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异种移植免疫原性和免疫抑制对大鼠中枢神经系统中宿主主要组织相容性复合体表达的影响。

The influence of xenotransplant immunogenicity and immunosuppression on host MHC expression in the rat CNS.

作者信息

Czech K A, Ryan J W, Sagen J, Pappas G D

机构信息

Department of Anatomy and Cell Biology, University of Illinois, Chicago Health Sciences 60612, USA.

出版信息

Exp Neurol. 1997 Sep;147(1):66-83. doi: 10.1006/exnr.1997.6589.

Abstract

During the early stages following neural transplantation, host immune responses are initiated that are not normally found in the CNS including the induction of major histocompatibility antigens (MHC I and II). Previous laboratory findings have demonstrated prolonged survival of bovine chromaffin cells (BCC) in the rat CNS following transient immunosuppression with cyclosporin A (CSA) providing chromaffin cells are isolated from highly immunogenic passenger cells. To assess the influence of passenger and chromaffin cells on host MHC I and II expression, either BCC, nonchromaffin cell adrenal constituents (NCC), or adrenal medullary endothelial cells (EC) were implanted into the host. At 2 weeks postimplantation, robust BCC survival was obtained in CSA-treated animals. This correlated with low expression of MHC I at the host-graft border and the virtual absence of MHC II. Good BCC survival with reduced MHC I expression only was seen at 6 weeks postimplantation in animals transiently immunosuppressed (4 weeks). In contrast, poor survival was seen in the EC group (even with CSA treatment). In addition, marked MHC I and II expression was found in and around these grafts at 2 weeks, and was particularly intense in EC implanted animals. The results of this study suggest that nonchromaffin passenger cells in BCC preparations, most notably endothelial cells, can induce strong immune responses even in the presence of immunosuppression. Based on MHC staining, removal of these passenger cells can reduce host responses and improve long term survival of xenogeneic chromaffin cells in the CNS.

摘要

在神经移植后的早期阶段,会引发宿主免疫反应,而这些反应在中枢神经系统中通常不会出现,包括主要组织相容性抗原(MHC I和II)的诱导。先前的实验室研究结果表明,在用环孢菌素A(CSA)进行短暂免疫抑制后,牛嗜铬细胞(BCC)在大鼠中枢神经系统中能够长期存活,前提是嗜铬细胞是从高度免疫原性的过客细胞中分离出来的。为了评估过客细胞和嗜铬细胞对宿主MHC I和II表达的影响,将BCC、非嗜铬细胞肾上腺成分(NCC)或肾上腺髓质内皮细胞(EC)植入宿主。植入后2周,CSA处理的动物获得了强大的BCC存活率。这与宿主-移植物边界处MHC I的低表达以及MHC II几乎不存在相关。在短暂免疫抑制(4周)的动物中,仅在植入后6周观察到BCC存活率良好且MHC I表达降低。相比之下,EC组的存活率较差(即使进行了CSA处理)。此外,在这些移植物及其周围在2周时发现了明显的MHC I和II表达,在植入EC的动物中尤为强烈。这项研究的结果表明,BCC制剂中的非嗜铬过客细胞,最显著的是内皮细胞,即使在存在免疫抑制的情况下也能诱导强烈的免疫反应。基于MHC染色,去除这些过客细胞可以降低宿主反应并提高异种嗜铬细胞在中枢神经系统中的长期存活率。

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