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NAC引导一种核糖体多酶复合物进行新生蛋白质加工。

NAC guides a ribosomal multienzyme complex for nascent protein processing.

作者信息

Lentzsch Alfred M, Yudin Denis, Gamerdinger Martin, Chandrasekar Sowmya, Rabl Laurenz, Scaiola Alain, Deuerling Elke, Ban Nenad, Shan Shu-Ou

机构信息

Division of Chemistry and Chemical Engineering, California Institute of Technology, Pasadena, CA, USA.

Department of Biology, Institute of Molecular Biology and Biophysics, ETH Zurich, Zurich, Switzerland.

出版信息

Nature. 2024 Sep;633(8030):718-724. doi: 10.1038/s41586-024-07846-7. Epub 2024 Aug 21.

Abstract

Approximately 40% of the mammalian proteome undergoes N-terminal methionine excision and acetylation, mediated sequentially by methionine aminopeptidase (MetAP) and N-acetyltransferase A (NatA), respectively. Both modifications are strictly cotranslational and essential in higher eukaryotic organisms. The interaction, activity and regulation of these enzymes on translating ribosomes are poorly understood. Here we perform biochemical, structural and in vivo studies to demonstrate that the nascent polypeptide-associated complex (NAC) orchestrates the action of these enzymes. NAC assembles a multienzyme complex with MetAP1 and NatA early during translation and pre-positions the active sites of both enzymes for timely sequential processing of the nascent protein. NAC further releases the inhibitory interactions from the NatA regulatory protein huntingtin yeast two-hybrid protein K (HYPK) to activate NatA on the ribosome, enforcing cotranslational N-terminal acetylation. Our results provide a mechanistic model for the cotranslational processing of proteins in eukaryotic cells.

摘要

大约40%的哺乳动物蛋白质组会经历N端甲硫氨酸切除和乙酰化,分别由甲硫氨酸氨肽酶(MetAP)和N-乙酰转移酶A(NatA)依次介导。这两种修饰都是严格共翻译的,且在高等真核生物中至关重要。目前对这些酶在翻译核糖体上的相互作用、活性和调控了解甚少。在这里,我们进行了生化、结构和体内研究,以证明新生多肽相关复合物(NAC)协调了这些酶的作用。NAC在翻译早期与MetAP1和NatA组装成一个多酶复合物,并将两种酶的活性位点预先定位,以便对新生蛋白质进行及时的顺序加工。NAC还解除了NatA调节蛋白亨廷顿酵母双杂交蛋白K(HYPK)的抑制性相互作用,从而在核糖体上激活NatA,加强共翻译N端乙酰化。我们的结果为真核细胞中蛋白质的共翻译加工提供了一个机制模型。

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