Table of contents :

• EGFR inhibitors. Gefitinib (250 mg/day) was the first molecularly targeted agent to be approved for the treatment of metastatic NSCLC, on the basis of data from 2 large phase II trials of gefitinib monotherapy (250 vs 500 mg/day) in previously treated patients with advanced NSCLC^{ref1, ref2}. In these trials, response rates and survival were the same for 250 mg/day and 500 mg/day gefitinib, but the frequency and severity of adverse events were greater at the higher dose. At the lower dose, the objective response rate was 12–18%, and higher objective response rates were observed in women, never-smokers, and patients with adenocarcinoma (in both trials^{ref1, ref2}) and in Japanese patients (in the trial by Fukuoka and colleagues^ref only)^{ref1, ref2, ref3}. Encouraging survival data (median survival 7–8 months; 1-year survival 27–35%) have been supported by data from > 21000 patients treated as part of an Expanded Access Programme, among whom 1-year survival was 30% (Ochs J, Grous JJ, Warner KL. Final survival and safety results for 21,064 non-small-cell lung cancer (NSCLC) patients who received compassionate use gefitinib in a U.S. expanded access program (EAP). Proc Am Soc Clin Oncol 2004; 23: 628abstr 7060). In a phase II trial of erlotinib in previously treated patients with NSCLC, the results were similar: the response rate was 12.3%, median survival was 8 months, and 1-year survival was 40%^ref. Response rates are 10 to 20% when these ATP-competitive anilinoquinazoline inhibitors are used as second- or third-line treatment for advanced disease^{ref1, ref2,ref3}. Responsiveness to these drugs is a characteristic of distinct subgroups of patients: women, patients who have never smoked, patients with adenocarcinoma, and Asians^ref. In the majority of patients with highly responsive tumors, the tumor contains somatic mutations of the EGFR gene. These mutations are small deletions that affect amino acids 747 through 750 or point mutations (most commonly a replacement of leucine by arginine at codon 858 [L858R])^{ref1, ref2, ref3}. These mutations mediate oncogenic effects by altering downstream signaling and antiapoptotic mechanisms^ref. Both types of mutation increase the sensitivity of the tumor to anilinoquinazoline inhibitors of EGFR, most likely by repositioning critical residues surrounding the ATP-binding cleft of the tyrosine kinase domain of the receptor, thereby stabilizing their interactions with both ATP and its competitive inhibitors^{ref1, ref2}. Notwithstanding the success of these drugs in cases of non–small-cell lung cancer with activating EGFR mutations, it appears that all cases eventually progress despite such treatment. It cause tumor regression in about 25% of NSCLC cases in Japan, but only about 10% of cases in the USA because activating EGFR mutations are found in 25% of tumors from Japan, and just ~1.5% of US tumors^ref1,ref2. Threonine-to-methionine amino acid change at position 790 of EGFR confers resistance^ref. Epithelial membrane protein-1 (EMP-1) is a surface biomarker of gefitinib resistance, independent of gefitinib-sensitizing EGFR somatic mutations^ref. Treatment with gefitinib as second-line or third-line treatment for patients with locally advanced or metastatic NSCLC was not associated with significant improvement in survival. There was pronounced heterogeneity in survival outcomes between groups of patients, with some evidence of benefit among never-smokers and patients of Asian origin^ref. EGF-R mutations^ref
• BCR-c-Abl inhibitors : therapy of chronic myelogenous leukemia (CML)^ref (clinical activity is highest in patients with chronic-phase CML^{ref1, ref2}), Ph⁺ B-cell acute lymphoblastic leukemia (B-ALL), GIST, and Leydig cell tumor^ref : around 12-20% of patients become resistant and up to now, 25 resistance-causing mutations have been spotted. The annual progression rate during treatment of chronic-phase CML with imatinib is 4%^ref. Imatinib therapy has side effects that can be dose-limiting in 10% of patients^ref
• imatinib mesylate / STI 571 / STI571 (Glivec^©; Novartis Pharmaceuticals Corp. changed the spelling from Glivec^© to Gleevec^© for the US market to avoid confusion with other medicines)

To realize the full potential of targeted protein kinase inhibitors for the treatment of cancer, it is important to address the emergence of drug resistance in treated patients. Mutant forms of BCR-ABL, KIT, and EGFR have been found that confer resistance to the drugs imatinib, gefitinib, and erlotinib. The mutations weaken or prevent drug binding, and interestingly, one of the most common sites of mutation in all 3 kinases is a highly conserved "gatekeeper" threonine residue near the kinase active site. The Aurora kinase inhibitor VX-680 and the p38 inhibitor BIRB-796 inhibit the imatinib- and BMS-354825-resistant ABL(T315I) kinase. The KIT/FLT3 inhibitor SU-11248 potently inhibits the imatinib-resistant KIT(V559D/T670I) kinase, consistent with the clinical efficacy of SU-11248 against imatinib-resistant gastrointestinal tumors, and the EGFR inhibitors EKB-569 and CI-1033, but not GW-572016 and ZD-6474, potently inhibit the gefitinib- and erlotinib-resistant EGFR(L858R/T790M) kinase. EKB-569 and CI-1033 are already in clinical trials, and they should be considered for testing in the treatment of gefitinib/erlotinib-resistant NSCLC. The results highlight the strategy of screening existing clinical compounds against newly identified drug-resistant mutant variants to find compounds that may serve as starting points for the development of next-generation drugs, or that could be used directly to treat patients that have acquired resistance to first-generation targeted therapy^ref.
BCR-ABL as a therapeutic target : chronic myeloid leukemia (CML) is characterized by the presence of a BCR-ABL fusion gene, which is the result of a reciprocal translocation between chromosomes 9 and 22, cytogenetically visible as a shortened chromosome 22 (Philadelphia [Ph] chromosome)^ref (Nowell P, Hungerford D. A minute chromosome in human chronic granulocytic leukemia. Science. 1960;132: 1497). Rare patients with a clinical presentation indistinguishable from CML do not express BCR-ABL and were previously diagnosed as "BCR-ABL– CML." Because this group of diseases is biologically different, the World Health Organization has defined CML as the BCR-ABL⁺ disease (Vardiman JW, Pierre R, Thiele J, et al. Chronic myeloproliferative diseases. In: Jaffe ES, Harris NL, Stein H, Vardiman JW, eds. Tumors of Haematopoietic and Lymphoid Tissues. Lyon: IARCPress; 2001: 15-59). To avoid confusion, patients without BCR-ABL expression should be diagnosed with "myeloproliferative syndrome, unclassifiable" if they do not fulfill diagnostic criteria of another entity. Research in the past 2 decades has established that BCR-ABL is the causal to the pathogenesis of CML, and that constitutive tyrosine kinase activity is central to BCR-ABL's capacity to transform hematopoietic cells in vitro and in vivo^{ref1, ref2}. The activation of multiple signal transduction pathways in BCR-ABL–transformed cells leads to increased proliferation, reduced growth-factor dependence and apoptosis, and perturbed interaction with extracellular matrix and stroma. It is thought that the expression of BCR-ABL endows a pluripotent hematopoietic progenitor cell and/or its progeny with a growth and survival advantage over normal cells, which in time leads to the clinical manifestation of CML. An in-depth appraisal of the molecular and cellular biology of CML is beyond the scope of this review, and the reader is referred to recent comprehensive publications^{ref1, ref2}. The fact that it proved difficult to identify "essential" components downstream of BCR-ABL indicates that from the therapeutic standpoint BCR-ABL is by far the most attractive drug target.
Development of an ABL tyrosine kinase inhibitor : the essential role of BCR-ABL tyrosine kinase activity for cellular transformation provided the rational for targeting this function therapeutically^ref. In 1992, Anafi and colleagues^{ref1, ref2} reported a tyrphostin, related to erbstatin, that inhibited the tyrosine kinase activity of BCR-ABL and suggested that it might be possible to design specific compounds for the treatment of ABL-associated human leukemias. Subsequently, the tyrphostins AG568, AG957, and AG1112 were identified as the most specific compounds. Growth inhibition of the CML cell line K562 occurred at micromolar concentrations and was associated with inhibition of BCR-ABL tyrosine kinase activity^ref. Tyrphostins are competitive toward adenosine triphosphate (ATP) or substrate, or both. Although active in vitro, they have not been developed for clinical use. Another early compound with activity toward BCR-ABL is herbimycin A, an antibiotic derived from Streptomyces hygroscopicus^ref. Herbimycin A was originally thought to inhibit BCR-ABL tyrosine kinase^ref but it was subsequently shown to promote BCR-ABL protein degradation^ref. Selective inhibition of primary CML cells was also shown for genistein, a flavonoid^ref. Starting in the late 1980s, scientists at Ciba Geigy (now Novartis), under the direction of N. Lydon and A. Matter, initiated projects on the identification of compounds with inhibitory activity against protein kinases. In one medicinal chemistry project focusing on protein kinase C (PKC) as a target, a 2-phenylaminopyrimidine derivative was identified as a lead compound (Figure 1)^{ref1, ref2}. This compound had low potency and poor specificity, inhibiting both serine/threonine and tyrosine kinases, but from this starting point, a series of derivatives were synthesized. The addition of a 3'-pyridyl group at the 3'-position of the pyrimidine (Figure 1A) enhanced the cellular activity of the derivatives. Activity against tyrosine kinases was enhanced by introduction of a benzamide group at the phenyl ring (Figure 1B). A key observation from analysis of structure activity relationships was that substitutions at the 6-position of the anilino phenyl ring led to loss of PKC inhibition. However, the introduction of a "flag-methyl" group at this position retained or enhanced activity against tyrosine kinases (Figure 1C). Profiling of the compounds showed that they also inhibited the ABL tyrosine kinase. The first series of compounds had poor oral bioavailability, with low water solubility. The attachment of a highly polar side chain, N-methylpiperazine, markedly improved solubility and oral bioavailability (Figure 1D). STI571 (formerly CGP57148B, now imatinib mesylate; Gleevec or Glivec, Novartis, Basel, Switzerland) emerged as the most promising compound for clinical development, since it had the highest selectivity for growth inhibition of BCR-ABL–expressing cells. Development of imatinib from a 2-phenylaminopyrimidine backbone (shown in white). (A) Activity in cellular assays was improved by introduction of a 3' pyridyl group (yellow) at the 3' position of the pyrimidine. (B) Activity against tyrosine kinases was further enhanced by addition of a benzamide group (orange) to the phenyl ring. (C) Attachment of a "flag-methyl" group (green) ortho to the diaminophenyl ring strongly reduced activity against PKC. (D) Addition of an N-methylpiperazine (purple) increased water solubility and oral bioavailability.

In vitro profile of imatinib :
• inhibition of kinase activity : studies using purified enzymes expressed as bacterial fusion proteins or using immunoprecipitations of intact proteins showed that imatinib potently inhibits all of the ABL tyrosine kinases. This includes cellular ABL, viral ABL (v-ABL), and BCR-ABL (Table 1)^{ref1, ref2, ref3}. In contrast, the compound was inactive against serine/threonine kinases, did not inhibit the epidermal growth factor (EGF) receptor intracellular domain, and showed weak or no inhibition of the kinase activity of the receptors for vascular endothelial growth factor (VEGF-R1 and VEGF-R2), fibroblast growth factor receptor 1 (FGF-R1), tyrosine kinase with immunoglobulin and EGF homology-2 (TIE-2 [TEK]), c-MET, and nonreceptor tyrosine kinases of the SRC family (FGR, LYN, and LCK).

enzyme	substrate phosphorylation IC50 [µM] (* = determined in immunocomplex assays)	cellular tyrosine phosphorylation IC50 [µM]
c-ABL	0.2; 0.025*	ND
v-ABL	0.038	0.1-0.3
P210BCR-ABL	0.025*	0.25
P185BCR-ABL	0.025*	0.25
TEL-ABL	ND	0.35
PDGF-R a and b	0.38 (PDGF-Rb)	0.1
Tel-PDGF-R	ND	0.15
c-KIT	0.41	0.1
FLT-3	> 10	> 10
Btk	> 10	ND
c-FMS and v-FMS	ND	> 10
c-SRC	> 100	ND
v-SRC	ND	> 10
c-LYN	> 100	ND
c-FGR	> 100	ND
LCK	9.0	ND
SYK (TPK-IIB)	> 100	ND
JAK-2	> 100*	> 100
EGF-R	> 100	> 100
Insulin receptor	> 10	> 100
IGF-IR	> 10	> 100
FGF-R1	31.2	ND
VEGF-R2 (KDR)	10.7	ND
VEGF-R1 (FLT-1)	19.5	ND
VEGF-R3 (FLT-4)	5.7	ND
TIE-2 (TEK)	> 50	ND
c-MET	> 100	ND
PKA	> 500	ND
PPK	> 500	ND
PKCa, b1, b2, g, d, e, z, or h	> 100	ND
Protein kinase CK-1, CK-2	> 100	ND
PKB	> 10	ND
P38	> 10	ND
PDK1	> 10	ND
c-Raf-1	0.97	ND
CDC2/cyclin B	> 100	ND

The results of the kinase assays were confirmed in cell lines expressing constitutively active forms of ABL such as v-ABL,17 p210^BCR-ABLref, p185 BCR-ABL^{ref1, ref2}, and translocated ets leukemia (TEL)–ABL^ref, where imatinib was found to inhibit ABL kinase activity with 50% inhibitory concentration (IC₅₀) values ranging between 0.1 and 0.35 µM. Numerous Ph⁺ cell lines derived from patients with CML or acute lymphoblastic leukemia (ALL) have subsequently been tested. In most of these lines, the IC50 values were also in the range of 0.1 to 0.5 µM, indicating that the compound effectively penetrates the cell membrane^{ref1, ref2, ref3}.
Consistent with its in vitro profile, imatinib inhibited signaling of the ligand-activated platelet-derived growth factor receptor (PDGFR)^{ref1, ref2}, as determined by ligand-stimulated PDGFR autophosphorylation, at an IC50 of 0.1 to 1 µM. Inhibition of the constitutively active TEL-PDGFR fusion protein was observed at an IC50 of 0.15 µM^ref. Furthermore, the compound potently inhibited autophosphorylation of the KIT receptor upon binding of its cognate ligand, stem-cell factor (SCF)^{ref1, ref2}, and to suppress KIT autophosphorylation in a cell line established from a patient with a gastrointestinal stromal tumor (GIST) with an activating Kit mutation^ref. In contrast, signal transduction mediated by EGF, insulin, insulin-like growth factor I (IGF-I), FGF, and phorbol ester was insensitive to imatinib^ref. Furthermore, imatinib did not affect FLT-3 or the receptor for colony-stimulating factor 1 (CSF-1, FMS), or the nonreceptor tyrosine kinases SRC and JAK-2. The latter mediates signaling from a number of cytokine receptors, including the receptors for IL-3, G-CSF, and erythropoietin^ref.
• effects upon cell proliferation and apoptosis in vitro : effects on cells with activated ABL signaling. Imatinib was tested for its antiproliferative activity against a variety of cell lines expressing activated ABL proteins, including lines that had been transduced to factor independence by p210BCR-ABL as well as their growth factor–dependent parental cells^ref. Imatinib potently inhibited the growth of cells expressing p210BCR-ABL, while up to 10 µM did not inhibit growth of parental or v-SRC–transformed cells. Similar activity was seen in p185BCR-ABL– and TEL-ABL–transformed cells^ref. The selective growth-inibitory effect was confirmed in many cell lines derived from CML or Ph+ ALL^{ref1, ref2, ref3, ref4, ref5}, while Ph– cell lines were unaffected^{ref1, ref2}. The in vitro IC₅₀ for inhibition of proliferation generally paralleled the IC₅₀ values for inhibition of BCR-ABL kinase activity seen in cellular assays. Exposure to imatinib led to apoptotic cell death^{ref1, ref2}. Additional studies demonstrated activity in fresh leukemic cells from patients with CML and Ph+^{ref1, ref2} 21,22 and selective inhibition of colony formation by committed progenitor cells from patients with CML, with little effect on normal hematopoiesis at concentrations of up to 1 µM^{ref1, ref2}. The latter findings were confirmed in stroma-dependent long-term cultures^ref.
• effects on cell lines with activated PDGFR or c-KIT signaling. Imatinib strongly inhibited proliferation of v-sis–transformed BALB/c 3T3 mouse fibroblasts, which proliferate autonomously due to autocrine PDGF production^ref. Furthermore, the compound dose-dependently suppressed PDGF-stimulated proliferation of A10 rat aorta smooth muscle cells but did not affect serum-induced growth^ref. Cells expressing a TEL-PDGF receptor fusion protein were also imatinib sensitive^ref. Growth inhibitory activity was also seen against a cell line established from a patient with a GIST, which contained an activating point mutation in KIT^ref. In contrast, no activity was seen in a cell line derived from human malignant mastocytosis with a mutation in the activation loop (A-loop) of the kinase (D816V)^ref. Thus, this specific mutation activates the kinase while conferring imatinib resistance at the same time. Imatinib was also found to inhibit SCF-mediated growth of small-cell lung cancer cell lines. The IC50 values for inhibition of KIT autophosphorylation and proliferation were 0.1 and 0.3 µM, respectively, in serum-free media, whereas growth inhibition in serum-containing media required higher drug levels and was not strictly correlated with KIT expression (IC50 in the range of 5 µM), suggesting that additional targets were modified^{ref1, ref2}.
• In vivo profile of imatinib: animal models. To test the effects of imatinib on tumor growth, BCR-ABL–transformed 32D cells were injected into syngeneic mice^ref. Once-daily intraperitoneal treatment using doses of imatinib from 2.5 to 50 mg/kg, starting 1 week after cell injection, caused dose-dependent inhibition of tumor growth (Figure 3), while 50 mg/kg intraperitoneal treatment was inactive against tumors derived from v-SRC–transformed 32D cells, consistent with the lack of inhibition of SRC kinase activity by imatinib. Similar experiments in nude mice using KU812 cells, a BCR-ABL+ human cell line, demonstrated the need for continuous inhibition of BCR-ABL kinase activity to achieve maximal antitumor effects^ref. Early pharmacokinetic studies at Novartis had demonstrated that imatinib is rapidly absorbed following oral administration to mice and pharmacologically relevant concentrations are achieved in the plasma, with a half-life of approximately 1.3 hours. Optimization of the treatment schedule to 3 times daily administration of 50 mg/kg intraperitoneally or 160 mg/kg orally for 11 consecutive days, assuring continuous blockage of p210BCR-ABL tyrosine kinase, resulted in tumor-free survival of mice injected with KU812 cells. With the same schedule, established tumor nodules began to regress 48 hours after beginning treatment; by day 8, no treated animal had measurable disease. 8 of 12 animals remained tumor free with over 200 days of follow-up, while 4 relapsed on days 48 through 60. The antitumor effect of imatinib was specific for p210BCR-ABL expressing cells, as no growth inhibition occurred in mice injected with U937, a BCR-ABL– myeloid cell line. Imatinib was also tested in the transduction-transplantation model of CML^ref. In this system, lethally irradiated syngeneic mice receive marrow infected with a BCR-ABL retrovirus and consistently die within 3 weeks from an aggressive CML^ref. Treatment with imatinib (50 mg/kg in the morning, 100 mg/kg in the evening) led to prolonged survival^ref. Responses were quite variable, with 25% of animals having refractory disease. Imatinib was not capable of preventing CML, even if started as early as 48 hours after transplantation, but none of the responders progressed on therapy. No consistent association between response and BCR-ABL mRNA and protein levels was seen, and no other cause underlying refractoriness could be determined. Notably, there was a trend toward "clonal depletion" in responding animals, suggesting that imatinib was able to successfully target some, but not all leukemic clones.
Clinical studies:
• imatinib monotherapy
• phase 1 trials with imatinib began in June of 1998 and were designed to determine the maximally tolerated dose, with clinical benefit as a secondary endpoint. Patients in the chronic phase of CML who had failed therapy with interferon- (IFN) were eligible^ref. Imatinib, given as daily oral therapy, was well tolerated, without dose-limiting toxicity. Hematologic responses were seen at doses of 140 mg and greater. Most remarkable was that 53 of 54 patients treated with at least 300 mg showed complete hematologic responses (CHR). Moreover, at doses of 300 mg and higher, cytogenetic responses were achieved in 31% of patients, with 13% achieving complete response. Pharmacokinetic studies revealed that above 300 mg, plasma levels equivalent to the effective in vitro level (1 µM) were achieved. At 400 mg, the current standard dose for CML in chronic phase, peak levels at steady state were approximately 4.6 µM and trough levels approximately 2.13 µM, with a half-life of 19.3 hours, indicating that once-daily dosing was sufficient to provide continuous kinase inhibition^ref. Side effects were generally mild and included nausea, diarrhea, periorbital edema, and skin rashes. Myelosuppression was frequent, likely reflecting efficacy due to suppression of Ph+ hematopoiesis rather than toxicity. Based on these extremely promising results, the phase 1 study was expanded to patients with myeloid and lymphoid blast crisis of CML and patients with relapsed or refractory Ph+ ALL^ref. With doses of 300 to 1000 mg/d, 11% of patients with myeloid blast crisis achieved CHR, and another 10% achieved a reduction of bone marrow blasts to < 5%, without complete recovery of peripheral blood counts. In patients with lymphoid disease, the corresponding remission rates were 20% and 15%, respectively. Unfortunately, most patients with myeloid and all but 1 patient with lymphoid blast crisis relapsed within weeks to months.
• phase 2 studies began in late 1999 using imatinib as a single agent for all stages of CML. For patients in blast crisis and with Ph+ ALL, these studies confirmed the results of the phase 1 trial^{ref1, ref2}. Patients in chronic phase who had failed IFN therapy did much better than expected, with CCR rates of 41% and major cytogenetic remission (MCR) of 60%^ref. Importantly, these responses were usually durable, resulting in a progression-free survival of 89.2% at 18 months. Not surprisingly, the efficacy in patients with accelerated phase was intermediate between chronic phase and blast crisis^ref. The results of the phase 1 and 2 trials led to the approval by the Food and Drug Administration of imatinib for the treatment of CML in advanced phase and after failure of IFN therapy. A recent retrospective study compared the survival of 143 patients who received imatinib after failure of IFN-based therapy with 246 historical controls managed with conventional therapy and found a significant overall survival benefit for patients treated with imatinib, which was, however, confined to those patients who achieved a cytogenetic response^ref. In contrast, a subsequent study showed a survival benefit for all patients treated with imatinib, regardless of cytogenetic response, a discordance that may be due to the statistical methods used^ref. Responses to imatinib in blast-crisis and accelerated phases of CML :

	overall hematologic response/CHR, %	sustained hematologic responses, % (> 4 wk)	MCR, %	CCR, %	median survival, mo
myeloid blast crisis, n = 229	52/15	31	16	7	6.8
Ph+ ALL and lymphoid blast crisis of CML, n = 56	59/22	27	NA	NA	4.9
accelerated phase, % (n = 181)	82/53	69	24	17	not reached
chronic phase after failure of IFN therapy	95% sustained CHR	95% sustained CHR	60	41	not reached

• phase 3 study : imatinib and the combination of IFN plus cytarabine were compared in a randomized trial, which showed imatinib to be vastly superior compared with CHR, MCR, and CCR, as well as progression-free survival^ref. A recent update showed a CCR rate of 81% at 30 months. Since the design of this study allowed crossover for lack of efficacy or intolerance, a large proportion of patients crossed from IFN/cytarabine to imatinib. As imatinib effectively rescued these individuals, the true differences between the groups were certainly underestimated, and no difference in overall survival was observed. However, a retrospective comparison with a historical control group treated with IFN showed superior survival for patients on imatinib^ref. In addition to its superior efficacy, patients on imatinib have a far better quality of life^ref. Based on these results, the drug was approved by the regulatory authorities for first-line treatment of CML in the United States and Europe.Responses to imatinib versus IFN plus cytarabine in newly diagnosed patients with CML in chronic phase (mmedian duration of follow-up equaled 19 months) :

	CHR, %	MCR, %	CCR, %	progression-free survival, 14 mo
imatinib, n = 553	95.3	85.2	73.8	92.1
IFN + cytarabine, n = 553	55.5	22.1	8.5	73.5
P	.001	.001	.001	.001

Monitoring of residual disease by quantitative RT-PCR in complete cytogenetic responders showed that the risk of disease progression was inversely correlated with the reduction of BCR-ABL mRNA compared with pretherapeutic levels. PFS was 100% at 24 months in patients who achieved a reduction of their BCR-ABL transcripts by 3 orders of magnitude or more by 12 months, a state termed major molecular response. In contrast, the risk of disease progression at 24 months was 5% in patients with a less than 3-log reduction of BCR-ABL transcripts, and 15% in those who failed to achieve CCR^ref. It should be noted that the average BCR-ABL expression of a group of untreated patients was used as the reference in this study, while other studies have used individual pretherapeutic levels^ref. It is possible that the use of individual pretherapeutic levels would lead to a slightly different predictive model.
• imatinib in combination with other agents : a number of studies were initiated to improve the efficacy of imatinib monotherapy by combining the drug with other active agents, such as IFN, homoharringtonine, and cytarabine, or by increasing the dose. The study populations included either newly diagnosed patients or patients after failure of IFN therapy. The general theme is that CCR tends to occur earlier, but at the expense of more toxicity, particularly myelosuppression. In a recently published phase 2 study with an imatinib/cytarabine combination, the rate of grades 3/4 hematologic toxicity was 53%^ref, compared with approximately 20% with imatinib monotherapy^ref. After 3 months, the rate of MCR was 70%, compared with approximately 60% for imatinib monotherapy. However, after 12 months, the gap had practically closed, with 83% major cytogenetic responses, compared with approximately 84% with imatinib alone. Similar observations were made with a combination of imatinib and pegylated IFN^ref. In a single-institution study of IFN-refractory patients, the rate of CCR on 800 mg imatinib daily was 89%, compared with 41% with 400 mg in the phase 2 multicenter trial^ref. Due to the fact that the risk profile in the single-center study was more favorable than in the phase 2 study, a direct comparison of the data is impossible. Nonetheless, together with the observation that dose escalation in cytogenetically refractory patients leads to cytogenetic responses in some patients^ref, these data lend support to the notion that response rates may increase with higher doses of imatinib. Several large phase 3 studies have been initiated in Europe that compare standard-dose imatinib versus higher doses and combinations with IFN or cytarabine, and a Southwest Oncology Group (SWOG) trial comparing 400 versus 800 mg imatinib daily is expected to start in early 2005. These studies should clarify whether combination treatment or higher doses of imatinib are superior to standard therapy. Given the high rates of CCR and progression-free survival with standard therapy, it might take many years to detect significant differences. Thus, novel surrogate endpoints such as negativity by RT-PCR are needed.
Resistance to imatinib :
• distinguishing refractory and resistant disease : response rates and the durability of responses to imatinib are highly dependent on the stage of disease at which treatment is initiated^{ref1, ref2, ref3, ref4}. Refractoriness (primary resistance) should be distinguished from secondary resistance that develops after an initial response, as the underlying mechanisms may be different. Potentially, the greatest long-term concern is the high rate of molecular refractoriness. In the phase 3 trial, < 4% of patients with CCR were negative for BCR-ABL on at least 1 occasion^{ref1, ref2} and another study found no molecular responders among 120 patients with late chronic phase^ref. The much higher rates of RT-PCR negativity reported in some other studies may be due to the use of less sensitive assays, such as quantitative RT-PCR only, without confirmation by nested RT-PCR^ref. Rates of complete hematologic remission, complete cytogenetic remission, and molecular remission (defined as RT-PCR negativity) in the phase 2 and 3 trials with imatinib monotherapy.


It is not yet known whether patients in CCR with minimal residual disease will invariably relapse after discontinuation of imatinib or remain in remission. Anecdotal cases suggest that both are possible^{ref1, ref2}, similar to patients on IFN^ref. Notably, IFN-induced CCR involves cytotoxic T-cell responses against leukemia-specific antigens, similar to allografting, whereas no such response is demonstrable in patients with imatinib-induced CCR. This may imply that continuous imatinib therapy is required to maintain CCR, as long as minimal residual disease persists^{ref1, ref2}. In patients after allografting, RT-PCR negativity is a therapeutic goal because of its strong predictive power for freedom from progression^ref, and longer follow-up will be necessary to establish whether this holds true for patients on imatinib^ref. Another unresolved issue is therapy-induced cytopenia, which is an adverse prognostic feature^ref. If cytopenia is the result of less intensive treatment because of dose interruptions or reflects more advanced disease is not yet clear, but G-CSF and/or erythropoietin to allow full dosing is widely used in such patients.
• laboratory studies : most BCR-ABL⁺ human cell lines are sensitive to imatinib at concentrations < 0.5 µM. Exceptions include SD-1 and KCL-22. Both lines proliferate in the presence of 0.5 to 1 µM imatinib, despite the fact that BCR-ABL autophosphorylation is inhibited^{ref1, ref2, ref3}. In SD-1 cells, resistance may be explained by their being EBV–transformed^ref, suggesting that their proliferation and survival are dependent on EBV-driven signals rather than BCR-ABL. In KCL-22 cells, comparison of gene expression by microarray showed marked differences between an imatinib-sensitive and an imatinib-resistant clone of this cell line, although it is not clear how exactly this relates to their resistant phenotype^ref. To model resistance in vitro, several groups have generated imatinib-resistant cell lines by culture in gradually increasing concentrations of imatinib, which usually required several months^{ref1, ref2, ref3}. The most common mechanism of resistance in these lines is a significant increase of BCR-ABL mRNA and protein, sometimes associated with gene amplification. In addition to overexpression of BCR-ABL, increased expression of MDR1 has been observed in imatinib-resistant Lama-84 cells, and resistance was partially reversible by verapamil, a P-glycoprotein (PGP) inhibitor^ref. Several other studies have since reported on the role of PGP as a transporter of imatinib in cell lines, indicating that MDR1 expression confers resistance^{ref1, ref2, ref3, ref4, ref5}, although this was not universially confirmed^ref. Overexpression of LYN, an SRC kinase, was demonstrated in an imatinib-resistant clone of the K562 cell line^ref. Compared with the parental line, these cells expressed reduced amounts of BCR-ABL, and inhibition of BCR-ABL by imatinib did not affect growth and viability. In contrast, treatment with an SRC kinase inhibitor affected the resistant but not the parental line. The in vitro selection conditions for resistant cell clones greatly influence the type of resistance. Mutations of the ABL kinase domain (KD) were only rarely found in imatinib-resistant lines^{ref1, ref2}, although a recent study was able to reproducibly generate KD mutant BaF/3BCR-ABL clones with a limiting dilution strategy^ref. The human BCR-ABL⁺ leukemia cell line KU812 injected into nude mice was used to study the mechanisms underlying in vivo resistance to imatinib^ref. If imatinib treatment was started in mice with measurable tumors, there was a high rate of relapse after an initial response. Surprisingly, the tumor cells retained sensitivity to imatinib in vitro, despite their apparent resistance in vivo. Additional studies showed that the plasma concentrations of a₁–acidic glycoprotein (AAG) in the animals with resistance were elevated and that AAG avidly binds imatinib, reducing its bioavailability^ref. The ability of AAG to mediate in vitro resistance to imatinib is still controversial^{ref1, ref2, ref3}.

The SLC22A1 / human organic cation transporter 1 (hOCT1) actively transports imatinib into cells, and low expression of hOCT1 has been detected before treatment in cells from patients who failed to achieve a good cytogenetic response^ref. Likewise, imatinib is also a substrate of the ABCB1 pump glycoprotein encoded by the MDR1 gene, the overexpression of which leads to excessive efflux and cellular resistance to imatinib^{ref1, ref2}. The relationship between imatinib and ABCG2 (BRCP), another efflux protein of the ATP binding cassette family, is, however, less clear, and the source of much controversy lately. At least 4 independent groups have investigated this issue, reaching somewhat different conclusions. Thus, Houghton et al^ref reported that imatinib is an inhibitor but not a substrate of ABCG2, whereas Burger et al^ref concluded otherwise when demonstrating that ABCG2-overexpressing cell lines are resistant to imatinib. Recently, Nakanishi et al^ref showed that the interaction between ABCG2 and imatinib in BCR-ABL–expressing cells is in fact rather complex, with ABCG2-mediated resistance to imatinib being counteracted by the inhibitor's capacity to down-modulate ABCG2 expression via the AKT signaling pathway. A crucial limitation of all 3 studies is the fact that they are based on cell lines engineered to overexpress ABCG2, and do not therefore represent the true clinical targets of imatinib (ie, primary cells from CML patients). A large proportion of CD34⁺ cells from patients at diagnosis of CML express significant amounts of ABCG2 protein, unlike their normal counterparts. Furthermore, by measuring the accumulation of imatinib in these CML progenitor CD34⁺ cells, they provide evidence that, as suggested by Houghton et al^ref, imatinib is an inhibitor but not a substrate of ABCG2, and does not therefore mediate resistance in these cells. Although rather compelling in their own right, the data still leave room for some questions. Thus, the use of 5 µM imatinib for inhibiting ABCG2-mediated substrate efflux in CML cells may not be clinically relevant. Likewise, such a high dose may be "saturating," blocking any possible additional effect of fumitremorgin C, a specific ABCG2 inhibitor, and obscuring therefore the possibility that imatinib could be also a substrate of ABCG2^ref
• clinical resistance :
• amplification and overexpression of BCR-ABL. In a study by Gorre et al^ref, FISH demonstrated amplification of BCR-ABL at the genomic level in 3 of 9 patients with resistant disease. In a subsequent report, an increase in the level of BCR-ABL mRNA was seen in 4 of 37 patients^ref.84 Both mechanisms are thought to lead to increased expression of BCR-ABL protein, although, due to the difficulties analyzing BCR-ABL protein in clinical specimens, this has not yet been formally demonstrated
• mutations of the BCR-ABL KD. Enzyme kinetics suggest that imatinib functions as a competitive inhibitor of ATP binding to the ABL kinase with a inhibition constant (Ki) value of 85 nM for c-ABL^ref. The crystal structure of the catalytic region of both the murine and human ABL kinase in complex with an imatinib analog^ref and with imatinib^ref (Manley PW, Cowan-Jacob SW, Buchdunger E, et al. Imatinib: a selective tyrosine kinase inhibitor. Eur J Cancer. 2002;38(suppl 5): S19-S27) has been solved. Imatinib intimately interacts with the KD, engaging > 21 amino acid residues^ref. The most important finding is that imatinib binds ABL in the kinase-inactive conformation, in which the A-loop, the major regulatory element, occludes the catalytic center. In contrast, steric hindrance prevents imatinib binding to the open, active conformation of the A-loop. This mode of binding is critical to imatinib's high selectivity for ABL over other kinases, since the structural diversity of the A-loops of different kinases is largely restricted to their inactive conformations, while the A-loops of active kinases are very similar.


Ribbon representation of ABL in complex with imatinib and ID180970. Shown is (A) the conformation of Abl (blue) in complex with imatinib (orange), with the A-loop (magenta) in a "closed" conformation, and (B) the Abl conformation (green) in the PD180970 (red) complex with the A-loop (magenta) in an "open" conformation. The P-loop (yellow) folds down over the inhibitor in both cases. Figure prepared by Sandra W. Cowan-Jacob based on reported structures^ref (Manley PW, Cowan-Jacob SW, Buchdunger E, et al. Imatinib: a selective tyrosine kinase inhibitor. Eur J Cancer. 2002;38(suppl 5): S19-S27)
Mutations of the KD are found in 50% to 90% of patients with secondary resistance^{ref1, ref2, ref3, ref4, ref5, ref6}. Characterization of the mutants by in vitro kinase assays, quantification of intracellular BCR-ABL phosphorylation, and proliferation assays generally revealed an IC₅₀ shift toward higher concentrations of imatinib, although the degree of resistance varies (values are given as fold changes over wild type) :
 

				IC50, µM
wild-type ABL numbering according to ABL exon Ia/Ib	Exchange	Patients, total = 177	%	BCR-ABL phosphorylation in cells	ABL autophosphorylation (in vitro kinase assay)	Cell proliferation
M244/M263	V	3	1.69	NR*	0.03, 0.64, 1	1, 1.6
L248/L267 (L267R had greater than 33-fold increased resistance in proliferation assays)	V	1	0.56	NR*	NR	NR
G250/G269	E	6	3.39	7.4 to > 10	1.6	4.5 to > 20
G250/G269	A	1	0.56	NR	NR	NR
Q252/Q271	H	8	4.52	2.9, 10.4	NR	2.8 to 9.3
Q252/Q271	R	1	0.56	10.4	NR	NR
Y253/Y272	F	6	3.39	5.9, 21.4	72	3 to 8.9
Y253/Y272	H	12	6.78	21.4	150	17.7, > 33
E255/E274	K	34	19.21	27.9	> 200	15 to 33
E255/E274	V	4	2.26	7.3	3.5, > 200	7.7, > 33
D276 (D276V had greater than 2-fold increased resistance in proliferation assays)/D295	G	1	0.56	NR	NR	NR
F311/F330	L	1	0.56	NR*	0.031, 1	0.7 to 2.1
T315/T334	I	37	20.9	> 10	> 10	5.2 to > 10
T315/T334	N	1	0.56	NR	NR	NR
F317/F336	L	7	3.95	0.8 to 11.8	0.25, 0.38, 8.3	1.3 to 13
M343/M362	T	1	0.56	NR	NR	NR
M351/M370	T	27	15.25	0.6 to 3.9	0.26, < 1	0.9 to 7.3
E355/E374	G	5	2.82	2.8, 10	0.02, 0.8	2.3, 4
F359/F378	A	1	0.56	NR	NR	NR
F359/F378	V	7	3.95	NR	0.05, 1.8	1.4, 2.8
V379/V398	I	1	0.56	NR	0.03, 1.1	1, 2
F382/F401	L	1	0.56	NR	NR	NR
L387/L406	M	1	0.56	NR	0.06, 2.1	1.1, 2.2
H396/H415	P	1	0.56	NR	0.34, 0.87	1.4 to 4.3
H396/H415	R	6	3.39	NR	0.22, 7.3	5.4, 11
S417/S436	Y	1	0.56	NR	NR	1.8
E459/E478	K	1	0.56	NR	NR	NR
F486/F505	S	1	0.56	1.1	0.67	1.4, 9.1

Frequency of BCR-ABL mutations detected in clinical specimens (n = 177). Mutations cluster in 4 distinct regions of the kinase domain. Mutations of the P-loop (amino acids 248-255, green) are most common, followed by mutations of T315 (red), which forms a hydrogen bond with imatinib. M351 (turquoise) interacts with the SH2 domain and participates in autoregulation of kinase activity. The fourth cluster (magenta) encompasses the A-loop (amino acids 379-398).


• P-loop mutations. The P-loop is an extremely flexible, glycine-rich structure encompassing amino acids 244 to 255 that normally accommodates the phosphate groups of ATP. Upon binding of imatinib, the P-loop undergoes a major downward displacement. This "induced fit" interaction with imatinib is stabilized by a water-mediated hydrogen bond between Y253 and N322^ref and the formation of a hydrophobic cage surrounding part of imatinib. Compared with wild-type BCR-ABL, P-loop mutants are 70- to > 100-fold less sensitive in kinase assays and approximately 10-fold less sensitive in cell proliferation assays^ref. In the case of mutant Y253, the main consequence of the mutation may be the disruption of the hydrogen bond to N322^ref. Other P-loop mutations may shift the equilibrium toward an active state by disfavoring the induced fit conformation of the P-loop required for imatinib binding^ref. An additional level of complexity arises from physiologic regulatory mechanisms that are operational within cells. For example, the Y253F mutant of BCR-ABL exhibits increased kinase activity compared with wild type when expressed in cells, but not in in vitro kinase assays using purified ABL, suggesting that this mutation may disrupt the binding of a physiologic ABL inhibitor^ref. For yet-unknown reasons, patients with P-loop mutations appear to have a particularly bad prognosis compared with patients with other types of mutations^ref.
• Mutations of T315. A second cluster of mutations affects T315, which forms a hydrogen bond with imatinib, and much less frequently F317, which binds imatinib via hydrophobic interactions. While the F317L mutant exhibits moderate imatinib resistance, the more frequent T315I mutant is largely insensitive to the drug^{ref1, ref2}. Substitution of threonine with the bulky isoleucine is expected not only to disrupt the hydrogen bond to imatinib but also to allosterically interfere with drug binding. Consistent with this, the insulin receptor kinase, which contains methionine in the position corresponding to T315 in ABL, is resistant to imatinib^ref. Notably, the homologous residue in the PDGFR alpha kinase was found mutated in a patient with hypereosinophilic syndrome, who had developed resistance to imatinib^ref.
• Mutations of M351. The mechanism underlying the resistance of this mutant had not been clear until recently, when the crystal structure of the N-terminal region of ABL was solved and the physiologic regulation of the ABL kinase was revealed^{ref1, ref2}. M351 contacts the ABL SH2 domain, an interaction that helps to stabilize the autoinhibited conformation of ABL. Although BCR-ABL is constitutively active, the mechanisms responsible for autoinhibition of ABL are partially maintained in the chimeric protein. Disruption of the interaction between the SH2 and the KD impairs autoinhibition, shifting the equilibrium toward the active conformation, to which imatinib cannot bind.
• A-loop mutations. The fourth cluster of mutations is localized in the A-loop, which comprises residues 381 to 402 of ABL. As mentioned, the position of the A-loop regulates kinase activity. The 3 residues at the N-terminal form a DFG (aspartate-phenylalanine-glycine) motif that is highly conserved among tyrosine kinases. In its active "open" position, the A-loop swings away from the catalytic center of the kinase, allowing D381 to bind Mg²⁺, which coordinates the phosphate groups of ATP, while the C-terminal part of the A-loop provides a platform for substrate binding. Under physiologic circumstances, (auto-) phosphorylation of Y393 is important for activation, as it stabilizes the open conformation of the A-loop. Consistent with this, ABL phosphorylated on tyrosine 393 is less sensitive to imatinib^{ref1, ref2}. Thus, it is likely that mutations in the A-loop prevent the kinase from adopting its inactive conformation, which is required for imatinib binding. A-loop mutants exhibit moderate resistance in cellular and in vitro kinase assays^{ref1, ref2}
• Mutations in other regions. Apart from the hotspots, mutations have been observed in many other positions in the KD. Some of these mutants have a sensitivity to imatinib that is not significantly different from wild-type BCR-ABL^ref. Thus, it seems unlikely that these mutants are able to confer imatinib resistance in vivo, unless accompanied by yet another mechanism. Consistent with this, some of these mutants (eg, F311L and F359V) have been observed in conjunction with other mutants that exhibit high-level resistance. Importantly, dose escalation of imatinib may be able to recapture responses in patients who harbor mutants with only marginally reduced sensitivity. Many additional KD mutants were recovered from an in vitro mutagenesis screen that used a mutation-prone strain of Escherichia coli^ref, which were frequently located in the C-helix or SH2 and SH3 domain contact sites of the KD. Generally, these mutations confer only moderate resistance and their relevance to clinical resistance is currently unknown. In the same experiment, several mutations outside the KD were also detected. As a rule, they affected amino acids that are critical for autoinhibition of ABL^{ref1, ref2} and exhibit a lower degree of imatinib resistance than KD mutants^ref. It is conceivable that such mutations further impair the residual autoinhibition of ABL within the BCR-ABL fusion protein, shifting the equilibrium to the active state, to which imatinib cannot bind. Information regarding the frequency of these atypical mutations in resistant patients is limited, as most studies sequenced only the KD. One report failed to detect mutations in the ABL SH2 and SH3 domains of 43 patients with clinical resistance to imatinib (Leguay T, Desplat V, Barthe C, et al. Study of mutations in the ATP binding domain and the SH2/SH3 domain of BCR-ABL in 43 chronic myeloid leukemia patients treated by imatinib mesylate (STI571) [abstract]. Blood. 2003;100: 369a)
• Mutations prior to imatinib therapy. In some patients, mutations recovered at relapse were detectable in samples taken prior to imatinib treatment, in one case even at diagnosis^{ref1, ref2, ref3}. This is consistent with the assumption that the selective pressure exerted by imatinib favors the outgrowth of pre-existing resistant cell clones. The failure to consistently detect mutations in imatinibnaive samples from patients who went on to relapse is likely due to the limited sensitivity of the assays used. An intriguing possibility is that the mutations confer some growth advantage regardless of imatinib and are related to disease progression. This would be consistent with the relatively high proportion of mutated alleles (20-40%) that was observed in 3 imatinib-naive patients with myeloid blast crisis^ref. One explanation could be increased kinase activity that has been ascribed to some BCR-ABL mutants (eg, Y253F100 and T315M106), although these data have not yet been confirmed in biochemical assays using full-length protein. It is also conceivable that certain mutants modify the disease by other mechanisms, such as altered downstream signaling. Point mutations of KIT and PDGFR have also been described in patients with imatinib-resistant GISTs (Fletcher JA, Corless C, Dimitrijevic S, et al. Mechanisms of resistance to imatinib mesylate (IM) in advanced gastrointestinal stromal tumor (GIST). [abstract]. Proceedings of ASCO. 2003;22: 815) and hypereosinophilic syndrome, respectively^ref. If point-mutation–induced resistance is typical of imatinib therapy or typical of cancer therapy with tyrosine kinase inhibitors in general remains to be determined. A striking analogy exists to resistance of HIV to protease and reverse transcriptase inhibitors. As with imatinib in CML, disease eradication is extremely difficult, if not impossible, and point mutations that interfere with drug binding are the leading cause of resistance (Brenner BG, Turner D, Wainberg MA. HIV-1 drug resistance: can we overcome? Expert Opin Biol Ther. 2002;2: 751-761)
• clonal evolution. Karyotypic abnormalities in addition to the Ph chromosome have been detected in some in patients at the time of resistance^{ref1, ref2, ref3}. There is no evidence that molecular changes related to specific abnormalities directly confer resistance, as the pattern of clonal evolution (CE) appears to be similar to that seen in patients on IFN therapy^ref. CE was associated with a high risk of disease progression in patients with CHR, suggesting that it should be regarded as a marker of relapse risk rather than a mechanism of resistance, per se^ref
Strategies to overcome resistance : reactivation of BCR-ABL signaling is an almost universal finding in patients with imatinib resistance. This implies that the cells continue to depend on the specific signaling output of the genetic event that initiated the malignant transformation in the first place, and that BCR-ABL remains the best therapeutic target^ref.
• dose escalation of imatinib : retrospective data suggest that dose escalation can overcome hematologic or cytogenetic resistance in some patients^ref, although these responses may not be maintained^ref. An important consideration is the specific type of mutation. Dose escalation is likely to be effective in the case of mutants with a low or moderate level of resistance to imatinib, such as H386P, but not in highly resistant mutants such as T315I or E255K^ref
• combination with conventional cytotoxic drugs : many drugs have been tested for synergism with imatinib (recently reviewed in La Rosee et al^ref). The use of different cell lines and different models of data analysis may explain why the results are not always consistent among the various studies. Altogether, it appears that most combinations are synergistic or at least additive. Since one of the pillars of BCR-ABL–mediated malignant transformation is inhibition of apoptosis^ref, this is consistent with the concept that inhibition of BCR-ABL function resensitizes the cells to the induction of apoptosis by conventional agents. Naturally, drugs with established activity in CML have attracted particular attention. Cytarabine, homoharringtonine, and IFN are synergistic in vitro, and combinations with imatinib are currently tested in clinical trials. Promising results have also been obtained for decitabine, a novel hypomethylating agent with activity in CML blast crisis^ref. In contrast, the data are conflicting for hydroxyurea^{ref1, ref2, ref3}, while methotrexate and topotecan are antagonistic in combination with imatinib. Given the requirement for many dose points, drug combination assessments are difficult to perform in primary cells. Thus, most of the data are based on cell lines, although in a strict sense, any combination would have to be tested in primary cells to confirm that the differential between CML and normal cells afforded by imatinib is maintained.
• alternative inhibitors of ABL : several compounds with inhibitory activity toward ABL kinase at nanomolar concentrations have been identified. Compared with imatinib, these compounds are less specific and have activity against SRC family kinases as well as various other targets. The crystal structure of the ABL KD in complex with the pyridopyrimidines PD173955 and PD180970 has been solved and revealed striking differences compared with imatinib^{ref1, ref2}

		IC50 cell proliferation, nM
compound	class	wild-type BCR-ABL	E255K	M351T	H396P	T3151	reference
PD180970	Pyridopyrimidine	25	140	45	15	840	ref
SKI DV-M016	Pyridopyrimidine	11	30	NR	10	> 500	ref
AP23848	Trisubstituted purine	14	94	24	8	9050	ref
BMS-354825	2-amino-thiazole-5-carboxamide	0.087-1.000	low nM range	low nM range	low nM range	> 1000	ref (Lee FY, Lombardo L, Borzilleri R, et al. BMS-354825 - a potent SRC/ABL kinase inhibitor possessing curative efficacy against imatinib sensitive and resistant human CML models in vivo [abstract]. AACR meeting 2004. 2004)

In contrast to imatinib, PD173955 is capable of binding to both inactive and active ABL conformations, regardless of the position of the A-loop. Given the structural similarity of active tyrosine kinases, it is not surprising that this is associated with some loss of specificity. One advantage of these potent ABL inhibitors over imatinib may be that the IC₅₀ and IC₉₀ values for inhibition of kinase activity and cellular proliferation of BCR-ABL–transformed cells are lower by 1 to 2 orders of magnitude. Thus, more complete inhibition of BCR-ABL tyrosine phosphorylation should be achievable in patients. Since there is evidence that higher doses of imatinib are superior to lower doses^{ref1, ref2, ref3}, stronger suppression of BCR-ABL kinase activity might lead to a more profound suppression of the leukemic clone. An even more important feature is the activity of alternative ABL inhibitors against imatinib-resistant mutants of BCR-ABL. One study showed that PD180970 inhibited the kinase activity of most clinically relevant BCR-ABL mutants, with the exception of T315I, with IC₅₀ values equal or only slightly higher than for wild-type ABL, and suppressed cell proliferation of BaF3 cells expressing the various mutants^ref. These results were subsequently confirmed^{ref1, ref2}. Unfortunately, the unfavorable pharmacokinetic profile of pyridopyrimidines precludes their clinical development. Another group of compounds with potent inhibitory activity toward SRC- and KD-mutant ABL are trisubstituted purines^ref. The most active derivative, AP23464, inhibits the proliferation of BaF3 cells expressing wild-type BCR-ABL with an IC₅₀ of 14 nM. BCR-ABL mutants except T315I and, to a lesser extent E255K, are inhibited at comparable concentrations. The pharmacologic properties of this class of compounds are not yet known. The most promising of the alternative ABL inhibitors is BMS-354825, which has a similar spectrum of activity against wild-type and mutant BCR-ABL and high oral bioavailability. Excellent responses were seen in severe combined immunodeficient (SCID) mice injected with BaF3 cells expressing wild-type or M351T mutant but not T315I mutant BCR-ABL^ref. A phase 1 study in patients with imatinib resistance is currently in progress. The fact that BMS-354825 and similar compounds inhibit SRC may be an advantage, as SRC kinases may be activated in rare patients with imatinib resistance^ref and play a role in signal transduction downstream of BCR-ABL.125-127 The disadvantage of anti-SRC activity may be an increased rate of side effects^ref
• agents that down-regulate BCR-ABL protein : geldanamycin and its less-toxic analog 17-AAG (17-allylaminogeldanamycin) lead to degradation of BCR-ABL protein by inhibiting Hsp90, a molecular chaperone required for stabilization of BCR-ABL^{ref1, ref2, ref3, ref4}. A recent study showed that BCR-ABL proteins with E255K and T315I mutations may be even more sensitive to 17-AAG than wild-type BCR-ABL^ref. Phase 1 studies with 17-AAG are in progress. The histone deacetylase inhibitor LAQ824 exerts similar effects as 17-AAG by acetylation of Hsp90, which in turn interferes with the protein's chaperone function^ref. In addition, this compound down-regulates BCR-ABL mRNA by an as-yet-unknown mechanism. Lastly, arsenic trioxide has been shown to induce down-regulation of BCR-ABL, although the precise mechanism is not known^{ref1, ref2, ref3}. In a small phase 1 study, the combination of imatinib and arsenic trioxide was well tolerated but no therapeutic activity was observed. This may be due to the fact that the imatinib dose had been reduced at study entry because of concerns about toxicity^ref.

combinations with other signal transduction inhibitors : extensive in vitro studies have tested specific inhibitors of signal transduction pathways downstream of BCR-ABL alone and in combination with imatinib. In most cases, synergistic or additive effects were demonstrable, in some instances also in imatinib-resistant cell lines. Several compounds, including farnesyl transferase inhibitors (FTIs), mammalian target of rapamycin (mTOR) inhibitors (rapamycin, RAD001), and flavopiridol, an inhibitor of cyclin-dependent kinases, are in early clinical development, alone or in combination with imatinib (Table 6). Although there is a rationale for these agents, BCR-ABL itself remains the best target, as resistance to imatinib is almost universally associated with reactivation of BCR-ABL kinase activity, and it is doubtful whether disrupting individual pathways downstream of BCR-ABL will be effective. Studies in mice with homozygous deletions of IL-3, GM-SCF^ref, or STAT5^ref revealed that BCR-ABL remained fully leukemogenic, indicating that targeting one of these pathways would not be sufficient. Another important lesson from preclinical studies is that synergism between imatinib and other agents depends on residual sensitivity of the leukemic cells to imatinib^ref. Thus, combinations of imatinib with decitabine, arsenic trioxide, or FTIs are synergistic in resistant cell lines with overexpression of BCR-ABL but not in lines expressing the T315I mutant^{ref1, ref2, ref3}. This emphasizes the need to establish the mechanism of resistance to allow for a rational choice of salvage therapy.

target	compound	activity in imatinib-resistant cells	clinical trials	reference
farnesyl transferase	lonafarnib, tipifamib	yes	yes	ref1, ref2 (Gotlib J, Mauro MJ, O'Dwyer ME, et al. Tipifarnib (ZARNESTRA) and imatinib (GLEEVEC) combination therapy in patients with advanced chronic myelogenous leukemia (CML): preliminary results of a phase I study [abstract]. Blood. 2003;102: 909; Cortes J, O'Brien S, Ferrajoli A et al. Phase I study of a imatinib and lonafarnib (SCH66336) in patients (pts) with chronic myeloid leukemia (CML) refractory to imatinib mesylate [abstract]. Blood. 2003;102: 909a)
MEK1	PD98059	yes	yes	ref
RAF-1	BAY43-9006	yes	yes	Choi YJ, Qing W, White S, et al. Imatinib-resistant cell lines are sensitive to the Raf inhibitor BAY 43-9006 [abstract]. Blood. 2002;100: 369
PI3 kinase	LY294002 Wortmannin	yes	no	ref
mTOR	rapamycin	yes	yes	ref1, ref2
cyclin-dependent kinases	flavopiridol	yes	yes	ref

Disease persistence : there is a strong correlation between disease phase and the incidence of refractoriness at the hematologic, cytogenetic, and molecular levels. It is evident that only a small fraction even of newly diagnosed patients achieve "molecular remission" (ie, become negative for BCR-ABL by RT-PCR)^ref. Even in those individuals, more sensitive tests revealed that the underlying disease burden is greater than in patients who become RT-PCR negative after an allogeneic transplantation, where molecular remission is associated with long-term freedom from progression^ref. It is at present unclear which mechanisms underlie the persistence of BCR-ABL⁺ cells and whether these mechanisms are similar to those responsible for acquired resistance. In vitro studies suggest that the primary effect of imatinib on BCR-ABL⁺ primitive progenitor cells is inhibition of proliferation, without induction of apoptosis^{ref1, ref2}. Hence, imatinib may be able to prevent stem cell proliferation but unable to eliminate "quiescent" cells, even if combined with other agents such as FTIs, cytarabine, PI3 kinase inhibitors, or Hsp90 inhibitors (Holyoake T, Allan EK, Grand F, et al. Combination therapies including imatinib do not eradicate quiescent chronic myeloid leukaemia stem cells in vitro [abstract]. Blood. 2003;102: 71a). It is unknown though whether the quiescent cells in these ex vivo assays correspond to the cells that persist in vivo. Several mechanisms might allow primitive progenitor cells to survive in the presence of imatinib (Figure 8). One explanation is that survival of persisting leukemia cells is dependent on physiological stimuli, rather than on BCR-ABL kinase activity. Circumstantial evidence for this comes from the observation that CD34+-selected CML cells treated in vitro with imatinib activate mitogen-activated protein kinase in a growth-factor–dependent manner, suggesting that they are capable of switching to an alternative survival and growth signal upon BCR-ABL inactivation^ref. Survival signals could also be derived from interaction with stroma cells and extracellular matrix. Studies in BCR-ABL⁺ cell lines treated with imatinib in combination with cytotoxic agents suggest that adhesion to integrins inhibits apoptosis, even in the absence of active BCR-ABL kinase^ref, although it remains to be seen whether these findings are relevant to primary CML cells. A second possibility is that imatinib is not able to completely inhibit BCR-ABL kinase activity, and that the residual activity is sufficient to promote survival but not proliferation. As discussed earlier, data from several groups indicate that imatinib is a substrate of PGP, and high levels of PGP in leukemic stem cells may efficiently reduce intracellular drug levels. If this is the case, then higher doses of imatinib should be more effective, which is in agreement with higher rates of RT-PCR negativity seen in chronic-phase patients treated with 800 mg rather than 400 mg imatinib daily^ref. Similarly, ABL inhibitors with greater potency may be able to improve the rates of molecular response by completely inhibiting BCR-ABL. Another mechanism for persistence is mutations in the BCR-ABL KD. A high rate of "unusual" KD mutations was recently reported in a small series of patient in CCR (Chu S, Snyder DS, Sawyers C, Forman SJ, Bhatia R. Detection of BCR/ABL kinase domain mutations in chronic myelogenous leukemia patients in complete cytogenetic remission on imatinib treatment [abstract]. Blood. 2003;102: 70a). In most instances, the specific mutations had been detected in the aforementioned in vitro mutagenesis screen^ref and are predicted to confer only low to moderate resistance. This would explain why these patients achieve CCR but fail to eradicate the disease, and would provide a rationale for therapy with alternative ABL inhibitors. Furthermore, a recent study showed that the levels of BCR-ABL mRNA in early hematopoietic progenitors from CML patients were much higher than in more mature cells, which may render such cells resistant to imatinib (Jiang X, Zhao Y, Chan P, Eaves A, Eaves C. Quantitative real-time RT-PCR analysis shows BCR-ABL expression progressively decreases as primitive leukemic cells from patients with chronic myeloid leukemia (CML) differentiate in vivo. Exp Hematol. 2003;31: 228-229)

Potential mechanisms underlying disease persistence (molecular refractoriness). (A) Kinase domain mutations that confer moderate resistance to imatinib. (B) BCR-ABL levels may be particularly high in the most primitive leukemic stem cells. (C) Inadequate intracellular levels of imatinib as a result of PGP expression. (D) Physiologic growth factor signaling or (E) integrin signals may maintain viability even with BCR-ABL kinase activity completely inhibited. (F) Quiescent (dormant) cells may be protected against imatinib. VLA-5 indicates very late activation antigen-5.
Future directions :
• imatinib and allogeneic HSCT : one of the biggest challenges in the management of CML is the integration of imatinib therapy and allogeneic HSCT. There appears to be consensus that patients who progressed beyond chronic phase should proceed to an allograft, if this is feasible, using imatinib as an induction therapy with low toxicity. In newly diagnosed patients in chronic phase, one option is to start all patients on imatinib, reserving allografting for those without adequate response. The value of this approach will ultimately depend on whether imatinib compromises the outcome of a subsequent allograft. Retrospective analyses, predominantly of high-risk patients, have yielded conflicting results, and the issue needs to be clarified prospectively (Deininger MWN, Schleuning M, Sayer HG, et al. Allografting after imatinib therapy: no evidence for increased transplant-related mortality and favorable results in patients transplanted in remission. A retrospective study by the EBMT [abstract]. Blood. 2002;100: 783a; Zander A, Zabelina T, Renges H, et al. Pretreatment with Glivec increases transplant-related mortality in afetr allogeneic transplant [abstract]. Blood. 2003;102: 468a) The other option is to define a group of patients with high-risk disease and a low risk of transplantation-related mortality, in whom allografting is performed as soon as possible, regardless of their response to imatinib. Given the relatively short follow-up of patients on imatinib, it is presently impossible to provide an unequivocal rationale for either approach. Under these circumstances, the patient's individual preference is a crucial factor in finding the optimal course of action.
• predicting response to imatinib : obviously, therapeutic decisions would be greatly facilitated if it were possible to accurately predict cytogenetic or molecular response prior to imatinib therapy. Although several baseline factors predictive of subsequent MCR have been identified, these variables are of little use for decision-making in individual patients^ref. Classification according to the Sokal score defines 3 distinct risk groups (Cervantes F. Durability of responses to imatinib in newly diagnosed chronic phase chronic myelogenous leukemia (CML): 24-moths update from the IRIS study [abstract]. Blood. 2003;102: 181) but other factors must be taken into account. For example, patients with deletions flanking the ABL or BCR breakpoint have lower rates of CCR and a shorter time to progression^ref. Given the success of gene profiling by microarray for prediction of treatment outcomes, several groups have used this technology to define expression signatures associated with MCR. In one study of 18 CML patients, most of them in chronic phase, 79 genes were identified with differential expression between peripheral blood mononuclear cells from cytogenetic responders and nonresponders^ref. In another study of newly diagnosed patients, mRNA isolated from unselected blood cells was used for expression profiling^ref. Again, a number of differentially expressed genes were identified. Unfortunately, since these results were not validated in independent cohorts, their significance is unclear. In our own experience, the differences in the gene expression profiles of white cells from responders and nonresponders are very small and may not predict cytogenetic response (Deininger MW, Mori M, Hsieh Y-C, et al. Gene expression profiling of total white cells may not predict complete cytogenetic response to imatinib in patients with chronic myelogenous leukemia [abstract]. Blood. 2003;102: 418a). In contrast, microarrays or quantitative PCR on rationally chosen candidate genes were successfully used to predict hematological response to imatinib in patients with Ph⁺ ALL^ref or myeloid blast crisis of CML^ref
• unexpected late side effects : another issue affecting therapeutic decisions is late side effects. Generally, imatinib is well tolerated, particularly in newly diagnosed patients, where most adverse events are grade 1 or 2. However, some side effects may become apparent only with longer follow-up. For example, gynecomastia and low testosterone levels are frequent in men treated with imatinib^ref. In addition, reduced sperm counts were observed in preclinical studies in dogs and monkeys^ref. Only limited data are available regarding the fertility of men treated with imatinib. A total of 18 pregnancies in partners of men taking imatinib had been reported to Novartis by spring 2003. At this time, 6 pregnancies were ongoing and 4 had no or limited information. Among the remaining 8, there were 4 healthy infants, 2 therapeutic abortions (on social grounds), 1 spontaneous abortion, and 1 death in utero. Imatinib is teratogenic in rats, and thus women are advised not to conceive while on treatment. Nonetheless, 26 pregnancies have been reported to Novartis. Eleven patients elected to have therapeutic abortions, 5 had spontaneous abortions, and 7 pregnancies were either ongoing or without sufficient information at the time of last follow-up. Only 3 infants had been carried to term, 2 of which were healthy, while 1 had a hypospadia. Given these very limited data, it is currently impossible to exclude even a major teratogenic effect in humans, and women of childbearing age should not conceive while on imatinib. For long-term therapy of younger women, this is evidently an important issue. If a pregnancy does occur, decisions must be individualized, until more data have been acquired^ref. A recent study at Novartis showed an increased frequency of genitourinary tumors in rats treated with 30 to 60 mg/kg imatinib daily for 24 months (G. R. Paul, Novartis Pharma, unpublished data, September 2004). A preliminary analysis of the safety data from clinical trials and spontaneous adverse event reports did not show evidence of an increased overall incidence of malignancies nor a specific increase in the incidence of bladder, kidney, or prostate tumors in patients treated with imatinib compared with that of the general population, but watchful monitoring of patients on imatinib seems nonetheless advisable. Another concern is chromosomal abnormalities in the Ph– cells of patients with an MCR, in some cases associated with a myelodysplastic syndrome.166 This finding may be an indication that the hematopoiesis of some CML patients has sustained genetic damage in addition to the Philadelphia translocation, for example, as a result of prior cytotoxic chemotherapy. For adequate counseling, it will be important to determine the prognosis of such patients.
• unexpected beneficial effects : normalization of hypercholesterolemia and hypertriglyceridemia^ref
Conclusion : imatinib is proof of principle that rationally designed, molecularly targeted therapy works. The clinical trials in CML, where imatinib produced an unprecedented rate of hematologic and cytogenetic remissions, confirm the essential role of the BCR-ABL tyrosine kinase. Equally important, though not the subject of this review, is the efficacy of imatinib in GISTs, chronic myelomonocytic leukemia with rearrangements of PDGFR, and the hypereosinophilic syndrome, all diseases where the activation of an imatinib-sensitive kinase is central to the pathogenesis^{ref1, ref2, ref3}. Imatinib represents a paradigm shift in cancer drug development. It is hoped that this will pave the way for a new generation of specific, targeted therapies for the many malignant conditions for which no efficient drug therapy is currently available.
Monitoring BCR-ABL levels in patients treated for CML has become an integral part of patient management. Real-time reverse transcriptase-polymerase chain reaction is the method of choice for this purpose because of its high analytical sensitivity and reproducibility. Given the variation of RNA quality and quantity in clinical specimens, accurate quantitative assessment of BCR-ABL depends on normalization of the BCR-ABL signal to an appropriate internal reference. However, the controls used by different laboratories vary, and there is no clear consensus on an ideal reference due to limited investigations. 9 commonly used control genes were compared for 3 criteria: mRNA abundance, levels in CML and non-CML cells, and their degradation kinetics in comparison with BCR-ABL. ß-glucuronidase (GUSB) is the most suitable among the 9 genes tested. Although ABL is most widely used, the amount of ABL is different in CML and non-CML cells. Moreover, ABL levels are regulated by cellular stress^ref.
Side effects :

	very common (> 1/10)	common (> 1/100, < 1/10)	not common (> 1/1000, < 1/100)	rare (< 1/1000)
infections			sepsis, pneumonia, herpes simplex, herpes zoster, URTI, gastroenteritis
blood	neutropenia (overcome by G-CSFref, but not alwaysref), thrombocytopenia, anemia	febrile neutropenia	pancytopenia
nutrition		anorexia	dehydration, hyperuricemia, hypokalemia, hyperphagia, anorexia, gout, hypophosphatemia	hyperkalemia, hyponatremia
psychiatric			depression, anxiety, reduction of libido	confusion
nervous system	headache	vertigo, parageusia, paresthesias, insomnia	cerebral hemorrhage, syncope, peripheral neuropathy, hypoesthesia, sleepiness, migraine, memory disorders	cerebral edema, intracranial hypertension, seizures
ocular disorders		conjunctivitis, lachrymation, blurred vision	ocular irritation, conjunctival hemorrhage, preorbital edema	macular edema, papilledema, retinal and vitreal hemorrhage, glaucoma
uditive and vestibular apparatus			vertigo, tinnitus
cardiac			heart failure, pulmonary edema, tachycardia	pericardial effusion, pericarditis
vascular			hematoma, systemic arterial hypotension and hypertension, flushing, cold extremities	thrombosis and embolism
respiratory, chest and mediastinum		epistaxis, dyspnea	pleural effusion, cough, pharyngolaryngeal pain	pulmonary fibrosis, interstitial pneumonia
gastrointestinal apparatus	nausea, vomiting, diarrhea, dyspepsia, abdominal pain	abdominal distention, flatulence, constipation, gastroesophageal reflux, mouth ulcers	gastrointestinal hemorrhage, melena, ascitis, gastric ulcer, gastritis, eruttation, xerostomia	colitis, acute intestinal occlusion, pancreatitis
hepatobiliary system		transaminitis	jaundice, hepatitis, hyperbilirubinemia	liver failure
skin and adnexa	periorbital edema, dermatitis/eczema/skin eruption	facial edema, palpebral edema, pruritis, erythema, dry skin, alopecia, night sweats	petechias, contusions, diaphoresis, urticaria, onychoclastia, photosensitivity, purpura, hypotrichosis, cheilitis, hyperpigmentation, psoriasis, esfoliative dermatitis, bullous eruptions	angioedema, vesicular rash, Stevens-Johnson syndrome
musculo-skeletal, connective and bone disorders	muscular cramps, musculo-skeletal and arthralgia	swollen joints	sciatica, joint and muscle stiffness
urinary			renal failure, nephralgia, pollakiuria and hematuria
reproductive			gynecomastia, mammary tenderness, scrotal edema, nipple pain, menorrhage, sexual disorders
systemic or local	fluid retention and edema, fatigue	pyrexia, malaise, chill	malaise, hemorrhage	anasarca, tumor hemorrhage or necrosis
research		weight gain	increase in serum alkaline phosphatase, creatinine, CPK, LDH, weight loss,

• hypophosphatemia (1,25-dihydroxyvitamin D levels in the upper normal range and PTH levels elevated) due to secondary hyperparathyroidism within a few weeks at high doses (600 mg/day), with associated changes in bone and mineral metabolism; the drug may inhibit bone remodeling (formation and resorption), even in patients with normal serum phosphate levels^ref. Hypophosphatemia has also been observed in patients with renal cancer taking sunitinib


• rapid reduction in cholesterol levels (8 out of 9 patients) and decrease in triglyceride levels (3 out of 4 patients)^ref. Since PDGF binds and phosphorylates the LRP, a member of the LDL receptor superfamily^ref, the authors postulate that inhibition of the PDGF receptor may modify the metabolism of lipids
• in patients with solid tumours selective kinase inhibition with daily imatinib intensifies toxicity of chemotherapy^ref. In patients with extensive-disease SCLC, the maximum tolerated dose for imatinib + cisplatin/irinotecan with G-CSF support was identified as imatinib at a dose of 300 mg/day with irinotecan (at a dose of 65 mg/m²) and cisplatin (at a dose of 30 mg/m²) given on days 1 and 8, every 21 days. The decreased irinotecan clearance may explain the high incidence of diarrhea and neutropenia noted in the current study^ref.
Dose adjustements :
• CP-CML and GIST (starting dose 400 mg/day or 260 mg/m² in babies) : if ANC < 1,000/ml and/or PLT < 50,000/ml : discontinue imatinib until ANC > 1,500/ml and PLT > 75,000/ml, then restart at 400 mg/day (260 mg/m² in babies). If ANC < 1,000/ml and/or PLT < 50,000/ml occurs again, discontinue as above and restart at 300 mg/day
• AP-CML  and BC-CML (starting dose 600 mg/day) : if ANC < 500/ml and/or PLT < 10,000/ml and therapy begun since > 1 month : check if cytopenia is CML-related with BMTB or BMAB : if not, reduce dose down to 400 mg/day (260 mg/m² in babies). If persists for 2 weeks, reduce down to 300 mg/day (200 mg/m² in babies). If persists for 4 weeks and continues to be not leukemia-related, discontinue imatinib until ANC > 1,000/ml and PLT > 20,000/ml, then restart treatment at 300 mg/day (200 mg/m² in babies)
• dasatinib / BMS-354825 (Sprycel^©; source : Bristol-Myers Squibb) is a dual SRC/ABL kinase inhibitor that binds ABL in both the active and inactive conformation differs from imatinib in that it can bind to both the active and inactive conformations of the ABL kinase domain ^{ref1, ref2} (Tokarski J, Newitt J, Lee F, et al. The crystal structure of Abl kinase with BMS-354825, a dual SRC/ABL kinase inhibitor. Blood 2004;104:160a-160a). Dasatinib also inhibits a distinct spectrum of kinases that overlaps with the array of kinases that imatinib inhibits (ABL, KIT, and EGFR)^ref. Since it has less stringent binding requirements than does imatinib, dasatinib has activity against many imatinib-resistant kinase domain mutations of BCR-ABL. In cell-line models, dasatinib inhibited 18 of 19 imatinib-resistant BCR-ABL mutations within a narrow concentration range, similar to that required to block wild-type BCR-ABL^{ref1, ref2}. The only exception is a single mutation deep within the ATP-binding pocket of the ABL tyrosine kinase (T315I) that confers a high degree of resistance to imatinib and dasatinib and to the imatinib analogue AMN-107^ref, presumably as a result of steric hindrance caused by replacement of threonine with the bulkier isoleucine residue : T315I is responsible for around 20% of all drug-resistant CML cases^{ref1, ref2, ref3}. It induces a 86% (n 36 pts) remission rate in the 12% of patients unresponsive to STI 571 by 40 months. In a phase 1 dose-escalation study, dasatinib (15 to 240 mg per day) was administered orally in 4-week treatment cycles, once or twice daily, a complete hematologic response was achieved in 37 of 40 patients with chronic-phase CML, and major hematologic responses were seen in 31 of 44 patients with accelerated-phase CML, CML with blast crisis, or Ph⁺ ALL. In these 2 phases, the rates of major cytogenetic response were 45% and 25%, respectively. Responses were maintained in 95% of patients with chronic-phase disease and in 82% of patients with accelerated-phase disease, with a median follow-up > 12 months and 5 months, respectively. Nearly all patients with lymphoid blast crisis and Ph⁺ ALL had a relapse within 6 months. Responses occurred among all BCR-ABL genotypes, with the exception of the T315I mutation, which confers resistance to both dasatinib and imatinib in vitro. Myelosuppression was common but not dose-limiting^ref.


Side effects : panniculitis in 2 imatinib-resistant CML females^ref. In the phase 1 study, 10 patients underwent thoracentesis and 2 underwent pleurodesis because of pleural effusion. Of the 10 patients, 4 had chronic-phase CML and 6 were in blast crisis. All 10 patients received dasatinib twice daily at total daily doses ranging from 50 to 240 mg. The rate of drug-related pleural effusion was 21% in a series of 5 phase 2 studies involving a total of 511 patients with chronic phase, accelerated phase, blast crisis, or Philadelphia chromosome–positive acute lymphoid leukemia. Full details of these studies have not yet been reported, but 28% of the patients had pleural effusions while receiving dasatinib at doses of less than 140 mg per day, with treatment administered twice daily. A randomized study now under way comparing once- with twice-daily treatment with dasatinib at a dose of 100 or 140 mg daily could determine whether the dose of this agent and the schedule affect the incidence of pleural effusion^ref
• nilotinib / AMN107 (Tasigna^®, source : Novartis) 400-mg twice daily, dubbed "super Glivec^©" (Weisberg E, Manley PW, Breitenstein W, et al. Characterization of AMN107, a selective inhibitor of native and mutant Bcr-Abl. Cancer Cell 2005;7:129-4; Manley P, von Bubnoff N, Duyster J, et al. AMN107: inhibitory profile against wild-type and mutant forms of the BCR-ABL tyrosine kinase. Presented at the 96th annual meeting of the American Association for Cancer Research, Anaheim, Calif., April 16–20, 2005). Like imatinib, nilotinib functions through competitive inhibition at the ATP-binding site of BCR-ABL, leading to the inhibition of tyrosine phosphorylation of proteins that are involved in the intracellular signal transduction that BCR-ABL mediates. Nilotinib has a higher binding affinity and selectivity for the ABL kinase than does imatinib. It also has 20 to 50 times the inhibitory activity of imatinib in imatinib-sensitive CML cell lines and 3 to 7 times the activity in imatinib-resistant cell lines. Nilotinib was also active in 32 of 33 imatinib-resistant cell lines with mutant ABL kinases^{ref1, ref2, ref3} ; serum half-life of 15 hours. It induces a 50% remission rate in CML and ALL pts. In contrast to imatinib mesylate, resistance to nilotinib was associated with a limited spectrum of Bcr-Abl kinase mutations. Among these were mutations affecting the P-loop and T315I. Rarely emerging resistant colonies at a concentration of 400 nM nilotinib exclusively expressed the T315I mutation. With the exception of T315I, all of the mutations that were identified were effectively suppressed when the nilotinib concentration was increased to 2000 nM, which falls within the peak - trough range in plasma levels (3.6-1.7 µM) measured in patients treated with 400 mg bid. Nilotinib might be superior to imatinib in terms of the development of resistance. However, clinical resistance to nilotinib may be associated with the predominant emergence of T315I^ref. In a phase 1 dose-escalation study, 119 patients with imatinib-resistant CML or acute lymphoblastic leukemia (ALL) received nilotinib orally at doses of 50 mg, 100 mg, 200 mg, 400 mg, 600 mg, 800 mg, and 1200 mg once daily and at 400 mg and 600 mg twice daily. No dose-limiting toxic effects were seen at doses of up to 600 mg daily. Common adverse events were myelosuppression, transient indirect hyperbilirubinemia, and rashes. Of 33 patients with the blastic phase of disease, 13 (39%) had a hematologic response and 9 (27%) had a cytogenetic response; of 46 patients with the accelerated phase, 33 (76%) had a hematologic response and 22 (55%) had a cytogenetic response. The rate of complete hematologic response in patients with chronic-phase CML was 92%, and the rate of complete cytogenetic response was 35%^ref
• ON012380 does not compete with ATP for binding BCR-ABL but, rather, competes with its substrates and works synergistically with imatinib in wild-type BCR-ABL inhibition. More importantly, ON012380 was found to induce apoptosis of all of the known imatinib-resistant mutants at concentrations of <10 nM concentration in vitro and cause regression of leukemias induced by i.v. injection of 32Dcl3 cells expressing the imatinib-resistant BCR-ABL isoform T315I. Daily i.v. dosing for up to 3 weeks with a >100 mg/kg concentration of this agent is well tolerated in rodents, without any hematotoxicity^ref


• SKI-606


• PD166326^ref
• allosteric non-ATP competitive mechanism
• GNF-2^ref


• dual Bcr-Abl/Lyn tyrosine kinase inhibitor :
• NS-187^ref / INNO-406 is 25-55 times more potent than imatinib in vitro and at least 10 times more potent in vivo. INNO-406, like imatinib, is a substrate for P-glycoprotein. The concentrations of INNO-406 in the CNS were about 10% of those in the plasma. However, this residual concentration was enough to inhibit the growth of Ph⁺ leukemic cells which expressed not only wild type but also mutated BCR-ABL in the murine CNS. Furthermore, cyclosporine A, a P-glycoprotein inhibitor, augmented the in vivo activity of INNO-406 against CNS Ph⁺ leukemia^ref
Combination therapies : N-ethyl-N-nitrosourea (ENU)-exposed Ba/F3-p210^BCR-ABL cells were used to compare incidence and types of kinase domain mutants emerging in the presence of imatinib, dasatinib and nilotinib, alone and in dual combinations. Although ENU is expected to induce mutations in multiple proteins, resistant clones were almost exclusively BCR-ABL KD mutant at relevant concentrations of nilotinib and dasatinib, consistent with a central role of KD mutations for resistance to these drugs. 20 different mutations were identified with imatinib, 10 with nilotinib (including only one novel mutation, E292V), and 9 with dasatinib. At intermediate drug levels the spectrum narrowed to F317V and T315I for dasatinib and Y253H, E255V, and T315I for nilotinib. Thus, cross resistance is limited to T315I, which is also the only mutant isolated at drug concentrations equivalent to maximal achievable plasma trough levels. With drug combinations maximal suppression of resistant clone outgrowth was achieved at lower concentrations compared to single agents, suggesting that such combinations may be equipotent to higher dose single agents. However, sequencing uniformly revealed T315I, consistent with the need for a T315I inhibitor to completely block resistance^ref
• CD117 / c-kit inhibitors : therapy of chronic myelogenous leukemia (CML), gastrointestinal stromal tumours (GIST). It has no major effect against adenoid cystic carcinoma of the salivary glands, which overexpress c-Kit^ref, and malignant endocrine tumors^ref. A 4 compartment model, based on the known biology of haematopoietic differentiation, can explain the kinetics of the molecular response to imatinib in a 169-patient data set. Successful therapy leads to a biphasic exponential decline of leukaemic cells. The first slope of 0.05 per day represents the turnover rate of differentiated leukaemic cells, while the second slope of 0.008 per day represents the turnover rate of leukaemic progenitors. The model suggests that imatinib is a potent inhibitor of the production of differentiated leukaemic cells, but does not deplete leukaemic stem cells. The probability of developing imatinib resistance mutations has been calculated and the time until detection of resistance has been estimated. The model provides the first quantitative insights into the in vivo kinetics of a human cancer thanks to the precise understanding of how imatinib exerts its therapeutic effect in CML and the ability to measure disease burden by quantitative PCR^ref.
• PDGF-R inhibitors : imatinib; therapy of all the chronic myeloproliferative syndromes and dermatofibrosarcoma protuberans
• FLT-3 inihibitors : resistant human cell lines created through prolonged co-culture with FLT3 TKIs and primary samples still exhibit inhibition of FLT3 phosphorylation upon FLT3 TKI treatment. However, FLT3 TKI resistant cell lines and primary samples often show continued activation of downstream PI3K/Akt and/or Ras/MEK/MAPK signaling pathways as well as continued expression of genes involved in FLT3-mediated cellular transformation. Inhibition of these signaling pathways restores partial sensitivity to FLT3 TKIs. Mutational screening of FLT3 TKI resistant cell lines revealed activating N-Ras mutations in 2 cell lines that were not present in the parental FLT3 TKI sensitive cell line. Taken together, these data indicate that FLT3 TKI resistant cells most frequently become FLT3 independent due to activation of parallel signaling pathways that provide compensatory survival/proliferation signals when FLT3 is inhibited. Anti-FLT3 mAb treatment was still cytotoxic to FLT3 TKI resistant clones. An approach combining FLT3 TKIs with anti-FLT3 antibodies and/or inhibitors of important pathways downstream of FLT3 may reduce the chances of developing resistance^ref
• M-CSF-R / c-fms inhibitors : imatinib^ref
• IGF-1R inhibitors
• adaphostin / NSC 680410
• AG 957
• PKB / AKT inhibitors^ref : in 33-50% of all cancers, such studies have revealed mutations in AKT or in the Akt regulatory proteins phosphatidylinositol 3-kinase (PI3K) and phosphatase and tensin homologue (PTEN). A recent report by Yoeli-Lerner et al.^ref, however, raises concern. Even though the inhibition of Akt should foil local tumor growth, it could promote invasion and metastasis in certain settings. The first evidence of a potential antimetastatic function of Akt was provided by a transgenic mouse model of breast cancer, as described by Hutchinson et al^ref. As expected, in mice with tumors that overexpress HER2/neu, larger primary tumors developed in the setting of ramped-up Akt activity, yet the mice had relatively fewer metastatic lesions. Yoeli-Lerner et al. confirmed the antimetastatic action of Akt in several breast-cancer cell lines and elucidated a potential mechanism involving the NFAT. The model implicates NFAT as a master switch that controls the expression of a set of genes that promotes invasion. Akt normally holds NFAT in check by promoting its destruction in the proteosome, thereby suppressing invasion and metastasis. Akt inhibition allows NFAT to escape destruction, translocate to the nucleus, and activate a gene-expression program that leads to metastasis. Although the yin–yang biology of Akt suggested by Yoeli-Lerner et al. is unexpected, it is not without precedent. The TGF-b–receptor pathway restrains the development of tumors in normal epithelium, yet inhibitors of the pathway block tumor growth in models of late-stage cancer^ref. In a similar way, an inhibitor of a kinase called the mammalian target of rapamycin (mTOR) blocks Akt-dependent tumor growth in mouse models but can stimulate Akt kinase activity^{ref1, ref2}
• KRX-0401 (perifosine)
• VEGFR and HGFR / MET inhibitors : XL880 (source : Exelixis, Inc) : PDGFR, RON, c-KIT, FLT3, and Tie-2 are also inhibited.

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