Clinical Acquired Resistance to KRASG12C Inhibition through a Novel KRAS Switch-II Pocket Mutation and Polyclonal Alterations Converging on RAS-MAPK Reactivation

通过新型 KRAS Switch-II 口袋突变和多克隆变异（以 RAS-MAPK 再激活为中心）获得对 KRASG12C 抑制的临床获得性耐药性

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作者：Noritaka Tanaka #, Jessica J Lin #, Chendi Li #, Meagan B Ryan, Junbing Zhang, Lesli A Kiedrowski, Alexa G Michel, Mohammed U Syed, Katerina A Fella, Mustafa Sakhi, Islam Baiev, Dejan Juric, Justin F Gainor, Samuel J Klempner, Jochen K Lennerz, Giulia Siravegna, Liron Bar-Peled, Aaron N Hata, Rebecc

期刊：

Cancer Discovery

影响因子：

29.700

时间：

2021

起止号：

2021 Aug;11(8):1913-1922.

doi：

10.1158/2159-8290.CD-21-0365

研究方向：

信号转导

信号通路：

MAPK/ERK

Significance

In one of the first reports of clinical acquired resistance to KRASG12C inhibitors, our data suggest polyclonal RAS-MAPK reactivation as a central resistance mechanism. We also identify a novel KRAS switch-II pocket mutation that impairs binding and drives resistance to inactive-state inhibitors but is surmountable by a functionally distinct KRASG12C inhibitor.See related commentary by Pinnelli and Trusolino, p. 1874.This article is highlighted in the In This Issue feature, p. 1861.

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