Leucine-tRNA initiates at CUG start codons for protein synthesis and presentation by MHC class I

亮氨酸-tRNA 在 CUG 起始密码子处启动，进行蛋白质合成并由 MHC I 类分子呈递

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作者：Shelley R Starck, Vivian Jiang, Mariana Pavon-Eternod, Sharanya Prasad, Brian McCarthy, Tao Pan, Nilabh Shastri

期刊：	Science	影响因子：	44.700
时间：	2012	起止号：	2012 Jun 29;336(6089):1719-23.
doi：	10.1126/science.1220270	研究方向：	信号转导

Abstract

Effective immune surveillance by cytotoxic T cells requires newly synthesized polypeptides for presentation by major histocompatibility complex (MHC) class I molecules. These polypeptides are produced not only from conventional AUG-initiated, but also from cryptic non-AUG-initiated, reading frames by distinct translational mechanisms. Biochemical analysis of ribosomal initiation complexes at CUG versus AUG initiation codons revealed that cells use an elongator leucine-bound transfer RNA (Leu-tRNA) to initiate translation at cryptic CUG start codons. CUG/Leu-tRNA initiation was independent of the canonical initiator tRNA (AUG/Met-tRNA(i)(Met)) pathway but required expression of eukaryotic initiation factor 2A. Thus, a tRNA-based translation initiation mechanism allows non-AUG-initiated protein synthesis and supplies peptides for presentation by MHC class I molecules.

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