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人自然杀伤细胞与猪内皮细胞的滚动黏附主要依赖于CD49d-CD106相互作用。

Rolling adhesion of human NK cells to porcine endothelial cells mainly relies on CD49d-CD106 interactions.

作者信息

Schneider Mårten K J, Strasser Marion, Gilli Urs O, Kocher Markus, Moser René, Seebach Jörg D

机构信息

Laboratory for Transplantation Immunology, University Hospital Zürich, CH-8091 Zürich, Switzerland.

出版信息

Transplantation. 2002 Mar 15;73(5):789-96. doi: 10.1097/00007890-200203150-00023.

Abstract

BACKGROUND

Acute vascular rejection in pig-to-primate xenotransplantation involves recognition and damage of porcine (po) endothelial cells (EC) by human (hu) leukocytes, probably including natural killer (NK) cells. To study such interactions we analyzed rolling and static adhesion of hu NK cells to po EC.

METHODS

The effects of blocking hu and po adhesion molecules on the adhesion hu NK cells to po EC monolayers was analyzed under shear stress (10 min, 37 degrees C, 0.7 dynes/cm2) or under static conditions (10 min, 37 degrees C). All used cell populations were phenotypically characterized by flow cytometry.

RESULTS

Blocking of CD106 on po EC or its ligand CD49d on hu NK cells decreased rolling adhesion of both fresh and activated hu NK cells by more than 75%. Masking of CD62L on fresh but not activated hu NK resulted in a 44% decrease in rolling adhesion, in line with the diminished cell surface expression of CD62L upon activation. Antibodies to CD31, CD54, CD62E, and CD62P on EC or CD11a, CD18, and CD162 on NK cells had only minor effects on rolling adhesion. The adhesion of the FcgammaRIII- hu NK cell line NK92 to po EC was inhibited by 95% after masking po CD106 whereas antibodies to po CD31, CD54, CD62E, or CD62P had no effect, thereby excluding effects of Fc-receptor-dependent binding of hu NK cells to po EC. Static adhesion of activated NK cells was reduced by approximately 60% by blocking either CD49d or CD106, by 47% by blocking CD11a, and by 82% upon simultaneous blocking of CD11a and CD49d.

CONCLUSIONS

Interactions between hu CD49d and po CD106 are crucial for both rolling and firm adhesion of hu NK cells to po EC and thus represent attractive targets for specific therapeutic interventions to prevent NK cell-mediated responses against po xenografts.

摘要

背景

猪到灵长类动物异种移植中的急性血管排斥反应涉及人类白细胞对猪内皮细胞的识别和损伤,其中可能包括自然杀伤细胞。为了研究此类相互作用,我们分析了人类自然杀伤细胞与猪内皮细胞的滚动和静态黏附情况。

方法

在剪切应力(10分钟,37摄氏度,0.7达因/平方厘米)或静态条件(10分钟,37摄氏度)下,分析阻断人类和猪黏附分子对人类自然杀伤细胞与猪内皮细胞单层黏附的影响。所有使用的细胞群体均通过流式细胞术进行表型特征分析。

结果

阻断猪内皮细胞上的CD106或其在人类自然杀伤细胞上的配体CD49d,可使新鲜和活化的人类自然杀伤细胞的滚动黏附减少75%以上。掩盖新鲜但未活化的人类自然杀伤细胞上的CD62L,可使滚动黏附减少44%,这与活化后细胞表面CD62L表达减少一致。内皮细胞上针对CD31、CD54、CD62E和CD62P的抗体,或自然杀伤细胞上针对CD11a、CD18和CD162的抗体,对滚动黏附的影响较小。掩盖猪CD106后,FcγRIII -人类自然杀伤细胞系NK92与猪内皮细胞的黏附被抑制95%,而针对猪CD31、CD54、CD62E或CD62P的抗体则无作用,从而排除了人类自然杀伤细胞通过Fc受体依赖性结合猪内皮细胞的影响。阻断CD49d或CD106可使活化自然杀伤细胞的静态黏附减少约60%,阻断CD11a可使其减少47%,同时阻断CD11a和CD49d可使其减少82%。

结论

人类CD49d与猪CD106之间的相互作用对于人类自然杀伤细胞与猪内皮细胞的滚动和牢固黏附至关重要,因此是预防自然杀伤细胞介导的针对猪异种移植物反应的特异性治疗干预的有吸引力的靶点。

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