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胚胎细胞系中I类主要组织相容性复合体分子的组装缺陷

Defective assembly of class I major histocompatibility complex molecules in an embryonic cell line.

作者信息

Bikoff E K, Otten G R, Robertson E J

机构信息

Department of Obstetrics, Gynecology, and Reproductive Sciences, Mount Sinai School of Medicine, New York, NY 10029.

出版信息

Eur J Immunol. 1991 Sep;21(9):1997-2004. doi: 10.1002/eji.1830210905.

DOI:10.1002/eji.1830210905
PMID:1716207
Abstract

Developmentally regulated expression of the products of the major histocompatibility complex (MHC) is thought to play a key role in maternal tolerance of the fetal allograft. Here we analyze a cell line (EE2H3), derived from early post-implantation-stage mouse embryos, that is defective for MHC class I assembly. To follow expression of a single well-defined class I product, we introduced the H-2Dd gene under control of the human beta-actin promoter. We found that the transfected EE2H3 cells expressed abundant levels of H-2Dd heavy chains and beta 2-microglobulin protein, but only small amounts of H-2Dd surface protein. Surface expression was rescued by the addition of an appropriate antigenic peptide, or by culturing the cells at low temperature. The phenotype exhibited by EE2H3 is thus remarkably similar to that described for class I-negative somatic cell variants selected using antibodies and complement. However, a striking difference was that surface expression in H-2Dd-transfected EE2H3 cells was markedly enhanced in response to treatment with interferon. Thus, we have identified a novel class I assembly-defective cell line. Considering that EE2H3 was established from primary cultures of mouse embryo cells without immunoselection, and is therefore likely to represent a cell population normally present in post-implantation-stage embryos, these findings raise the possibility that expression of class I surface antigens during early development may in part be controlled post-translationally at the level of MHC class I assembly.

摘要

主要组织相容性复合体(MHC)产物的发育调控表达被认为在母体对胎儿同种异体移植物的耐受性中起关键作用。在此,我们分析了一种源自植入后早期小鼠胚胎的细胞系(EE2H3),该细胞系在MHC I类组装方面存在缺陷。为了追踪单一明确的I类产物的表达,我们在人β-肌动蛋白启动子的控制下引入了H-2Dd基因。我们发现,转染的EE2H3细胞表达了大量的H-2Dd重链和β2-微球蛋白,但只有少量的H-2Dd表面蛋白。通过添加适当的抗原肽或在低温下培养细胞可以挽救表面表达。因此,EE2H3表现出的表型与使用抗体和补体选择的I类阴性体细胞变体所描述的表型非常相似。然而,一个显著的差异是,用干扰素处理后,H-2Dd转染的EE2H3细胞中的表面表达明显增强。因此,我们鉴定出一种新型的I类组装缺陷细胞系。鉴于EE2H3是从小鼠胚胎细胞的原代培养物中建立的,没有进行免疫选择,因此很可能代表植入后阶段胚胎中正常存在的细胞群体,这些发现增加了早期发育过程中I类表面抗原的表达可能部分在MHC I类组装水平上受到翻译后控制的可能性。

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