BCL-2 和 BOK 通过其 C 端跨膜结构域的相互作用调节细胞凋亡。

IF 6.5 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY EMBO Reports Pub Date : 2024-09-01 Epub Date: 2024-07-24 DOI:10.1038/s44319-024-00206-6
Tobias B Beigl, Alexander Paul, Thomas P Fellmeth, Dang Nguyen, Lynn Barber, Sandra Weller, Benjamin Schäfer, Bernhard F Gillissen, Walter E Aulitzky, Hans-Georg Kopp, Markus Rehm, David W Andrews, Kristyna Pluhackova, Frank Essmann
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引用次数: 0

摘要

Bcl-2 家族通过促凋亡蛋白和抗凋亡蛋白的直接相互作用来控制细胞凋亡。其主要机制是促凋亡蛋白的 BH3 结构域与抗凋亡同胞的疏水沟结合,已获批准的 BH3 拟态抗癌药物利用了这一机制。有证据表明,Bcl-2 蛋白的跨膜结构域(TMD)也能介导 Bcl-2 相互作用。我们开发了一种高度特异性的分离荧光素酶测定法,可以分析活细胞中孔形成凋亡效应物 BAX、BAK 和 BOK 与抗凋亡 Bcl-2 蛋白的 TMD 相互作用。我们证实了 BAX-TMD 的同型相互作用,还新发现了抗凋亡 BCL-2 的 TMD 与 BOK(一种特殊的促凋亡 Bcl-2 蛋白)的 TMD 之间的相互作用。BOK-TMD 和 BCL-2-TMD 在内质网上相互作用。分子动力学模拟证实了 BOK-TMD 和 BCL-2-TMD 的动态二聚体和稳定的异构四聚体。在预测的关键残基上突变 BCL-2-TMD,可消除与 BOK-TMD 的相互作用。此外,BCL-2 对 BOK 诱导的细胞凋亡的抑制作用特别依赖于它们的 TMD。因此,Bcl-2 蛋白的 TMD 是调节细胞凋亡的相关相互作用界面,并提供了一个新的潜在药物靶点。
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BCL-2 and BOK regulate apoptosis by interaction of their C-terminal transmembrane domains.

The Bcl-2 family controls apoptosis by direct interactions of pro- and anti-apoptotic proteins. The principle mechanism is binding of the BH3 domain of pro-apoptotic proteins to the hydrophobic groove of anti-apoptotic siblings, which is therapeutically exploited by approved BH3-mimetic anti-cancer drugs. Evidence suggests that also the transmembrane domain (TMD) of Bcl-2 proteins can mediate Bcl-2 interactions. We developed a highly-specific split luciferase assay enabling the analysis of TMD interactions of pore-forming apoptosis effectors BAX, BAK, and BOK with anti-apoptotic Bcl-2 proteins in living cells. We confirm homotypic interaction of the BAX-TMD, but also newly identify interaction of the TMD of anti-apoptotic BCL-2 with the TMD of BOK, a peculiar pro-apoptotic Bcl-2 protein. BOK-TMD and BCL-2-TMD interact at the endoplasmic reticulum. Molecular dynamics simulations confirm dynamic BOK-TMD and BCL-2-TMD dimers and stable heterotetramers. Mutation of BCL-2-TMD at predicted key residues abolishes interaction with BOK-TMD. Also, inhibition of BOK-induced apoptosis by BCL-2 depends specifically on their TMDs. Thus, TMDs of Bcl-2 proteins are a relevant interaction interface for apoptosis regulation and provide a novel potential drug target.

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来源期刊
EMBO Reports
EMBO Reports 生物-生化与分子生物学
CiteScore
11.20
自引率
1.30%
发文量
267
审稿时长
1 months
期刊介绍: EMBO Reports is a scientific journal that specializes in publishing research articles in the fields of molecular biology, cell biology, and developmental biology. The journal is known for its commitment to publishing high-quality, impactful research that provides novel physiological and functional insights. These insights are expected to be supported by robust evidence, with independent lines of inquiry validating the findings. The journal's scope includes both long and short-format papers, catering to different types of research contributions. It values studies that: Communicate major findings: Articles that report significant discoveries or advancements in the understanding of biological processes at the molecular, cellular, and developmental levels. Confirm important findings: Research that validates or supports existing knowledge in the field, reinforcing the reliability of previous studies. Refute prominent claims: Studies that challenge or disprove widely accepted ideas or hypotheses in the biosciences, contributing to the correction and evolution of scientific understanding. Present null data: Papers that report negative results or findings that do not support a particular hypothesis, which are crucial for the scientific process as they help to refine or redirect research efforts. EMBO Reports is dedicated to maintaining high standards of scientific rigor and integrity, ensuring that the research it publishes contributes meaningfully to the advancement of knowledge in the life sciences. By covering a broad spectrum of topics and encouraging the publication of both positive and negative results, the journal plays a vital role in promoting a comprehensive and balanced view of scientific inquiry. 
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