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Raf/LIN-45的C末端远端尾部片段对……中的信号传导起负调控作用。

The Raf/LIN-45 C-terminal distal tail segment negatively regulates signaling in .

作者信息

Townley Robert A, Stacy Kennedy S, Cheraghi Fatemeh, de la Cova Claire C

出版信息

bioRxiv. 2024 Jul 17:2024.07.16.603803. doi: 10.1101/2024.07.16.603803.

DOI:10.1101/2024.07.16.603803
PMID:39071268
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11275798/
Abstract

Raf protein kinases act as Ras-GTP sensing components of the ERK signal transduction pathway in animal cells, influencing cell proliferation, differentiation, and survival. In humans, somatic and germline mutations in the genes and are associated with malignancies and developmental disorders. Recent studies shed light on the structure of activated Raf, a heterotetramer consisting of Raf and 14-3-3 dimers, and raised the possibility that a Raf C-terminal distal tail segment (DTS) regulates activation. We investigated the role of the DTS using the which has a single Raf ortholog termed . We discovered that truncations removing the DTS strongly enhanced , a weak gain-of-function allele equivalent to mutations found in patients with Noonan Syndrome. We generated mutations to test three elements of the LIN-45 DTS, which we termed the active site binding sequence (ASBS), the KTP motif, and the aromatic cluster. In the context of mutation of either the ASBS, KTP motif, or aromatic cluster enhanced activity. We used AlphaFold to predict DTS protein interactions for LIN-45, fly Raf, and human BRAF, within the activated heterotetramer complex. We propose distinct functions for the LIN-45 DTS elements: i) the ASBS binds the kinase active site as an inhibitor, ii) phosphorylation of the KTP motif modulates DTS-kinase domain interaction, and iii) the aromatic cluster anchors the DTS in an inhibitory conformation. This work establishes that the Raf/LIN-45 DTS negatively regulates signaling in and provides a model for its function in other Raf proteins.

摘要

Raf蛋白激酶在动物细胞中作为ERK信号转导通路的Ras - GTP传感组件,影响细胞增殖、分化和存活。在人类中,相关基因的体细胞和种系突变与恶性肿瘤和发育障碍有关。最近的研究揭示了活化的Raf的结构,它是一种由Raf和14 - 3 - 3二聚体组成的异源四聚体,并提出Raf C末端远端尾段(DTS)调节激活的可能性。我们使用具有单个Raf直系同源物(称为LIN - 45)的秀丽隐杆线虫来研究DTS的作用。我们发现去除DTS的截短突变强烈增强了LIN - 45的活性,这是一个功能获得性弱等位基因,相当于努南综合征患者中发现的突变。我们生成突变以测试LIN - 45 DTS的三个元件,我们将其称为活性位点结合序列(ASBS)、KTP基序和芳香族簇。在LIN - 45突变的背景下,ASBS、KTP基序或芳香族簇的突变都会增强活性。我们使用AlphaFold预测活化的异源四聚体复合物中LIN - 45、果蝇Raf和人类BRAF的DTS蛋白相互作用。我们提出LIN - 45 DTS元件具有不同的功能:i)ASBS作为抑制剂结合激酶活性位点,ii)KTP基序的磷酸化调节DTS - 激酶结构域相互作用,iii)芳香族簇将DTS锚定在抑制构象中。这项工作证实了Raf / LIN - 45 DTS在秀丽隐杆线虫中负调节信号传导,并为其在其他Raf蛋白中的功能提供了模型。