双重SRC/ABL激酶抑制剂达沙替尼和热休克蛋白90抑制剂IPI-504对胃肠道间质瘤相关的血小板衍生生长因子受体A D842V突变的活性。

Activity of dasatinib, a dual SRC/ABL kinase inhibitor, and IPI-504, a heat shock protein 90 inhibitor, against gastrointestinal stromal tumor-associated PDGFRAD842V mutation.

作者信息

Dewaele Barbara, Wasag Bartosz, Cools Jan, Sciot Raf, Prenen Hans, Vandenberghe Peter, Wozniak Agnieszka, Schöffski Patrick, Marynen Peter, Debiec-Rychter Maria

机构信息

Department of Human Genetics, K.U. Leuven, and VIB Department of Molecular and Developmental Genetics, VIB, Leuven, Belgium.

出版信息

Clin Cancer Res. 2008 Sep 15;14(18):5749-58. doi: 10.1158/1078-0432.CCR-08-0533.

DOI:10.1158/1078-0432.CCR-08-0533

PMID:18794084

Abstract

PURPOSE

Activating mutations in platelet-derived growth factor receptor-alpha (PDGFRA) have been reported in approximately 5% to 10% of patients with gastrointestinal stromal tumors (GIST). Imatinib efficiently inhibits the juxtamembrane PDGFRA mutations, whereas many tyrosine kinase domain activation loop PDGFRA mutations confer primary resistance to imatinib. In this study, we compared the efficacy of second-line tyrosine kinase inhibitors such as dasatinib, sorafenib, and nilotinib against two GIST-related PDGFRA mutants, PDGFRA(D842V) and PDGFRA(DeltaDIM842-844). In addition, we sought to investigate the inhibitory effect of the heat shock protein 90 inhibitor, IPI-504, on these mutants.

EXPERIMENTAL DESIGN

Primary imatinib-resistant tumor cells and cell lines expressing imatinib-resistant PDGFRA(D842V) or imatinib-sensitive PDGFRA(DeltaDIM842-844) mutants were treated with different concentrations of dasatinib, sorafenib, nilotinib, and IPI-504. The effect of treatment on proliferation, survival, and signaling was determined.

RESULTS

All inhibitors tested exhibited a high efficacy toward the PDGFRA(DeltaDIM842-844) mutant. In contrast, ex vivo and in vitro assays revealed that only dasatinib potently inhibited the PDGFRA(D842V) isoform with an IC(50) value of 62 nmol/L. Sorafenib and nilotinib were significantly less efficacious against this mutation, inhibiting the PDGFRA kinase activity at >1,000 and >5,000 nmol/L, and suppressing the proliferation of the cells expressing the PDGFRA(D842V) mutant with an IC(50) value of 239 and 1,310 nmol/L, respectively. IPI-504 treatment potently inhibited PDGFRA kinase activity by inducing the degradation of PDGFRA(D842V) and PDGFRA(DeltaDIM842-844) at 256 and 182 nmol/L, respectively.

CONCLUSIONS

Treatment with dasatinib or the heat shock protein 90 inhibitor IPI-504 may provide a therapeutic alternative for GIST patients whose tumors carry the imatinib-resistant PDGFRA(D842V) mutant isoform.

摘要

目的

据报道，在约5%至10%的胃肠道间质瘤（GIST）患者中存在血小板衍生生长因子受体α（PDGFRA）激活突变。伊马替尼可有效抑制近膜区PDGFRA突变，而许多酪氨酸激酶结构域激活环PDGFRA突变会导致对伊马替尼原发性耐药。在本研究中，我们比较了二线酪氨酸激酶抑制剂（如达沙替尼、索拉非尼和尼洛替尼）对两种GIST相关的PDGFRA突变体PDGFRA（D842V）和PDGFRA（ΔDIM842 - 844）的疗效。此外，我们试图研究热休克蛋白90抑制剂IPI - 504对这些突变体的抑制作用。

实验设计

用不同浓度的达沙替尼、索拉非尼、尼洛替尼和IPI - 504处理原发性伊马替尼耐药肿瘤细胞以及表达伊马替尼耐药的PDGFRA（D842V）或伊马替尼敏感的PDGFRA（ΔDIM842 - 844）突变体的细胞系。确定治疗对增殖、存活和信号传导的影响。

结果

所有测试的抑制剂对PDGFRA（ΔDIM842 - 844）突变体均显示出高效。相比之下，体内外试验表明，只有达沙替尼能有效抑制PDGFRA（D842V）异构体，IC50值为62 nmol/L。索拉非尼和尼洛替尼对该突变的疗效明显较差，在>1000和>5000 nmol/L时抑制PDGFRA激酶活性，并分别以239和1310 nmol/L的IC50值抑制表达PDGFRA（D842V）突变体的细胞增殖。IPI - 504处理分别在256和182 nmol/L时通过诱导PDGFRA（D842V）和PDGFRA（ΔDIM842 - 844）的降解有效抑制PDGFRA激酶活性。