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免疫原性肽在早期溶酶体区室中与II类主要组织相容性复合体分子结合。

Immunogenic peptides bind to class II MHC molecules in an early lysosomal compartment.

作者信息

Harding C V, Geuze H J

机构信息

Institute of Pathology, Case Western Reserve University School of Medicine, Cleveland, OH 44106.

出版信息

J Immunol. 1993 Oct 15;151(8):3988-98.

PMID:8409381
Abstract

Exogenous protein Ag are processed within endocytic compartments to produce peptides that bind to class II MHC (MHC-II) molecules for presentation to T cells. We have now identified a subcellular compartment in which immunogenic peptides bind to MHC-II as a subset of high density lysosomes. Immunoelectron microscopy of whole cells and dense Percoll gradient subcellular fractions showed early tubulovesicular lysosomes with high levels of MHC-II. Typical mature lysosomes contained less MHC-II. Pulse-chase biosynthetic labeling of macrophages followed by immunoprecipitation of MHC-II from dense lysosomal fractions showed that MHC-II molecules targeted efficiently to lysosomes after biosynthesis. Moreover, lysosomal MHC-II molecules were rapidly loaded with immunogenic peptide (as detected by T cells) soon after exposure of macrophages to Ag and before similar expression of peptide-MHC-II complexes on the plasma membrane; this loading was blocked at 18 degrees C. We propose that nascent MHC-II molecules target to early tubulovesicular lysosomes and bind immunogenic peptides therein; the resulting peptide-MHC-II complexes are then transported to the plasma membrane.

摘要

外源性蛋白质抗原在内吞小室中被加工处理,以产生与II类主要组织相容性复合体(MHC-II)分子结合的肽段,从而呈递给T细胞。我们现已鉴定出一种亚细胞区室,其中免疫原性肽段作为高密度溶酶体的一个亚群与MHC-II结合。对全细胞和经Percoll密度梯度离心分离的亚细胞组分进行免疫电子显微镜观察显示,早期的管状囊泡状溶酶体中MHC-II水平较高。典型的成熟溶酶体中MHC-II含量较少。对巨噬细胞进行脉冲追踪生物合成标记,随后从致密溶酶体组分中免疫沉淀MHC-II,结果表明MHC-II分子在生物合成后能有效地靶向溶酶体。此外,巨噬细胞暴露于抗原后,在肽-MHC-II复合物在质膜上出现类似表达之前,溶酶体中的MHC-II分子很快就被免疫原性肽段(如T细胞检测到的)快速装载;这种装载在18℃时被阻断。我们提出,新生的MHC-II分子靶向早期的管状囊泡状溶酶体,并在其中结合免疫原性肽段;然后,产生的肽-MHC-II复合物被转运到质膜。

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