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异位小鼠心脏同种异体移植中,移植物特异性MHC II类基因对同种异体刺激的反应性表达。

Graft-specific MHC class II gene expression in response to allogeneic stimulus in heterotopic murine cardiac allografts.

作者信息

Xu R, Burdick J F, Scott A, Beschorner W E, Adler W, Kittur D S

机构信息

Department of Surgery, Johns Hopkins University School of Medicine, Baltimore, Maryland.

出版信息

Immunology. 1992 Feb;75(2):361-5.

PMID:1551698
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1384720/
Abstract

Although, major histocompatibility complex (MHC) class II antigen expression in allografts is thoroughly studied, regulation of the genes for these antigens is not fully understood. The graft-specific MHC class II genes are potentially important in determining the immunogenicity of graft but their detection in a mixed-cell population such as in the allograft would require unambiguous differentiation of graft-specific class II expression from those in host lymphoid cells. With an oligonucleotide probe that specifically hybridizes to I-Ab mRNA from H-2k haplotype mice, we have studied I-A gene expression in cardiac allografts heterotopically transplanted from B10.Br (H-2k) to B10.D2 (H-2d) mice. Normal B10.Br hearts do not have appreciable I-Ab transcripts as determined with this probe, but 4 days after allografting, a substantial increase in I-Abk messenger RNA (mRNA) content was noted in the allografted hearts which persisted for the next 2 days and then decreased concomitant with destruction of the heart. The increase in I-Abk mRNA preceded the expression of surface Iak antigens on dendritic and endothelial cells in the allograft. These data indicate increased transcription of the I-Ab gene in cells of graft origin suggesting that transcriptional regulation is the initial mechanism for expression of class II genes in allografts. The sustained rise in graft-specific class II mRNA also seen in these allografts suggests that increased mRNA stability may be another mechanism for the increased density of class II antigens in allografts undergoing rejection.

摘要

尽管对同种异体移植中主要组织相容性复合体(MHC)II类抗原的表达进行了深入研究,但这些抗原基因的调控尚未完全明了。移植特异性MHC II类基因在决定移植物免疫原性方面可能具有重要意义,但其在诸如同种异体移植中的混合细胞群体中的检测需要将移植特异性II类表达与宿主淋巴细胞中的表达明确区分开来。利用一种能与H-2k单倍型小鼠的I-Ab mRNA特异性杂交的寡核苷酸探针,我们研究了从B10.Br(H-2k)异位移植到B10.D2(H-2d)小鼠的心脏同种异体移植中I-A基因的表达。用该探针检测发现,正常B10.Br心脏没有明显的I-Ab转录本,但在同种异体移植后4天,同种异体移植心脏中I-Abk信使核糖核酸(mRNA)含量显著增加,这种增加持续了接下来的2天,然后随着心脏的破坏而下降。I-Abk mRNA的增加先于同种异体移植中树突状细胞和内皮细胞表面Iak抗原的表达。这些数据表明移植来源细胞中I-Ab基因的转录增加,提示转录调控是同种异体移植中II类基因表达的初始机制。在这些同种异体移植中也观察到移植特异性II类mRNA的持续升高,这表明mRNA稳定性增加可能是同种异体移植排斥过程中II类抗原密度增加的另一种机制。

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Graft-specific MHC class II gene expression in response to allogeneic stimulus in heterotopic murine cardiac allografts.异位小鼠心脏同种异体移植中,移植物特异性MHC II类基因对同种异体刺激的反应性表达。
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引用本文的文献

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