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健康原位角膜同种异体移植小鼠的细胞介导免疫受损。

Impaired cell-mediated immunity in mice bearing healthy orthotopic corneal allografts.

作者信息

Sonoda Y, Streilein J W

机构信息

Department of Microbiology and Immunology, University of Miami School of Medicine, FL 33101.

出版信息

J Immunol. 1993 Mar 1;150(5):1727-34.

PMID:8436812
Abstract

A very high proportion of orthotopically grafted, histoincompatible corneas are accepted in healthy condition for prolonged intervals (> 8 weeks) by naive untreated BALB/c mice. Because these grafts form the anterior surface of the anterior chamber of the eye and because alloantigens placed in the anterior chamber elicit a deviant, stereotypic, systemic immune response known as anterior chamber-associated immune deviation, we have examined the state of alloantigen-specific cell-mediated immunity in BALB/c mice with accepted corneal allografts, as well as mice that had rejected their corneal grafts. Attempts to induce alloantigen-specific delayed hypersensitivity (DH) by s.c. injections of lymphoid cells, genetically identical to the grafts, resulted in positive responses only in "rejector" mice; "acceptor" mice failed to develop or display DH. Spleens cells from acceptors and rejectors were then assayed for the ability to suppress local adoptive transfer of alloantigen-specific DH. It was found that transfer reactions failed to develop if spleen cells from acceptor mice were added to the inoculum, whereas spleen cells from rejected mice had no similar inhibitory effects. The suppression mediated by acceptor spleen cells in local adoptive transfer assays was determined to be specific for the alloantigens expressed on the long-standing corneal allografts. We conclude that, when orthotopic corneal allografts are accepted indefinitely by adult mice, graft success correlates with the induction of alloantigenically specific anterior chamber-associated immune deviation. It is proposed that suppression of alloantigen-specific DH, which is characteristic of mice with accepted grafts, plays a critical role in the success of grafted corneas.

摘要

在未接受过处理的单纯BALB/c小鼠中,很大比例的原位移植、组织不相容的角膜能在健康状态下被长期接受(超过8周)。由于这些移植物形成了眼前房的前表面,并且由于置于前房的同种异体抗原会引发一种异常的、刻板的全身免疫反应,即前房相关免疫偏离,我们研究了接受角膜同种异体移植的BALB/c小鼠以及已排斥角膜移植物的小鼠中同种异体抗原特异性细胞介导免疫的状态。通过皮下注射与移植物基因相同的淋巴细胞来诱导同种异体抗原特异性迟发型超敏反应(DH),结果仅在“排斥者”小鼠中产生了阳性反应;“接受者”小鼠未能产生或表现出DH。然后检测了接受者和排斥者的脾细胞抑制同种异体抗原特异性DH局部过继转移的能力。结果发现,如果将接受者小鼠的脾细胞添加到接种物中,过继转移反应就无法发生,而排斥小鼠的脾细胞则没有类似的抑制作用。在局部过继转移试验中,接受者脾细胞介导的抑制作用被确定为对长期存在的角膜同种异体移植物上表达的同种异体抗原具有特异性。我们得出结论,当成年小鼠无限期接受原位角膜同种异体移植时,移植物的成功与同种异体抗原特异性前房相关免疫偏离的诱导相关。有人提出,接受移植物的小鼠所特有的同种异体抗原特异性DH的抑制作用在移植角膜的成功中起关键作用。

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