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αβT细胞受体阳性(αβ TCR+)的T细胞在小鼠心脏同种异体移植排斥反应中发挥着不可替代的作用。

Alpha beta TCR+ T cells play a nonredundant role in the rejection of heart allografts in mice.

作者信息

Exner B G, Que X, Mueller Y M, Domenick M A, Neipp M, Ildstad S T

机构信息

Institute for Cellular Therapeutics, University of Louisville, Glenolden, Pa. 19036, USA.

出版信息

Surgery. 1999 Aug;126(2):121-6.

Abstract

BACKGROUND

Although the transplantation of solid organs and cellular grafts is a clinical routine, the morbidity and mortality associated with immunosuppression is significant. This could be avoided by the induction of donor-specific tolerance. To develop targeted antirejection strategies and regimens to induce donor-specific tolerance, cell populations in the recipient-mediating rejection of solid organ and cellular grafts must be defined. In this study we examined the role of alpha beta-TCR+ cells in the rejection of allogeneic heart grafts, by use of knockout (KO) mice deficient in the production of alpha beta-TCR+ T cells.

METHODS

C57BL/6-TcrbtmlMom (alpha beta-KO) and C57BL6/J (B6) recipient mice were transplanted with B10.BR/SgSnJ (B10.BR) or BALB/c heart allografts. Animals also received bone marrow from normal B10.BR donors, followed by donor-specific or third-party heart transplants.

RESULTS

Naive B6 control mice rejected B10.BR and BALB/c grafts within 16 days. In striking contrast, B10.BR and BALB/c heart allografts were indefinitely accepted in unmanipulated alpha beta-KO mice. The immune responsiveness was restored after bone marrow transplantation from normal donors. After bone marrow transplantation major histocompatibility-disparate BALB/c third-party heart grafts were rejected, whereas donor-specific grafts were still accepted.

CONCLUSIONS

alpha beta-TCR+ T cells play a nonredundant role in the rejection of heart allografts in mice. Bone marrow chimerism is associated with donor-specific transplantation tolerance.

摘要

背景

尽管实体器官移植和细胞移植已是临床常规操作,但免疫抑制相关的发病率和死亡率仍很高。诱导供体特异性耐受可避免这一情况。为制定有针对性的抗排斥策略和方案以诱导供体特异性耐受,必须明确受体中介导实体器官和细胞移植排斥反应的细胞群体。在本研究中,我们通过使用缺乏αβ-TCR+T细胞产生的基因敲除(KO)小鼠,研究了αβ-TCR+细胞在同种异体心脏移植排斥反应中的作用。

方法

将C57BL/6-TcrbtmlMom(αβ-KO)和C57BL6/J(B6)受体小鼠移植B10.BR/SgSnJ(B10.BR)或BALB/c心脏异体移植物。动物还接受来自正常B10.BR供体的骨髓移植,随后进行供体特异性或第三方心脏移植。

结果

未经处理的B6对照小鼠在16天内排斥B10.BR和BALB/c移植物。与之形成鲜明对比的是,未经处理的αβ-KO小鼠可长期接受B10.BR和BALB/c心脏异体移植物。从正常供体进行骨髓移植后,免疫反应性得以恢复。骨髓移植后,主要组织相容性不相容的BALB/c第三方心脏移植物被排斥,而供体特异性移植物仍被接受。

结论

αβ-TCR+T细胞在小鼠心脏异体移植排斥反应中发挥着不可替代的作用。骨髓嵌合与供体特异性移植耐受相关。

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