JAK3抑制剂VI是一种针对具有守门人突变T790M的表皮生长因子受体的突变特异性抑制剂。
JAK3 inhibitor VI is a mutant specific inhibitor for epidermal growth factor receptor with the gatekeeper mutation T790M.
作者信息
Nishiya Naoyuki, Sakamoto Yasumitsu, Oku Yusuke, Nonaka Takamasa, Uehara Yoshimasa
机构信息
Naoyuki Nishiya, Yusuke Oku, Yoshimasa Uehara, Department of Microbial Chemical Biology and Drug Discovery, Iwate Medical University School of Pharmacy, Yahaba, Iwate 028-3694, Japan.
出版信息
World J Biol Chem. 2015 Nov 26;6(4):409-18. doi: 10.4331/wjbc.v6.i4.409.
AIM
To identify non-quinazoline kinase inhibitors effective against drug resistant mutants of epidermal growth factor receptor (EGFR).
METHODS
A kinase inhibitor library was subjected to screening for specific inhibition pertaining to the in vitro kinase activation of EGFR with the gatekeeper mutation T790M, which is resistant to small molecular weight tyrosine kinase inhibitors (TKIs) for EGFR in non-small cell lung cancers (NSCLCs). This inhibitory effect was confirmed by measuring autophosphorylation of EGFR T790M/L858R in NCI-H1975 cells, an NSCLC cell line harboring the gatekeeper mutation. The effects of a candidate compound, Janus kinase 3 (JAK3) inhibitor VI, on cell proliferation were evaluated using the MTT assay and were compared between T790M-positive and -negative lung cancer cell lines. JAK3 inhibitor VI was modeled into the ATP-binding pocket of EGFR T790M/L858R. Potential physical interactions between the compound and kinase domains of wild-type (WT) or mutant EGFRs or JAK3 were estimated by calculating binding energy. The gatekeeper residues of EGFRs and JAKs were aligned to discuss the similarities among EGFR T790M and JAKs.
RESULTS
We found that JAK3 inhibitor VI, a known inhibitor for JAK3 tyrosine kinase, selectively inhibits EGFR T790M/L858R, but has weaker inhibitory effects on the WT EGFR in vitro. JAK3 inhibitor VI also specifically reduced autophosphorylation of EGFR T790M/L858R in NCI-H1975 cells upon EGF stimulation, but did not show the inhibitory effect on WT EGFR in A431 cells. Furthermore, JAK3 inhibitor VI suppressed the proliferation of NCI-H1975 cells, but showed limited inhibitory effects on the WT EGFR-expressing cell lines A431 and A549. A docking simulation between JAK3 inhibitor VI and the ATP-binding pocket of EGFR T790M/L858R predicted a potential binding status with hydrogen bonds. Estimated binding energy of JAK3 inhibitor VI to EGFR T790M/L858R was more stable than its binding energy to the WT EGFR. Amino acid sequence alignments revealed that the gatekeeper residues of JAK family kinases are methionine in WT, similar to EGFR T790M, suggesting that TKIs for JAKs may also be effective for EGFR T790M.
CONCLUSION
Our findings demonstrate that JAK3 inhibitor VI is a gatekeeper mutant selective TKI and offer a strategy to search for new EGFR T790M inhibitors.
目的
鉴定对表皮生长因子受体(EGFR)耐药突变体有效的非喹唑啉激酶抑制剂。
方法
用激酶抑制剂文库筛选对具有守门人突变T790M的EGFR体外激酶激活有特异性抑制作用的物质,该突变对非小细胞肺癌(NSCLC)中EGFR的小分子酪氨酸激酶抑制剂(TKI)耐药。通过检测NCI-H1975细胞(一种携带守门人突变的NSCLC细胞系)中EGFR T790M/L858R的自磷酸化来确认这种抑制作用。使用MTT法评估候选化合物Janus激酶3(JAK3)抑制剂VI对细胞增殖的影响,并在T790M阳性和阴性肺癌细胞系之间进行比较。将JAK3抑制剂VI模拟到EGFR T790M/L858R的ATP结合口袋中。通过计算结合能来估计该化合物与野生型(WT)或突变型EGFR或JAK3的激酶结构域之间潜在的物理相互作用。对EGFR和JAK的守门人残基进行比对,以讨论EGFR T790M与JAK之间的相似性。
结果
我们发现JAK3抑制剂VI(一种已知的JAK3酪氨酸激酶抑制剂)在体外选择性抑制EGFR T790M/L858R,但对WT EGFR的抑制作用较弱。JAK3抑制剂VI还能在EGF刺激后特异性降低NCI-H1975细胞中EGFR T790M/L858R的自磷酸化,但对A431细胞中的WT EGFR没有抑制作用。此外,JAK3抑制剂VI抑制NCI-H1975细胞的增殖,但对表达WT EGFR的细胞系A431和A549的抑制作用有限。JAK3抑制剂VI与EGFR T790M/L858R的ATP结合口袋之间的对接模拟预测了一种通过氢键的潜在结合状态。JAK3抑制剂VI与EGFR T790M/L858R的估计结合能比其与WT EGFR的结合能更稳定。氨基酸序列比对显示,JAK家族激酶的守门人残基在WT中为甲硫氨酸,与EGFR T790M相似,这表明JAK的TKI对EGFR T790M也可能有效。
结论
我们的研究结果表明JAK3抑制剂VI是一种守门人突变体选择性TKI,并提供了一种寻找新的EGFR T790M抑制剂的策略。
Zotero 插件