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同种反应性淋巴细胞对人动脉内皮细胞单层的黏附

Adherence of alloreactive lymphocytes to human arterial endothelial cell monolayers.

作者信息

Colson Y L, Markus B H, Zeevi A, Duquesnoy R J

机构信息

Division of Clinical Immunopathology, University of Pittsburgh, PA 15213-3417.

出版信息

Clin Exp Immunol. 1989 Aug;77(2):206-10.

Abstract

Early events of cellular infiltration during allograft rejection involve interactions between alloreactive lymphocytes and vascular endothelium. These interactions have been studied in an in vitro model of lymphocyte adherence to human arterial endothelial cell (HAEC) monolayers. Alloreactive lymphocytes primed against donor HLA antigens (DPL) or unrelated HLA antigens from a third party (TPL) were studied for their adherence to HAEC derived from organ transplant donors. DPL exhibited a degree of adherence to donor HAEC which was nearly twice that of the TPL population and developed a morphologically blastoid appearance. DPL adherence was dependent on the recognition of donor HLA antigens expressed on the HAEC surface and investigation of DPL and TPL adherence at various lymphocyte concentrations showed that the binding of DPL and TPL to HAEC was saturable. Monoclonal antibody (MoAb) directed against HLA class I antigens showed inhibition of only DPL adherence to HAEC monolayers expressing donor class I HLA antigens, whereas MoAb directed against other HAEC surface antigens failed to inhibit either the DPL or TPL populations. The results of this study suggest that in a transplant situation, lymphocyte activation and adherence to the graft endothelium is increased in the context of allorecognition.

摘要

同种异体移植排斥反应中细胞浸润的早期事件涉及同种反应性淋巴细胞与血管内皮之间的相互作用。这些相互作用已在淋巴细胞与人动脉内皮细胞(HAEC)单层黏附的体外模型中进行了研究。研究了针对供体HLA抗原(DPL)或来自第三方的无关HLA抗原(TPL)致敏的同种反应性淋巴细胞对来自器官移植供体的HAEC的黏附情况。DPL对供体HAEC的黏附程度几乎是TPL群体的两倍,并呈现出形态学上的母细胞样外观。DPL的黏附依赖于对HAEC表面表达的供体HLA抗原的识别,在不同淋巴细胞浓度下对DPL和TPL黏附的研究表明,DPL和TPL与HAEC的结合是可饱和的。针对HLA I类抗原的单克隆抗体(MoAb)仅显示抑制DPL对表达供体I类HLA抗原的HAEC单层的黏附,而针对其他HAEC表面抗原的MoAb未能抑制DPL或TPL群体。这项研究的结果表明,在移植情况下,同种识别的背景下淋巴细胞活化和对移植物内皮的黏附会增加。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f1d/1541983/c2f3eba04f66/clinexpimmunol00083-0054-a.jpg

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