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One Atom Makes All the Difference: Getting a Foot in the Door between SOS1 and KRAS

机译:一个原子使得所有差异有所作为:在SOS1和KRA之间的门口进入门口

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摘要

KRAS, the most common oncogenic driver in human cancers, is controlled and signals primarily through protein-protein interactions (PPIs). The interaction between KRAS and SOS1, crucial for the activation of KRAS, is a typical, challenging PPI with a large contact surface area and high affinity. Here, we report that the addition of only one atom placed between Y884(SOS1) and A73(KRAS) is sufficient to convert SOS1 activators into SOS1 inhibitors. We also disclose the discovery of BI-3406. Combination with the upstream EGFR inhibitor afatinib shows in vivo efficacy against KRAS(G13D) mutant colorectal tumor cells, demonstrating the utility of BI-3406 to probe SOS1 biology. These findings challenge the dogma that large molecules are required to disrupt challenging PPIs. Instead, a "foot in the door" approach, whereby single atoms or small functional groups placed between key PPI interactions, can lead to potent inhibitors even for challenging PPIs such as SOS1-KRAS.
机译:KRAS是人类癌症中最常见的致癌因子,主要通过蛋白质-蛋白质相互作用(PPI)来控制和发出信号。KRAS和SOS1之间的相互作用对KRAS的激活至关重要,是一种典型的、具有挑战性的PPI,具有大的接触表面积和高亲和力。在这里,我们报告说,仅在Y884(SOS1)和A73(KRAS)之间添加一个原子就足以将SOS1激活剂转化为SOS1抑制剂。我们还披露了BI-3406的发现。与上游EGFR抑制剂afatinib的组合显示了对KRAS(G13D)突变大肠肿瘤细胞的体内有效性,证明了BI-3406在探测SOS1生物学方面的实用性。这些发现挑战了需要大分子来破坏具有挑战性的PPI的教条。相反,一种“进门”的方法,即放置在关键PPI相互作用之间的单原子或小官能团,可以产生有效的抑制剂,即使对于具有挑战性的PPI,如SOS1-KRAS。

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