can initially be ruled out by history and by distribution of the lesions. Dentures or foreign objects can be removed to rule out contact dermatitis and patch testing can be done to detect any other contact or allergic factors. Histologically, lesions of allergic contact dermatitis reveal spongiosis with infiltrate of monocytes and histiocytes in the dermis. Primary irritant dermatitis presents with superficial vesicles containing polymorphonuclear leukocytes.
chronic, granulomatous disease sarcoidosis can affect mucous membranes, including the palate, tongue, buccal mucosa or posterior pharynx. In the oral cavity, the lesions are papules that may coalesce to form a flat plaque (Odom, RB, James, WD, Berger, TG. Andrew's Diseases of the Skin Clinical Dermatology, 9th Edition. Philadelphia: W.B. Saunders Co., 2000). Microscopic examination reveals large, epithelioid histiocytes with a few giant cells and lymphocytes, and occasional asteroid bodies with no evidence of a plasma-cell infiltrate.
mucous membrane plasmacytosis can clinically resemble cheilitis granulomatosa ; however, histopathology shows evidence of a granulomatous infiltrate rather than a plasma-cell infiltrate.
plasma-cell granulomas tend to locate in the oral cavity, primarily on the periodontal tissue. These lesions are often single; whereas, the lesions of mucous membrane plasmacytosis tend to be multiple. On histologic evaluation, plasma cells are prominent but are intermixed with abundant other cellular elements and usually surrounded by connective-tissue septae, distinguishing it from mucous membrane plasmacytosis^ref
plasmoacanthoma is described as a discrete, verrucous tumor with hyperkeratosis, pronounced acanthosis of the epidermis and plasmacytic infiltrate in the dermis on histologic examination. Plasmoacanthoma is considered a separate disease entity from plasma-cell orificial mucositis; however, in 1995 van de Kerhof and van Baar^ref described the simultaneous occurrence of these conditions in a patient and suggested that both conditions are part of one single disease entity.
rhinoscleroma is a chronic, inflammatory, granulomatous disease of the upper aerodigestive tract, associated with Klebsiella rhinoscleromatis infection, which can have a clinical presentation similar to that of mucous membrane plasmacytosis. Rhinoscleroma affects both sexes equally, most commonly during the third and fourth decades in persons from Russia, Central Europe, Egypt, Pakistan, Africa, and South and Central America. Histology reveals a granulomatous tumor consisting primarily of plasma cells, an occasional Russell body, a few spindle cells and hypertrophic collagenous tissue. Warthin-Starry silver stain can allow for visualization of the bacilli of rhinoscleroma within the foamy macrophages (Mikulicz's cells). Culture and serologic tests can also be performed to rule out rhinoscleroma (Odom, RB, James, WD, Berger, TG. Andrew's Diseases of the Skin Clinical Dermatology, 9th Edition. Philadelphia: W.B. Saunders Co., 2000)
Rosai-Dorfman disease (sinus histiocytosis with massive lymphadenopathy) can involve the head and neck^ref. Most patients who present with skin lesions are 40 years old or older at presentation. The lesions can be isolated or disseminated yellow-brown papules or nodules or macular erythema. The histopathologic features of Rosai-Dorfman disease are a superficial and deep, perivascular infiltrate of lymphocytes and plasma cells, in addition to a diffuse dermal infiltrate of large, foamy histiocytes. Additionally, fibrosis and lymphophagocytosis are characteristically present, features not common in mucous membrane plasmacytosis. The elements of epithelial psoriasiform changes and dyskeratosis typical of mucous membrane plasmacytosis are not seen in Rosai-Dorfman disease (Odom, RB, James, WD, Berger, TG. Andrew's Diseases of the Skin Clinical Dermatology, 9th Edition. Philadelphia: W.B. Saunders Co., 2000)
Melkerson-Rosenthal syndrome consists of a triad of recurring facial paralysis or paresis; soft, nonpitting edema of the lips; and scrotal tongue. Usually starting in adolescence, the first symptoms can be the swelling of the skin and mucous membranes of the face and mouth. A tuberculoid type of granuloma with lymphedema and a banal perivascular infiltrate are seen on microscopic examination (Odom, RB, James, WD, Berger, TG. Andrew's Diseases of the Skin Clinical Dermatology, 9th Edition. Philadelphia: W.B. Saunders Co., 2000)
on the basis of histology, extramedullary or primary cutaneous plasmacytoma needs to be considered. This tumor is found in the upper respiratory tract in approximately 80% of cases, especially in the nasal cavity and sinuses, nasopharynx, and larynx and can be sessile, polypoid or pedunculated^ref. Histologically, plasmacytomas are composed of a diffuse infiltrate of plasma cells in the dermis and subcutaneous tissue. There is minimal to prominent nuclear atypical of the plasma cells and on immunohistochemistry they are monoclonal, distinguishing plasmacytoma from plasmacytosis. Gene-rearrangement studies can be done if immunohistochemistry is inconclusive.

Therapy

₂

corticosteroids have been used with the most frequency but with inconsistent results. A review of the literature by White et al.^refin 1986 revealed that topical and intralesionally administered steroids were of no benefit and other studies have reported some symptomatic improvement but no true regression of the disease^{ref1,
ref2,
ref3,
ref4,
ref5}. Additionally, the patient reported in this case report has not responded to topical or systemic corticosteroids. A few cases in which corticosteroids induced marked regression with residual scarring^{ref1,
ref2}, as well as total eradication of the disease have been reported^{ref1,
ref2,
ref3}
antibiotics have also been used to treat mucous membrane plasmacytosis. Treatment with oral nystatin was found to be ineffective in the patient described in this case report as well in another case report^ref. Ferrerio et al.^ref report on 2 patients treated with antibiotics (type unspecified) without effect. In one case, 2% fusidic acid was found to be an effective treatment^ref and ineffective in another^ref. Tamaki et al.^ref described two patients with plasma-cell cheilitis who responded to oral griseofulvin with complete remission of lesions.
Fogarty^ref reports on a case of gingival plasmacytosis that had progressed to involve the larynx and was treated with systemic chemotherapy (cyclophosphamide, vincristine, and prednisolone) with temporary improvement, but symptoms progressed after therapy was discontinued. Eventually, this patient was treated with low-dose radiation therapy, which subsequently caused symptomatic improvement, which was maintained at 12month followup.
several authors report on resorting to debulking procedures, either surgical excision, electrocoagulation, carbon dioxide laser, or cryotherapy, to reduce the mass effect of the mucous membrane plasmacytosis involving the pharynx and larynx^{ref1,
ref2,
ref3,
ref4,
ref5}. These procedures resulted in improvement of symptoms; however, the procedures are a temporary measure as the lesions and symptoms recurred. In fact, a few patients have required a tracheostomy, owing to the progression of the mucous membrane plasmacytosis lesions causing subglottic strictures^{ref1,
ref2}

Prognosis

^ref

^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6}

^{ref1,
ref2}

^ref

Castleman's disease (CD) / angiofollicular lymphoid hyperplasia / giant lymph node hyperplasia : a polyclonal, nonneoplastic condition resembling lymphoma but without recognizable malignant cells; there are isolated masses of lymphoid tissue and lymph node hyperplasia. Understanding CD and the literature about CD requires not only recognizing these very different types of CD but also recognizing that, because CD in many circumstances is a diagnosis made by exclusion, there can easily be overusage of this diagnosis by pathologists, and, at the same time the diagnosis can also be easily overlooked in certain circumstances. CD is a set of complex disorders that range from localized benign tumor masses to extremely aggressive disseminated proliferations. Although the major subtypes of CD do have some features in common, suggesting a possible relationship to one another, their differences are much greater and must be recognized both for clinical purposes and to best study their underlying biologic features.

Histology

hyaline vascular or hyalinovascular type (HV-CD) (more common) is a disorder of stromal cells, which presents as a solitary mass that is usually curable surgically. It can be complicated by the development of soft tissue sarcomas. It presents numerous small hyalinized and hypervascular GCs with hypervascular interfollicular stroma and sinus effacement. It was described in 1956 by Benjamin Castleman and colleagues as a localized mediastinal mass in otherwise usually asymptomatic patients^ref
plasma cell type (PC-CD) (less common) is a plasma cell disorder with elevated levels of IL-6 . It presents fewer but larger (hyperplastic) GCs with plasma cell aggregates in lymph node paracortex and partially spared sinuses. It is associated with more generalized lymphadenopathy and immunological abnormalities. This disease occurs more frequently in older individuals and is more common in men. It was described that was also localized but had very different clinical and histopathologic features^ref

Localizations

localised Castleman's disease (LCD) : single lymph node in mediastinum, pulmonary hilum, or extrathoracic localization

HV-LCD

Epidemiology

Aetiology

HHV-4 / EBV

HHV-8 / KSHV

IL-6

^{ref1,
ref2}

Pathogenesis

VEGF

^ref

⁺

^ref

FDC dysplasia

^{ref1,
ref2}

EGFR

^ref

Symptoms & signs

^{ref1,
ref2,
ref3}

^ref

Laboratory examinations

^{ref1,
ref2}

^ref

⁺

a/b

^ref

Therapy

^{ref1,
ref2,
ref3}

Radiation therapy

^ref

PC-LCD

Epidemiology

Pathogenesis

IL-6

^{ref1,
ref2}

^ref

VEGF

^ref

Symptoms & signs

aggregate of lymph nodes

^{ref1,
ref2,
ref3}

^ref

Laboratory examinations

usually polyclonal but sometimes monoclonal plasma cells

^ref

Prognosis

^ref

Therapy

^{ref1,
ref2}

steroids

radiation therapy

Epidemiology

Symptoms & signs

Therapy

multicentric Castleman's disease (MCD) / multicentric angiofollicular hyperplasia : isolated masses of lymphoid tissue and lymph node hyperplasia, usually in the abdominal or mediastinal area (mainly involves lymph nodes and spleen). They may develop autoimmune phenomena, cytopenias, skin rashes, and intercurrent infections. Patients with MCD frequently develop malignancies, most commonly KS and non-Hodgkin's lymphoma. Notably, MCD is characterized by vascular proliferation in the germinal centers which is reminiscent of KS. However, this virus is present in MCD in patients with AIDS whether accompanied by KS or not. It was first described in 1980's

Epidemiology

^ref

^{ref1,
ref2,
ref3}

plasmablastic type (PB-M-CD)

^{ref1,
ref2}

Aetiology

HIV

^ref

HHV-8 / KSHV

⁺

HHV-4 / EBV

⁺

^ref

Pathogenesis

PC-LCD

IL-6

VEGF

^{ref1,
ref2}

Symptoms & signs

PC-LCD

^{ref1,
ref2,
ref3,
ref4}

Laboratory examinations

^ref

Therapy

^ref

prednisone

^{ref1,
ref2}

anti-IL-6R antibody

^ref

Anti-IL-6 antibodies

rituximab

^ref

ganciclovir

^ref

plasmablastic MCD (PB-MCD)^ref

Aetiology

HHV-8 / KSHV

HIV

⁺

^ref

Pathogenesis

⁺

IL-6

^{ref1,
ref2}

mantle zone large immunoblastic B cells

^ref

naïve

⁺

^{ref1,
ref2}

⁺

monoclonal

microlymphomas

plasmablastic lymphomas

PEL

^ref

⁺

HHV-4 / EBV

^{ref1,
ref2}

^ref

IL-6R

^ref

⁺

IL-6

IL-10

^ref

⁺

^ref

Differential diagnosis

⁺

germinotropic lymphoproliferative disorder (GLD)

^+ref

Prognosis

^{ref1,
ref2}

^ref

idiopathic plasmacytic lymphadenopathy with polyclonal hypergammaglobulinemia

^–ref

Prognosis

^ref

Differential diagnosis

^ref

^+ref

^ref

Hodgkin lymphoma

^ref

during hypersensitivities
during autoimmunity
hairy cell leukemia

monoclonal lymphocytosis

lymphomas
monoclonal lymphocytosis of undetermined significance (MLUS)

benign monoclonal B-cell lymphocytosis (MBL) (BMBL) / B-cell monoclonal lymphocytosis of undetermined significance (B-MLUS) : very low levels of circulating monoclonal B-cell subpopulations can now be detected using flow cytometry, in apparently healthy individuals with a prolonged asymptomatic or benign clinical course, and essentially normal humoral and cellular immunity and normal karyotype. The majority of individuals with MBL will have cells that are indistinguishable from B-cell chronic lymphocytic leukaemia (CLL). However, this blood cell clonal expansion of CD5⁺ or CD5^- B-lymphocytes is age-dependent and immunophenotypic heterogeneity is common. Longitudinal studies are required to determine whether MBL is a precursor state to CLL or other B-lymphoproliferative disease in a situation analogous to a monoclonal gammopathy of undetermined significance and myeloma. Future studies of MBL should be directed towards determining its relationship to clinical disease, particularly in individuals from families with a genetic predisposition to developing CLL^{ref1,
ref2}

^{ref1,
ref2}

⁺

^ref

⁹

Diagnostic criteria

detection of a monoclonal B-cell population in the peripheral blood with

overall k:l ratio >3:1 or <0.3:1, or
> 25% of B cells lacking or expressing low level surface immunoglobulin or
a disease-specific immunophenotype.

repeat assessment should demonstrate that the monoclonal B-cell population is stable over a 3-month period.
exclusion criteria

lymphadenopathy and organomegaly, or
associated autoimmune/infectious disease, or
B-lymphocyte count >5 · 10⁹/l, or
any other feature diagnostic of a B-lymphoproliferative disorder. However, a paraprotein may be present or associated with MBL and should be evaluated independently.

subclassification:

CD5⁺23⁺: this is the major subcategory and corresponds to a CLL immunophenotype (Cheson et al, 1996).
CD5⁺23^-: correlate moderate level of CD20 and CD79b expression with atypical CLL.
CD5^-: corresponds to non-CLL lymphoproliferative disease (LPD).

Notes:

1 > 1 set of k/l light chain reagents may be used, the detection of any B-cell monoclonal population by light chain restriction is sufficient. Confirmation with IgH-PCR may be helpful but is not essential.
2 The monoclonal B-cell population may represent a minority of total B cells when identified by a disease-specific immunophenotype. These may be demonstrable even if the overall k:l ratio is normal, although clonality must be demonstrated within the cellular population identified by the disease-specific phenotype.
3 MBL lacking surface immunoglobulin is associated with CD5⁺CD23⁺ MBL.
4 A minimum of 3 colours (CD19 or CD20, anti-k and anti-l) should be used to confirm clonality, although four or more colours are preferable.
5 The fluorescence intensity of surface immunoglobulin, CD20 and CD79b expression if moderately increased should be noted.
6 The number of cells analysed should allow the formation of a cluster containing at least 50 events.
7 Repeat flow cytometric analysis is not necessary for research applications if monoclonality is confirmed by other approaches, e.g. fluorescence in situ hybridization or PCR, but may be useful for monitoring.
8 A disease-specific phenotype exists for hairy cell leukaemia (CD5^-CD103⁺CD11c⁺CD25^±) but it is probable that a full diagnosis of hairy cell leukaemia will be made in the presence of any level of circulating disease.
9 Other subclassifications may be included if sufficiently specific tests with evidence of a clinical association can be confirmed.

Natural history of the disorder

⁺

Populations to consider

^{ref1,
ref2}

^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7}

⁺

^ref

Recommendations for follow-up

⁺

^ref

Laboratory examinations

L chain restriction^ref
absolute lymphocyte count (ALC) in PB < 5 · 10⁹/l
immunophenotype : patients with a prominent lymphadenopathy and/or splenomegaly had CD22⁺ leukemic cells while in patients with a progressive lymphocytosis the B-cell clone expressed Leu-8. Thus, CD22 might be related to the homing capacity of B lymphocytes for lymphnodes and spleen, while Leu-8 might define a circulating B-cell subset. In B-MLUS about 50% of the monoclonal B cells co-expressed Leu8 which is consistent with a more differentiated phenotype compared to B-CLL with progressive lymphocytosis. The CD22 expression was mostly low in B-MLUS although a few patients showed high values. The expression of receptors for growth factors (CD23, CD25, CD71) was higher in B-CLL compared to B-MLUS patients (p < 0.001), which is consistent with a difference in lymphocyte activation stage and/or response to growth factors^ref

monoclonal T-cell dyscrasia of undetermined significance (MTUS)

Laboratory examinations

⁺

^-ref

chronic granular T cell lymphocytosis of undetermined significance

Laboratory examinations

⁺

^+ref

Therapy

GR agonists

lymphohistiocytosis : lymphocytosis + histiocytosis.

erythrophagocytic or hemophagocytic lymphohistiocytosis (HLH) / hemophagocytic or hemophagocytosis syndrome (HPS / HS) / hemophagocytic lymphohistiocytic syndrome (HLS)

Epidemiology :

Aetiology

genetic, hereditary, primary or familial HLH (a few cases) autosomal recessive inheritance. Both genetic subgroups are associated with impaired NK cell function

disease

chromosome location

associated gene

gene function

FHLH-1

9q21.3-22

Not known (10%) (linkage analysis in 4 HLH families of Pakistani origin^ref)

not known

FHLH-2

10q21-22

perforin (PRF1)

^ref (15-50% depending on the geographical and ethnic origin of the patients^ref) was the first gene associated with FHLH (1999) : 2 novel mutations in Oman^ref. Prenatal diagnosis^ref

mutation type^ref	protein- sequence alteration	nucleotide- sequence alteration	exon
nonsense:
	Trp374stop (Turkey)	1122 G=>A	3
	Tyr219stop (Turkey)	657 C=>A	3
missense:
	Ile224asp (Turkey)	671 T=>A	3
	Val50met (Turkey)	148 G=>A	2
deletion:
	Dlys285 (Turkey)	853-855 del AAG	3

induction of apoptosis

FHLH-3

17q25

UNC13D / Munc13-4 (30%^ref) was the second gene associated with FHLH

cytolytic granule exocytosis^ref. UNC13D mutations do not affect docking of secretory vesicles (also known as lytic granules or secretory lysosomes) at the plasma membrane, but they impair priming of these vesicles and the subsequent release of cytolytic enzymes; defective CD107a surface expression^ref

FHLH-4

6q24

syntaxin 11 (STX11)^ref

t-SNARE involved in intracellular trafficking, but its precise role is not known. The protein is strongly associated with intracellular membrane fractions and is detectable only in monocytes and not in lymphocytes. So far, mutations in the coding exon of syntaxin 11 seem to be restricted to patients from Turkey

GS-2

15q21

RAB27A^ref. XLP results from mutations in the SH2D1A gene^ref

vesicle transport; small GTPase. Activated T cells of Rab27-deficient patients are unable to dock their secretory granules at the plasma membrane, thereby impairing secretion via the immunological synapse^ref. A direct interaction between Munc13-4 and Rab27 has recently been demonstrated, and the complex seems to be an essential regulator of secretory granule fusion with the plasma membrane^ref

Chediak-Higashi syndrome (CHS)

1q42.1-q42.2

LYST, which encodes a 3801 amino acid protein

required, by an unknown mechanism, for the final steps of granule secretion^{ref1,
ref2}

X-linked lymphoproliferative syndrome (XLP)

Xq25

SH2D1A (SAP).

required for the signaling lymphocytic activating molecule (SLAM), which itself is important for signal transduction in immune cells and for activation of granule-mediated cytotoxicity of NK cells and CTLs^ref. Mutation screening in male patients with HLH may be useful as some of them harbor mutations in SH2D1A^ref

familial HLH (FHLH) / Farquhar disease / familial erythrophagocytic lymphohistiocytosis / familial erythrophagocytic, hemophagocytic or histiocytic medullary reticulosis / familial reticuloendotheliosis with eosinophilia / Omenn's syndrome

Epidemiology

^ref

Aetiology

unknown gene defects (FHL1)
known gene defects:

Symptoms & signs

immune deficiency syndromes with distinctive clinical features in which the development of HLH is sporadic, though frequent. HLH is often the presenting symptom but may also occur later during the course of disease

Chediak-Higashi syndrome (CHS) show albinism and frequent pyogenic infections. Their WBCs exhibit decreased chemotaxis and characteristic giant inclusion bodies (lysosomes)
Griscelli syndrome (GS) also have hypopigmentation and various degrees of neutrophil dysfunction but lack the giant granules

Griscelli syndrome type 2 (GS2) / partial albinism with immunodeficiency : mutation in RAB27A

X-linked lymphoproliferative syndrome (XLP) is mainly characterized by a predisposition for EBV-associated HLH

inborn errors of metabolism : it is not clear what role metabolic products may play as triggers to the immune response

Pathogenesis

hypersecretion of pro-inflammatory cytokines such as IFN-g, TNF-a, IL-6, IL-10 and M-CSF by activated T-lymphocytes and histiocytes that infiltrate all tissues, and lead to tissue necrosis and organ failure

⁺

^ref

severe impairment of the cytotoxic function of NK cells and CTLs

^ref

acquired, reactive, or secondary HLH :

malignancy-associated HS (MAHS)

acute lymphoblastic leukemia^ref
lymphoma -associated hemophagocytic syndrome (LAHS) is a well-known entity in adults but is rare in children. Cases formerly diagnosed as histiocytic medullary reticulosis or malignant histiocytosis included patients with LAHS, but also IAHS.

B-cell lymphoma : EBV genome was detected only rarely in patients with B-cell lymphoma

ileum-origin B-cell lymphoma^ref

T/NK cell lymphoma (48.5% in Japan^ref) mostly occurs in extra nodal, especially nasal, cutaneous, or malignant lymphoma involving liver and spleen : EBV genome demonstrated in > 80% of patients^ref. EBV-infected T/NK cells appear to play a major role in the development of LAHS as well as EBV-associated HLH without lymphoma^ref, and in both LAHS and EBV-HLH the infected T/NK cells show a monoclonal or oligoclonal proliferation

peripheral T cell lymphoma^{ref1,
ref2}
hepatosplenic gd- T-cell lymphoma with isochromosome 7q and trisomy 8^ref
gastric T-cell lymphoma^ref
CD30⁺ anaplastic large cell lymphoma ^ref

Laboratory examinations

1) high fever for > 1 week (peak 38.5°C)
2) anemia (Hb < 9 g/dl) or thrombocytopenia (platelet < 100,000 ?/l)
3)

a) LDH >= 2 × upper limit
b) hyperferritinemia >= 1,000 ng/dl)
c) hepatosplenomegaly on CT, US or MRI
d) FDP >= 10 mg/ml

4) hemophagocytosis in bone marrow, spleen or liver
5) no evidence of infection
6) histopathologically confirmed malignant lymphoma

^ref

Prognosis

^ref

autoimmune disease

macrophage activation syndrome (MAS)^{ref1,
ref2}occurs in children and adults with autoimmune diseases. It is most commonly seen in association with systemic-onset juvenile rheumatoid arthritis (sjRA)^ref (expecially after administration of etanercept ) or adult-onset Still's disease (AOSD), but also occurs rarely with systemic lupus erythematosus (SLE)^ref or other entities^{ref1,
ref2}. The clinical picture has all of the characteristic features of HLH including clinical symptoms, laboratory findings (especially very high ferritin levels^ref), and hemophagocytosis. Pronounced coagulopathy and severe cardiac impairment are common and potentially life-threatening^ref. Patients with MAS exhibit the defective NK cell function common to other patients with HLH. They may also have decreased expression of perforin or SAP, mimicking the defects associated with FHLH and XLP, respectively^{ref1,
ref2,ref3}. Furthermore, low NK cell function and perforin expression was found to distinguish patients with sJRA from those with other clinical forms of JRA^ref.

Epidemiology

Aetiology

methotrexate

gold-salt injections

Laboratory examinations

^ref

familial disease/known genetic defect
clinical and laboratory criteria (5/8 criteria)

fever
splenomegaly
cytopenia >= 2 cell lines

hemoglobin < 9 g/dL (below 4 weeks < 12 g/dL)
neutrophils < 1,000/mL

hypertriglyceridemia and/or hypofibrinogenemia

fasting triglycerides >= 3 mM
fibrinogen < 1.5 g/L

ferritin > 500 µg/L
sCD25 >= 2400 U/mL (Janka G, Henter JI, Imashuku S. Clinical aspects and therapy of hemophagocytic lymphohistiocytosis. In: Histiocytic Disorders of Children and Adults: Cambridge University Press; 2005:353–37)
decreased or absent NK-cell activity
hemophagocytosis in bone marrow, CSF or lymph nodes

Therapy :

^ref

Prognosis

exogenous agents (infectious organisms, toxins)

infection -associated hemophagocytic syndrome (IAHS) : whereas in the first report by Risdall et al the majority of cases had an acquired iatrogenic immune deficiency, most patients in subsequent reports had no known genetic or acquired immune defect. A review of the published cases in children diagnosed with IAHS before 1996 reported that > 50% of them were from the Far East. The identification of an infectious organism does not help to differentiate FHLH from acquired HLH since the former is also usually triggered by infectious agents. This cannot be emphasized enough, since appropriate therapy should not be withheld when an infectious agent has been found

Plasmodium vivax ^ref
Leishmania spp.^ref
Mycoplasma pneumoniae ^ref
adrenal gland Mycobacterium tuberculosis ^ref
virus-associated hemophagocytic syndrome (VAHS) : the patients in the original report by Risdall and colleagues were mostly adults with a viral infection following organ transplantation^ref

HHV-4 / EBV -associated hemophagocytic lymphohistiocytosis (EBV-HLH) (74%^ref) : although the majority of EBV-HLH cases develop in apparently immunocompetent children and adolescents, it also occurs in association with infectious mononucleosis, chronic active EBV infection, familial HLH, X-linked lymphoproliferative disease, lymphoproliferative disease like peripheral T-cell lymphoma and NK cell leukemia. The majority of successfully treated EBV-HLH patients have a good outcome and remain disease-free^ref., but EBV-HLH may run an acute, fulminant course
HHV-6 ^{ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7,
ref8,
ref9,
ref10}
smoldering adult T-cell leukemia/lymphoma from HTLV-1 ^ref
HSV
adenovirus
fulminant ulcerative colitis and HHV-5 / CMV infection^ref
acute HHV-5 / CMV and HBV sexual co-infection^ref

^ref

endogenous products (tissue damage, metabolic products)

Pathogenesis

^ref

Pathogenesis

^{ref1,
ref2,
ref3}

Symptoms & signs

fever

hepatosplenomegaly

cytopenias

Lymphadenopathy

Laboratory examinations

^ref

a chain of the soluble IL-2R (sCD25)

impaired NK cell activity

^ref

In acquired cases it usually reverts to normal, but some patients show prolonged impairment

^{ref1, ref2}

Diagnostic problems in HLH

^{ref1,
ref2,
ref3}

A high LDH may suggest a hemolytic anemia, but most patients with HLH characteristically have only moderately elevated reticulocytes in the presence of severe anemia, compatible with ineffective erythropoiesis

Highly activated immature-looking lymphocytes in lymph node biopsies may suggest a malignant process

Therapy

to kill pathogen-infected APCs and thus remove the stimulus for the ongoing but ineffective activation of T cells. The search for a triggering infectious agent like HSV, VZV, EBV, CMV, adenovirus, and Leishmania is important since most of these organisms are treatable. However, it should be emphasized that, with the possible exception of leishmaniasis, in which most patients promptly respond to liposomal amphotericin B , anti-infectious therapy alone is not sufficient to control HLH. Viral PCRs are more helpful than serology. Positive results are useful to follow during antiviral treatment
in genetic HLH the ultimate aim must be allogeneic HSCT to exchange the congenitally defective immune system with normal functioning immune effector cells.

Mortality was 14 times higher for patients with EBV-associated HLH who did not receive etoposide within the first 4 weeks

^ref

Although symptoms and laboratory abnormalities usually improve within 2–3 weeks of treatment, persistent cytopenias could indicate either non-response to therapy or myelosuppression by etoposide. A repeat bone marrow examination may be helpful

at least 3–4 doses of etoposide should be given before a decision is made to interrupt the drug

daclizumab

alemtuzumab

Antithymocyte globulin

^ref

allogeneic HSCT

^ref

methotrexate

^ref

HLH protocol

intensive supportive therapy
treatment of coagulopathy disorders
specific antiviral therapy
pulse therapy with high-dose GR agonists ^ref and immunosuppressive treatment
effective control of disease in some patients with infection-associated HPS can be achieved with 20 to 25 mg/kg chloroquine per day orally for 7 days^ref
splenic irradiation (720 cGy in fraction of 180 cGy) => splenectomy and IFN-a for 2 years^ref
continuous hemofiltration in attenuating the consequences of excess cytokine activity, with therapy titrated to the degree of lactic acidosis^ref
anti-cancer therapy should be preceded by anti-viral therapy and withdrawal of immunosuppressive therapy in patients under immunosuppressive therapy, as long as the clinical situation permits^ref
anti-CD25 antibody ^ref

Prognosis

Therapy

lymphocytapheresis

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