抑制致癌性 K-Ras 的方法。
Approaches to inhibiting oncogenic K-Ras.
机构信息
Department of Integrative Biology and Pharmacology, McGovern Medical School, The University of Texas Health Science Center at Houston , Houston, TX, USA.
Programs of Biochemistry & Cell and Therapeutics & Pharmacology, MD Anderson UTHealth Graduate School of Biomedical Sciences , Houston, TX, USA.
出版信息
Small GTPases. 2021 Mar;12(2):96-105. doi: 10.1080/21541248.2019.1655883. Epub 2019 Aug 22.
Abstract
Activating somatic K-Ras mutations are associated with >15% all human tumors and up to 90% of specific tumor types such as pancreatic cancer. Successfully inhibiting abnormal K-Ras signaling would therefore be a game changer in cancer therapy. However, K-Ras has long been considered an undruggable target for various reasons. This view is now changing by the discovery of allosteric inhibitors that directly target K-Ras and inhibit its functions, and by the identification of new mechanisms to dislodge it from the plasma membrane and thereby abrogate its cellular activities. In this review, we will discuss recent progresses and challenges to inhibiting aberrant K-Ras functions by these two approaches. We will also provide a broad overview of other approaches such as inhibition of K-Ras effectors, and offer a brief perspective on the way forward.
摘要
体细胞 KRAS 突变与超过 15%的所有人类肿瘤有关,并且与特定肿瘤类型(如胰腺癌)高达 90%的肿瘤相关。因此,成功抑制异常的 KRAS 信号将是癌症治疗中的一个重大突破。然而,由于各种原因,KRAS 长期以来一直被认为是一个不可成药的靶点。这种观点正在发生改变,因为发现了能够直接靶向 KRAS 并抑制其功能的变构抑制剂,以及发现了将其从质膜上置换出来从而阻断其细胞活性的新机制。在这篇综述中,我们将讨论这两种方法抑制异常 KRAS 功能的最新进展和挑战。我们还将广泛概述其他方法,如抑制 KRAS 效应物,并简要展望未来的发展方向。
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