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主要组织相容性复合体I类异二聚体在完整细胞内质网中的折叠和组装先于肽的结合。

Folding and assembly of major histocompatibility complex class I heterodimers in the endoplasmic reticulum of intact cells precedes the binding of peptide.

作者信息

Neefjes J J, Hämmerling G J, Momburg F

机构信息

Tumor Immunology Program, German Cancer Research Center, Heidelberg.

出版信息

J Exp Med. 1993 Dec 1;178(6):1971-80. doi: 10.1084/jem.178.6.1971.

Abstract

Major histocompatibility complex (MHC) class I molecules are heterotrimers consisting of a polymorphic H chain, beta 2-microglobulin (beta 2m) and peptide. Peptides are thought to associate early during biosynthesis but the order of assembly of class I molecules from their component subunits in intact cells is not settled. We have studied the assembly of MHC class I molecules in intact cells with or without peptide transporters. MHC class I H chain/beta 2m heterodimers can be efficiently recovered only 4 min after translation and are preceded by a folding intermediate. Approximately 2 min after their formation, the class I heterodimers are loaded with peptides resulting in stable class I heterotrimers. In these in vivo studies, no evidence was obtained that peptide binding to the H chain preceded the association with beta 2m. In contrast, nonassembled class I H chains could be recovered immediately after translation, but this pool did not participate in the formation of class I molecules.

摘要

主要组织相容性复合体(MHC)I类分子是由一条多态性重链、β2-微球蛋白(β2m)和肽组成的异源三聚体。肽被认为在生物合成早期就发生缔合,但完整细胞中I类分子从其组成亚基组装的顺序尚未确定。我们研究了有或没有肽转运体的完整细胞中MHC I类分子的组装。MHC I类重链/β2m异二聚体在翻译后仅4分钟就能有效回收,且在其之前有一个折叠中间体。在其形成后约2分钟,I类异二聚体加载肽,形成稳定的I类异源三聚体。在这些体内研究中,没有证据表明肽与重链的结合先于与β2m的缔合。相反,未组装的I类重链在翻译后可立即回收,但这部分重链不参与I类分子的形成。

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