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环己酰亚胺抑制的翻译核糖体的结构。

Structure of the translating ribosome arrested by cycloheximide.

机构信息

Department of Biology, Texas A&M University, College Station, TX 77843.

Department of Bioengineering, Stanford University, Stanford, CA 94305.

出版信息

Proc Natl Acad Sci U S A. 2021 Nov 30;118(48). doi: 10.1073/pnas.2111862118.

DOI:10.1073/pnas.2111862118
PMID:34815343
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8640747/
Abstract

Ribosomes translate RNA into proteins. The protein synthesis inhibitor cycloheximide (CHX) is widely used to inhibit eukaryotic ribosomes engaged in translation elongation. However, the lack of structural data for actively translating polyribosomes stalled by CHX leaves unanswered the question of which elongation step is inhibited. We elucidated CHX's mechanism of action based on the cryo-electron microscopy structure of actively translating ribosomes bound with CHX at 2.7-Å resolution. The ribosome structure from this filamentous fungus contains clearly resolved ribosomal protein eL28, like higher eukaryotes but unlike budding yeast, which lacks eL28. Despite some differences in overall structures, the ribosomes from , yeast, and humans all contain a highly conserved CHX binding site. We also sequenced classic CHX-resistant alleles. These mutations, including one at a residue not previously observed to affect CHX resistance in eukaryotes, were in the large subunit proteins uL15 and eL42 that are part of the CHX-binding pocket. In addition to A-site transfer RNA (tRNA), P-site tRNA, messenger RNA, and CHX that are associated with the translating ribosome, spermidine is present near the CHX binding site close to the E site on the large subunit. The tRNAs in the peptidyl transferase center are in the A/A site and the P/P site. The nascent peptide is attached to the A-site tRNA and not to the P-site tRNA. The structural and functional data obtained show that CHX arrests the ribosome in the classical PRE translocation state and does not interfere with A-site reactivity.

摘要

核糖体将 RNA 翻译成蛋白质。蛋白质合成抑制剂环己酰亚胺(CHX)被广泛用于抑制参与翻译延伸的真核核糖体。然而,由于缺乏被 CHX stall 的活跃翻译多核糖体的结构数据,尚不清楚哪种延伸步骤被抑制。我们基于 2.7-Å 分辨率的与 CHX 结合的活跃翻译核糖体的冷冻电子显微镜结构阐明了 CHX 的作用机制。这个丝状真菌的核糖体结构包含清晰可辨的核糖体蛋白 eL28,与高等真核生物一样,但与缺乏 eL28 的芽殖酵母不同。尽管在整体结构上存在一些差异,但来自 、酵母和人类的核糖体都包含一个高度保守的 CHX 结合位点。我们还测序了经典的 CHX 抗性等位基因。这些突变,包括一个以前在真核生物中观察到不影响 CHX 抗性的残基突变,位于大亚基蛋白 uL15 和 eL42 中,它们是 CHX 结合口袋的一部分。除了与翻译核糖体相关的 A 位 tRNA(tRNA)、P 位 tRNA、信使 RNA 和 CHX 外,靠近大亚基 E 位的 CHX 结合位点附近还存在 spermidine。肽酰转移酶中心的 tRNAs 位于 A/A 位和 P/P 位。新生肽与 A 位 tRNA 而不是 P 位 tRNA 结合。获得的结构和功能数据表明,CHX 将核糖体阻滞在经典的 PRE 易位状态,并且不干扰 A 位反应性。