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皮肤移植后预防同种抗体形成,体内抗L3T4未延长移植存活时间。

Prevention of alloantibody formation after skin grafting without prolongation of graft survival by anti-L3T4 in vivo.

作者信息

Auchincloss H, Ghobrial R R, Russell P S, Winn H J

机构信息

Transplantation Unit, Massachusetts General Hospital, Boston 02114.

出版信息

Transplantation. 1988 Jun;45(6):1118-23. doi: 10.1097/00007890-198806000-00024.

DOI:10.1097/00007890-198806000-00024
PMID:3289152
Abstract

Treatment of mice in vivo with monoclonal antibodies against the L3T4 antigen (CD4 in human beings) has been shown to suppress the humoral response to several foreign antigens and to prolong the survival of allografts in some cases. Experiments were therefore performed to test whether anti-L3T4 antibody treatment would suppress alloantibody production after skin transplantation. Monoclonal anti-L3T4 antibody (GK1.5) was administered to C57BL/6 (B6) mice prior to BALB/c skin grafting. The production of B6 anti-BALB/c alloantibody was then tested after graft rejection. The results showed that: (1) graft survival of BALB/c skin on B6 mice was not substantially prolonged by anti-L3T4 treatment; (2) graft survival was significantly prolonged if mice were treated with both anti-L3T4 and anti-Lyt2 antibody; (3) the production of alloantibody following grafting was decreased by anti-L3T4 treatment and was completely eliminated if thymectomy was also performed; (4) thymectomy prolonged the effectiveness of the anti-L3T4 treatment; (5) tolerance to alloantigens presented at the time of anti-L3T4 treatment was not achieved; and (6) well-established cytotoxic antibody titers rose to higher levels after secondary grafting even with concurrent anti-L3T4 treatment, while weak antibody titers remained stable or decreased. These results indicate that L3T4+ cells are essential in providing the "help" necessary for generating humoral responses to alloantigens but that elimination of these L3T4+ cells still allows the generation of help for cell-mediated immunity. The data also suggest that class I antigens must be presented on class II molecules in order to elicit an antibody response.

摘要

用针对L3T4抗原(人类中的CD4)的单克隆抗体对小鼠进行体内治疗,已显示可抑制对几种外来抗原的体液反应,并在某些情况下延长同种异体移植物的存活时间。因此,进行了实验以测试抗L3T4抗体治疗是否会抑制皮肤移植后的同种异体抗体产生。在将BALB/c皮肤移植到C57BL/6(B6)小鼠之前,给它们注射单克隆抗L3T4抗体(GK1.5)。然后在移植物排斥后测试B6抗BALB/c同种异体抗体的产生。结果表明:(1)抗L3T4治疗并未显著延长BALB/c皮肤在B6小鼠上的移植物存活时间;(2)如果用抗L3T4和抗Lyt2抗体同时治疗小鼠,移植物存活时间会显著延长;(3)抗L3T4治疗可降低移植后同种异体抗体的产生,如果同时进行胸腺切除术,则可完全消除;(4)胸腺切除术延长了抗L3T4治疗的效果;(5)未实现对抗L3T4治疗时呈现的同种异体抗原的耐受;(6)即使同时进行抗L3T4治疗,二次移植后已建立的细胞毒性抗体滴度仍会升至更高水平,而弱抗体滴度则保持稳定或下降。这些结果表明,L3T4+细胞对于产生针对同种异体抗原的体液反应所必需的“辅助”至关重要,但消除这些L3T4+细胞仍可产生针对细胞介导免疫的辅助作用。数据还表明,I类抗原必须呈现在II类分子上才能引发抗体反应。

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Prevention of alloantibody formation after skin grafting without prolongation of graft survival by anti-L3T4 in vivo.皮肤移植后预防同种抗体形成,体内抗L3T4未延长移植存活时间。
Transplantation. 1988 Jun;45(6):1118-23. doi: 10.1097/00007890-198806000-00024.
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Comparison of GK1.5 and chimeric rat/mouse GK1.5 anti-CD4 antibodies for prolongation of skin allograft survival and suppression of alloantibody production in mice.比较GK1.5和嵌合型大鼠/小鼠GK1.5抗CD4抗体在延长小鼠皮肤同种异体移植存活时间及抑制同种抗体产生方面的作用。
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Transgenic anti-CD4 monoclonal antibody secretion by mouse segmental pancreas allografts promotes long term survival.小鼠节段性胰腺同种异体移植分泌转基因抗CD4单克隆抗体可促进长期存活。
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