通过对 MET 受体酪氨酸激酶结构域进行深度突变扫描,揭示并膜结构域和激酶 N-lobe 中的保守调控基团

IF 6.4 1区 生物学 Q1 BIOLOGY eLife Pub Date : 2024-09-13 DOI:https://doi.org/10.7554/elife.91619.3
Gabriella O Estevam, Edmond M Linossi, Christian B Macdonald, Carla A Espinoza, Jennifer M Michaud, Willow Coyote-Maestas, Eric A Collisson, Natalia Jura, James S Fraser
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引用次数: 0

摘要

MET 是一种受体酪氨酸激酶(RTK),负责启动参与发育和伤口修复的信号通路。MET 的激活依赖于配体与细胞外受体的结合,从而促使二聚化、细胞内磷酸化以及相关信号蛋白的招募。临床上观察到的突变主要发生在细胞内的并膜和激酶结构域,这些突变会破坏典型的 MET 调节机制。了解并膜变异(如外显子 14 跳越(METΔEx14))和罕见的激酶结构域突变如何增加信号传导,往往导致癌症,仍然是一项挑战。在这里,我们对野生型和 METΔEx14 两种融合蛋白背景下的 MET 细胞内激酶结构域进行了平行深度突变扫描(DMS)。我们的比较方法揭示了并膜区段与激酶⍺C-螺旋之间的关键疏水相互作用,指出了 MET 与其他 RTK 之间调控机制的潜在差异。此外,我们还发现了一个 β5 矩阵,它是 MET 和其他 TAM 家族激酶中激酶结构域的结构枢轴。我们还描述了许多以前未知的激活突变,有助于注释 MET 激酶结构域中的驱动突变、乘客突变和耐药性突变。
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Conserved regulatory motifs in the juxtamembrane domain and kinase N-lobe revealed through deep mutational scanning of the MET receptor tyrosine kinase domain
MET is a receptor tyrosine kinase (RTK) responsible for initiating signaling pathways involved in development and wound repair. MET activation relies on ligand binding to the extracellular receptor, which prompts dimerization, intracellular phosphorylation, and recruitment of associated signaling proteins. Mutations, which are predominantly observed clinically in the intracellular juxtamembrane and kinase domains, can disrupt typical MET regulatory mechanisms. Understanding how juxtamembrane variants, such as exon 14 skipping (METΔEx14), and rare kinase domain mutations can increase signaling, often leading to cancer, remains a challenge. Here, we perform a parallel deep mutational scan (DMS) of the MET intracellular kinase domain in two fusion protein backgrounds: wild-type and METΔEx14. Our comparative approach has revealed a critical hydrophobic interaction between a juxtamembrane segment and the kinase ⍺C-helix, pointing to potential differences in regulatory mechanisms between MET and other RTKs. Additionally, we have uncovered a β5 motif that acts as a structural pivot for the kinase domain in MET and other TAM family of kinases. We also describe a number of previously unknown activating mutations, aiding the effort to annotate driver, passenger, and drug resistance mutations in the MET kinase domain.
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来源期刊
eLife
eLife BIOLOGY-
CiteScore
12.90
自引率
3.90%
发文量
3122
审稿时长
17 weeks
期刊介绍: eLife is a distinguished, not-for-profit, peer-reviewed open access scientific journal that specializes in the fields of biomedical and life sciences. eLife is known for its selective publication process, which includes a variety of article types such as: Research Articles: Detailed reports of original research findings. Short Reports: Concise presentations of significant findings that do not warrant a full-length research article. Tools and Resources: Descriptions of new tools, technologies, or resources that facilitate scientific research. Research Advances: Brief reports on significant scientific advancements that have immediate implications for the field. Scientific Correspondence: Short communications that comment on or provide additional information related to published articles. Review Articles: Comprehensive overviews of a specific topic or field within the life sciences.
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