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Inhibition of allograft rejection by anti-T-cell receptor-alpha beta monoclonal antibodies preserving resistance to bacterial infection.

机译：抗T细胞受体αβ单克隆抗体抑制同种异体移植排斥从而保持了对细菌感染的抵抗力。

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Anti-CD3 monoclonal antibody (mAb) has been administered in clinical organ transplantation to reverse acute allograft rejection; however, severe immunodeficiency can result from such mAb treatment and cause an increased incidence of opportunistic infections. Therefore, new model systems are required in order to establish better methods for suppressing allograft rejection while preserving resistance to opportunistic infections. In this study, we compared the effects of the in vivo administration of anti-T-cell receptor-alpha beta (TcR alpha beta) mAb, H57-597, with those of anti-CD3 mAb, 145-2C11. Much to our surprise, the in vivo administration of anti-TcR alpha beta mAb prior to skin grafting led to a longer allograft survival than that of anti-CD3 mAb at any of the comparable dosages examined. In the lymphoid organs of mice treated with anti-TcR alpha beta mAb, TcR alpha beta-bearing cells were almost completely depleted, while TcR gamma delta-bearing cells remained at a relatively increased level on day 14 after anti-TcR alpha beta mAb treatment. The in vitro stimulation by anti-TcR gamma delta mAb clearly showed that such TcR gamma delta-bearing cells were functionally intact. Furthermore, the mice treated with anti-TcR alpha beta mAb, but not anti-CD3 mAb, were observed to be resistant to infection with Listeria monocytogenes. Finally, treatment with H57-597, but not with 145-2C11, led to a marked prolongation of skin allograft survival in the thymectomized mice. These results strongly suggest that anti-TcR alpha beta mAb, which partially preserved anti-bacterial resistance, may be more effective in preventing graft rejection than anti-CD3 mAb in the periphery, and indicate that anti-TcR alpha beta mAb may thus be potentially applicable for human transplantation. In addition, these results also indicate that the TcR gamma delta-bearing cells alone, at least in the absence of TcR alpha beta-bearing cells, do not contribute to allograft rejection in vivo.

机译：已在临床器官移植中使用抗CD3单克隆抗体（mAb）来逆转急性同种异体移植排斥；但是，此类mAb治疗可能导致严重的免疫缺陷，并导致机会性感染的发生率增加。因此，需要新的模型系统以建立更好的方法来抑制同种异体移植排斥，同时保持对机会感染的抵抗力。在这项研究中，我们比较了抗T细胞受体αβ（TcRαβ）mAb H57-597和抗CD3 mAb 145-2C11的体内给药效果。令我们惊讶的是，在任何可比较的剂量下，在皮肤移植之前体内施用抗TcRαβmAb导致的同种异体移植存活期长于抗CD3 mAb。在接受抗TcRαβmAb的小鼠的淋巴器官中，含有TcR alphaβ的细胞几乎被完全耗尽，而抗TcR alphaβmAb的治疗在第14天时，含有TcRγδ的细胞保持相对升高的水平。。抗TcRγ单克隆抗体的体外刺激清楚地表明，这种TcRγ轴承细胞功能完整。此外，观察到用抗TcRαβmAb而非抗CD3 mAb治疗的小鼠对单核细胞增生李斯特菌感染具有抗性。最后，用H57-597而非145-2C11进行的治疗导致在经胸腺切除的小鼠中皮肤同种异体移植物存活时间显着延长。这些结果有力地表明，部分保留了抗菌抗性的抗TcRαβmAb在预防移植排斥方面可能比外周抗CD3 mAb更有效，并表明抗TcRαβmAb因此可能适用于人体移植。另外，这些结果还表明，至少在不存在TcRα-β的细胞的情况下，单独的TcR-γ-轴承的细胞对体内同种异体移植排斥没有贡献。

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期刊名称 Immunology
作者
M Eto; Y Yoshikai; Y Nishimura; K Hiromatsu; T Maeda; K Nomoto; Y Y Kong; R T Kubo; J Kumazawa; K Nomoto;
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作者单位

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年(卷),期 1994(81),2
年度 1994
页码 198–204
总页数 7
原文格式 PDF
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中图分类免疫学;
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专利

1. Monoclonal antibody against beta7 integrins, but not beta7 deficiency, attenuates intestinal allograft rejection in mice. [J] . Kellersmann R, Lazarovits A, Grant D, Transplantation: Official Journal of the Transplantation Society . 2002,第9期

机译：针对beta7整联蛋白的单克隆抗体（而非beta7缺乏的单克隆抗体）减弱了小鼠的同种异体肠排斥反应。
2. Inhibition of intestinal allograft rejection by an anti-CD8 monoclonal antibody is not mediated by depletion alone. [J] . He G, Hart J, Thistlethwaite JR Jr, Transplantation Proceedings . 1998,第4期

机译：抗CD8单克隆抗体对肠道同种异体移植排斥的抑制作用并非仅通过消耗来介导。
3. Anti‐C1s monoclonal antibody BIVV BIVV 009 in late antibody‐mediated kidney allograft rejection—results from a first‐in‐patient phase 1 trial [J] . Eskandary F., Jilma B., Mühlbacher J., American journal of transplantation: official journal of the American Society of Transplantation and the American Society of Transplant Surgeons . 2018,第4期

机译：抗C1S单克隆抗体BIVVVV 009在晚期抗体介导的肾同种异体移植物排斥反应 - 来自第一患者的第1期试验
4. RELEVANCE OF DIFFERENT ANTIBODY DETECTION METHODS FOR PREDICTION OF ANTIBODY MEDIATED REJECTION OF DECEASED DONOR KIDNEY ALLOGRAFTS [C] . Adriana I. Colovai, George Vlad, Eric K. Ho, Clinical Histocompatibility Workshop. . 2009

机译：不同抗体检测方法的相关性，用于预测抗体介导的死亡肾同种异体移植物的抑制作用
5. Transforming growth factor beta, allograft acceptance and chronic allograft rejection. [D] . Faust, Susan Marie. 2009

机译：转化生长因子β，同种异体移植接受和慢性同种异体移植排斥。
6. Prevention of anti-T-cell receptor alpha beta monoclonal antibody-induced side-effects by treatment with cyclosporin A without interference of monoclonal antibody-induced immunosuppression in mice. [O] . Y Murakami, Y Y Kong, Y Nishimura, 1995

机译：通过用环孢菌素A的治疗来预防抗T细胞受体αβ单克隆抗体引起的副作用而不会干扰小鼠中单克隆抗体引起的免疫抑制。
7. Effect of anti-.ALPHA..BETA. T cell receptor monoclonal antibody on skin allograft rejection in mice. [O] . Kiichiro Uchiyama 1994

机译：抗.beta的影响。 T细胞受体单克隆抗体对小鼠皮肤同种异体移植物排斥反应。
8. Monoclonal Antibodies for Dengue Virus prM Glycoprotein Protect Mice against Lethal Dengue Infection. [R] . Kaufman, B. M., Summers, P. L., Dubois, D. R., 1989

机译：用于登革病毒prm糖蛋白的单克隆抗体保护小鼠免受致死性登革热感染。

Inhibition of allograft rejection by anti-T-cell receptor-alpha beta monoclonal antibodies preserving resistance to bacterial infection.

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