Department of Pediatrics, UCSF, San Francisco, California, USA.
Plexxikon Inc., South San Francisco, California, USA.
JCI Insight. 2023 Sep 8;8(17):e168445. doi: 10.1172/jci.insight.168445.
A T50I substitution in the K-Ras interswitch domain causes Noonan syndrome and emerged as a third-site mutation that restored the in vivo transforming activity and constitutive MAPK pathway activation by an attenuated KrasG12D,E37G oncogene in a mouse leukemia model. Biochemical and crystallographic data suggested that K-RasT50I increases MAPK signal output through a non-GTPase mechanism, potentially by promoting asymmetric Ras:Ras interactions between T50 and E162. We generated a "switchable" system in which K-Ras mutant proteins expressed at physiologic levels supplant the fms like tyrosine kinase 3 (FLT3) dependency of MOLM-13 leukemia cells lacking endogenous KRAS and used this system to interrogate single or compound G12D, T50I, D154Q, and E162L mutations. These studies support a key role for the asymmetric lateral assembly of K-Ras in a plasma membrane-distal orientation that promotes the formation of active Ras:Raf complexes in a membrane-proximal conformation. Disease-causing mutations such as T50I are a valuable starting point for illuminating normal Ras function, elucidating mechanisms of disease, and identifying potential therapeutic opportunities for Rasopathy disorders and cancer.
K-Ras 开关区的 T50I 取代导致努南综合征,并作为第三个点突变出现,恢复了体内转化活性,并通过在小鼠白血病模型中减弱的 KrasG12D,E37G 致癌基因持续激活 MAPK 途径。生化和晶体学数据表明,K-RasT50I 通过非 GTPase 机制增加 MAPK 信号输出,可能通过促进 T50 和 E162 之间的不对称 Ras:Ras 相互作用。我们生成了一个“可切换”系统,其中生理水平表达的 K-Ras 突变蛋白取代了缺乏内源性 KRAS 的 MOLM-13 白血病细胞对 fms 样酪氨酸激酶 3(FLT3)的依赖性,并使用该系统研究了单个或复合 G12D、T50I、D154Q 和 E162L 突变。这些研究支持 K-Ras 在远离质膜的方向上不对称横向组装在促进形成膜近端构象的活性 Ras:Raf 复合物中的关键作用。像 T50I 这样的致病突变是阐明正常 Ras 功能、阐明疾病机制以及为 Rasopathy 疾病和癌症确定潜在治疗机会的有价值起点。
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