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免疫抑制疗法可消除因胸腺识别供体抗原而导致的对肾移植的无反应性。

Immunosuppressive therapy abrogates unresponsiveness to renal allograft induced by thymic recognition of donor antigens.

作者信息

Perico N, Imberti O, Bontempelli M, Remuzzi G

机构信息

Mario Negri Institute for Pharmacological Research, Bergamo, Italy.

出版信息

J Am Soc Nephrol. 1995 Feb;5(8):1618-23. doi: 10.1681/ASN.V581618.

Abstract

This laboratory and others have previously shown that the intrathymic injection of donor cells or major histocompatibility complex allopeptides induced indefinite survival of a subsequent graft without immunosuppression. This approach may open interesting new perspectives for transplant medicine. Studies to explore the feasibility of the technique in humans can only be designed with some form of concomitant immunosuppression to avoid the risk of irreversible rejection in the case that the thymus approach fails. Thus, one of the first issue to address is whether conventional immunosuppression interfered with the process of thymus tolerance. This study was designed to investigate the above issue. In transplanted Lewis control rats, cyclosporin A (CsA) (10 mg/kg per day) and methylprednisolone (MP) (10 mg/kg twice daily) for 3 days were invariably followed by kidney graft rejection within 10 days. In subsequent experiments, five groups of Lewis rats were injected with medium alone or Brown-Norway (BN) leukocytes into the thymus, and 24 h later, they were orthotopically transplanted with major histocompatibility complex-incompatible kidneys from BN rats. At the time of transplantation, Lewis rats received MP (10 mg/kg twice daily) CsA (10 mg/kg per day), or the combination of the two (MP+CsA at the same dose) for 3 days. Lewis rats injected intrathymically with BN leukocytes but not receiving immunosuppressants had indefinite survival of their kidney graft. The effect of the intrathymic injection of donor cells of inducing unresponsiveness to a subsequent kidney graft was abolished by concomitant immunosuppression. All animals given immunosuppressants rejected their graft within 12 days after surgery.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

本实验室及其他研究机构先前已表明,胸腺内注射供体细胞或主要组织相容性复合体同种异体肽可使后续移植在无免疫抑制的情况下长期存活。这种方法可能为移植医学开辟有趣的新前景。探索该技术在人类中可行性的研究只能在某种形式的伴随免疫抑制下进行设计,以避免在胸腺方法失败时出现不可逆排斥反应的风险。因此,首先要解决的问题之一是传统免疫抑制是否会干扰胸腺耐受过程。本研究旨在调查上述问题。在移植的Lewis对照大鼠中,每天给予环孢素A(CsA)(10 mg/kg)和甲基强的松龙(MP)(10 mg/kg,每日两次),持续3天,随后10天内肾脏移植均被排斥。在后续实验中,五组Lewis大鼠胸腺内单独注射培养基或Brown-Norway(BN)白细胞,24小时后,原位移植来自BN大鼠的主要组织相容性复合体不相容的肾脏。移植时,Lewis大鼠接受MP(10 mg/kg,每日两次)、CsA(10 mg/kg,每日一次)或两者联合使用(相同剂量的MP + CsA),持续3天。胸腺内注射BN白细胞但未接受免疫抑制剂的Lewis大鼠肾脏移植长期存活。伴随免疫抑制消除了胸腺内注射供体细胞对后续肾脏移植诱导无反应性的作用。所有给予免疫抑制剂的动物在手术后12天内排斥了移植肾。(摘要截选至250字)

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