Sotorasib 是一种泛 RASG12C 抑制剂,能够促进 NRASG12C 癌症的临床反应。

IF 29.7 1区 医学 Q1 ONCOLOGY Cancer discovery Pub Date : 2024-05-01 DOI:10.1158/2159-8290.CD-23-1138
Douglas A Rubinson, Noritaka Tanaka, Ferran Fece de la Cruz, Kevin S Kapner, Michael H Rosenthal, Bryanna L Norden, Haley Barnes, Sara Ehnstrom, Alvin A Morales-Giron, Lauren K Brais, Christopher T Lemke, Andrew J Aguirre, Ryan B Corcoran
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引用次数: 0

摘要

KRASG12C 抑制剂(如 sotorasib 和 adagrasib)通过与突变半胱氨酸的共价相互作用,有效且选择性地抑制 KRASG12C,从而提高了 KRASG12C 肿瘤的临床疗效。由于三种主要的 RAS 异构体--KRAS、NRAS 和 HRAS--的氨基酸序列高度相似,我们推测一些 KRASG12C 抑制剂可能也会靶向 NRASG12C 和/或 HRASG12C,它们在一些肿瘤中并不常见,但却是关键的致癌驱动突变。一些抑制剂(如 adagrasib)对 KRASG12C 具有高度选择性,而其他抑制剂也能有效抑制 NRASG12C 和/或 HRASG12C。值得注意的是,与 KRASG12C 或 HRASG12C 相比,sotorasib 对 NRASG12C 的抑制作用要强 5 倍。结构和互变研究表明,异构体特异性结合的差异是由一个氨基酸介导的:KRAS 中的组氨酸-95(NRAS 中的亮氨酸-95)。一名 NRASG12C 结直肠癌患者在接受索托拉西布和抗表皮生长因子受体抗体帕尼单抗治疗后,肿瘤反应明显,这表明索托拉西布对 NRASG12C 突变肿瘤临床有效。
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Sotorasib Is a Pan-RASG12C Inhibitor Capable of Driving Clinical Response in NRASG12C Cancers.

KRASG12C inhibitors, like sotorasib and adagrasib, potently and selectively inhibit KRASG12C through a covalent interaction with the mutant cysteine, driving clinical efficacy in KRASG12C tumors. Because amino acid sequences of the three main RAS isoforms-KRAS, NRAS, and HRAS-are highly similar, we hypothesized that some KRASG12C inhibitors might also target NRASG12C and/or HRASG12C, which are less common but critical oncogenic driver mutations in some tumors. Although some inhibitors, like adagrasib, were highly selective for KRASG12C, others also potently inhibited NRASG12C and/or HRASG12C. Notably, sotorasib was five-fold more potent against NRASG12C compared with KRASG12C or HRASG12C. Structural and reciprocal mutagenesis studies suggested that differences in isoform-specific binding are mediated by a single amino acid: Histidine-95 in KRAS (Leucine-95 in NRAS). A patient with NRASG12C colorectal cancer treated with sotorasib and the anti-EGFR antibody panitumumab achieved a marked tumor response, demonstrating that sotorasib can be clinically effective in NRASG12C-mutated tumors.

Significance: These studies demonstrate that certain KRASG12C inhibitors effectively target all RASG12C mutations and that sotorasib specifically is a potent NRASG12C inhibitor capable of driving clinical responses. These findings have important implications for the treatment of patients with NRASG12C or HRASG12C cancers and could guide design of NRAS or HRAS inhibitors. See related commentary by Seale and Misale, p. 698. This article is featured in Selected Articles from This Issue, p. 695.

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来源期刊
Cancer discovery
Cancer discovery ONCOLOGY-
CiteScore
22.90
自引率
1.40%
发文量
838
审稿时长
6-12 weeks
期刊介绍: Cancer Discovery publishes high-impact, peer-reviewed articles detailing significant advances in both research and clinical trials. Serving as a premier cancer information resource, the journal also features Review Articles, Perspectives, Commentaries, News stories, and Research Watch summaries to keep readers abreast of the latest findings in the field. Covering a wide range of topics, from laboratory research to clinical trials and epidemiologic studies, Cancer Discovery spans the entire spectrum of cancer research and medicine.
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