肿瘤坏死因子受体TNFR-I（P55）和TNFR-II（P75）在角膜移植中的作用

Role of tumor necrosis factor receptors TNFR-I (P55) and TNFR-II (P75) in corneal transplantation.

作者信息

Yamada J, Streilein J W, Dana M R

机构信息

Department of Ophthalmology, Harvard Medical School, Boston, Massachusetts 02114, USA.

出版信息

Transplantation. 1999 Oct 15;68(7):944-9. doi: 10.1097/00007890-199910150-00008.

DOI:10.1097/00007890-199910150-00008

PMID:10532532

Abstract

BACKGROUND

To determine the role of tumor necrosis factor-alpha (TNF-alpha) receptor (TNFR) function in corneal allograft immunology.

METHODS

Animals with gene-targeted deficiency in TNFR-I (p55-/-), TNFR-II (p75-/-), or combined TNFR-I/TNFR-II deficiency (p55-/-p75-/-) and their wild-type controls were used as recipients of fully-mismatched (BALB/c; n=88) or multiple minor alloantigen-mismatched (BALB.b; n=62) orthotopic corneal transplants to determine the effect of selective deficiency in one or both TNF-alpha receptors on corneal allograft survival. Grafted recipients were followed biomicroscopically for signs of rejection, and survival data were analyzed by the Kaplan-Meier method.

RESULTS

There was no discernible difference in survival of fully-mismatched BALB/c corneal grafts in p55-/- (n=12; P=0.76) or in double-knockout p55-/-p75-/- (n=13; P=0.41) as compared with wild-type C57BL/6.129 hosts. However, the survival of BALB/c allografts was lower in p75-/- (n=10; median survival 20 days) as compared with control C57BL/6 (n=30; median survival 30 days) hosts (P=0.02). In contrast, there was no discernible effect in survival of minor alloantigen-disparate BALB.b corneal grafts in p75-/- (n=13; P=0.95) or in combined p55-/-p75-/-(n=10; P=0.17) hosts as compared with C57BL/6 (n=9) and C57BL/6.129 (n=10) wild-type controls, respectively. However, there was a profound enhancement in the survival of BALB.b allografts in p55-/- recipients (n= 10; median survival 35 days) as compared to wild-type C57BL/6.129 (n=10; median survival 25 days) controls (P<0.01).

CONCLUSIONS

Our data suggest that the two TNF-alpha receptors largely play discrete roles in mediating rejection of murine corneal allografts. TNFR-I (p55) function seems to be integral to the rejection of minor-disparate grafts, and its selective suppression leads to enhancement of allograft survival. In contrast, TNFR-II (p75) function appears to be associated with enhanced survival of major histocompatibility complex-disparate allografts. The combined deletion of TNFR functionality in p55-/-p75-/- confers no net advantage or disadvantage to major histocompatibility complex or minor alloantigen-disparate grafts.

摘要

背景

确定肿瘤坏死因子-α（TNF-α）受体（TNFR）功能在角膜移植免疫学中的作用。

方法

将TNFR-I（p55-/-）、TNFR-II（p75-/-）基因靶向缺陷或TNFR-I/TNFR-II联合缺陷（p55-/-p75-/-）的动物及其野生型对照作为完全不匹配（BALB/c；n = 88）或多个次要同种异体抗原不匹配（BALB.b；n = 62）原位角膜移植的受体，以确定一种或两种TNF-α受体选择性缺陷对角膜移植存活的影响。对移植受体进行生物显微镜检查以观察排斥迹象，并采用Kaplan-Meier方法分析存活数据。

结果

与野生型C57BL/6.129宿主相比，p55-/-（n = 12；P = 0.76）或双敲除p55-/-p75-/-（n = 13；P = 0.41）中完全不匹配的BALB/c角膜移植的存活没有明显差异。然而，与对照C57BL/6（n = 30；中位存活时间30天）宿主相比，p75-/-（n = 10；中位存活时间20天）中BALB/c同种异体移植的存活较低（P = 0.02）。相比之下，与C57BL/6（n = 9）和C57BL/6.129（n = 10）野生型对照相比，p75-/-（n = 13；P = 0.95）或联合p55-/-p75-/-（n = 10；P = 0.17）宿主中次要同种异体抗原不同的BALB.b角膜移植的存活没有明显影响。然而，与野生型C57BL/6.129（n = 10；中位存活时间25天）对照相比，p55-/-受体（n = 10；中位存活时间35天）中BALB.b同种异体移植的存活有显著提高（P<0.01）。

结论

我们的数据表明，两种TNF-α受体在介导小鼠角膜同种异体移植排斥中主要发挥不同作用。TNFR-I（p55）功能似乎是次要不同移植排斥所必需的，其选择性抑制导致同种异体移植存活的提高。相比之下，TNFR-II（p75）功能似乎与主要组织相容性复合体不同的同种异体移植存活的提高有关。p55-/-p75-/-中TNFR功能的联合缺失对主要组织相容性复合体或次要同种异体抗原不同的移植没有净优势或劣势。