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主要组织相容性复合体和次要抗原错配对角膜移植排斥反应的影响。

Effect of mismatches for major histocompatibility complex and minor antigens on corneal graft rejection.

作者信息

Nicholls S M, Bradley B B, Easty D L

机构信息

Department of Ophthalmology, School of Medical Sciences, Bristol Eye Hospital, Bristol, United Kingdom.

出版信息

Invest Ophthalmol Vis Sci. 1991 Sep;32(10):2729-34.

PMID:1894472
Abstract

The importance of minor histocompatibility genes in corneal graft rejection was investigated using a model that simulates the major histocompatibility complex (MHC) and minor mismatches of the human allograft more accurately than previous animal models. DA(RT1a) x LEW(RT1(1]F1 hybrid rats were backcrossed to LEW, and the backcross generation were used as corneal graft recipients. Female DA(RT1a) strain animals were used as donors throughout. As in humans, the MHC disparity (a to 1) between each donor-recipient pair could be controlled; minor mismatches were variable and unknown. The MHC haplotype of each backcross individual (either homozygous l/l) or heterozygous a/l) was determined. Depending on this haplotype, the transplanted DA cornea was either matched or mismatched with the recipient for MHC antigens. The average proportion of minor disparate loci was 50%, although this was variable and unknown from recipient to recipient. Some animals of each MHC type were sensitized with three subcutaneous DA strain skin grafts at intervals of 2 weeks. Prior sensitization caused more rapid corneal graft rejection in both MHC mismatched (P less than 0.001) and matched (P less than 0.01) animals. All animals in the two MHC-mismatched groups (sensitized, 26; unsensitized, 17) and most in the MHC-matched groups (sensitized, 25 of 27; unsensitized, all 13) rejected their grafts. The MHC matching resulted in a greater range of survival times, although the difference in survival in unsensitized animals between matched and mismatched groups was not significant (unsensitized, P greater than 0.05; sensitized, P less than 0.001).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

利用一种比以往动物模型更精确模拟人类同种异体移植主要组织相容性复合体(MHC)和次要错配的模型,研究了次要组织相容性基因在角膜移植排斥反应中的重要性。将DA(RT1a)×LEW(RT1l)F1杂交大鼠与LEW回交,回交后代用作角膜移植受体。整个实验过程中均使用雌性DA(RT1a)品系动物作为供体。与人类一样,可控制每对供体 - 受体之间的MHC差异(a对1);次要错配是可变的且未知。确定每个回交个体的MHC单倍型(纯合子l/l或杂合子a/l)。根据这种单倍型,移植的DA角膜在MHC抗原方面与受体匹配或不匹配。次要不同位点的平均比例为50%,尽管受体之间存在差异且未知。每种MHC类型的一些动物每隔2周用三次皮下DA品系皮肤移植进行致敏。预先致敏在MHC不匹配(P小于0.001)和匹配(P小于0.01)的动物中均导致角膜移植排斥反应更快。两个MHC不匹配组中的所有动物(致敏组,26只;未致敏组,17只)以及MHC匹配组中的大多数动物(致敏组,27只中的25只;未致敏组,全部13只)均排斥了它们的移植物。MHC匹配导致存活时间范围更大,尽管未致敏动物中匹配组和不匹配组之间的存活差异不显著(未致敏组,P大于0.05;致敏组,P小于0.001)。(摘要截断于250字)

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