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环孢素可预防BB大鼠胰腺移植排斥反应和复发性糖尿病的证据。

Evidence that cyclosporine prevents rejection and recurrent diabetes in pancreatic transplants in the BB rat.

作者信息

Dugoni W E, Bartlett S T

机构信息

Department of Surgery, School of Medicine, University of California, Davis 95616.

出版信息

Transplantation. 1990 May;49(5):845-8. doi: 10.1097/00007890-199005000-00001.

Abstract

Cyclosporine prevents the development of diabetes in spontaneously diabetic BB rats and NOD mice. However, islet transplants have been shown to be subject to immunologic destruction in hosts treated with CsA and anti-CD4 antibody or those rendered tolerant to donor antigens. This study determines whether the minimum dose of CsA necessary to prevent rejection of pancreatic transplants will also prevent recurrent diabetes in pancreas transplants in BB rats. Lewis recipients promptly reject BN (n = 13, MST 9.2 +/- 0.7 days) and Fisher (n = 6, MST = 11.3 +/- 0.8 days) pancreatic transplants. Treatment with CsA 5 mg/kg/day 0-50 days posttransplant and 2 mg/kg/day 51-100 days (low-dose CsA) produced indefinite survival of BN (n = 5) but not Fisher (n = 4) allografts. Fisher allografts were uniformly successful if maintained on 5 mg/kg/day (n = 4). Treatment with CsA 5 mg/kg/day for 14 days had no deleterious effect on glucose tolerance in Lewis isografts (control [K = 1.81 +/- 0.24, n = 8] vs. CsA treated [K = 1.76 +/- 0.20, n = 8, P = NS]). Low-dose CsA ensured permanent survival of MHC-compatible WF (n = 7, MST greater than 115 days) and MHC-incompatible BN (n = 9, MST greater than 117 days, P = NS) pancreatic transplants in spontaneously diabetic BB/Wor hosts. Three of 11 recipients surviving greater than 100 days enjoyed seemingly permanent acceptance of their allografts after discontinuation of CsA. Immunocompetence was demonstrated by rejection of their pancreas transplants when challenged with donor skin. Vascularized pancreatic allografts treated with CsA appear to be less vulnerable to recurrent diabetes than are islet transplants. Low-dose CsA protects vascularized pancreatic allografts in BB rats from both rejection and recurrent diabetes.

摘要

环孢素可预防自发性糖尿病BB大鼠和非肥胖糖尿病(NOD)小鼠发生糖尿病。然而,胰岛移植在接受环孢素A(CsA)和抗CD4抗体治疗的宿主中或那些对供体抗原产生耐受的宿主中已被证明会受到免疫破坏。本研究确定预防胰腺移植排斥所需的CsA最小剂量是否也能预防BB大鼠胰腺移植中的复发性糖尿病。Lewis受体迅速排斥BN(n = 13,平均存活时间[MST] 9.2 ± 0.7天)和Fisher(n = 6,MST = 11.3 ± 0.8天)胰腺移植。移植后0 - 50天给予5 mg/kg/天的CsA治疗,51 - 100天给予2 mg/kg/天(低剂量CsA),可使BN(n = 5)同种异体移植物无限期存活,但不能使Fisher(n = 4)同种异体移植物存活。如果维持在5 mg/kg/天,Fisher同种异体移植物均成功(n = 4)。给予CsA 5 mg/kg/天治疗14天对Lewis同基因移植物的葡萄糖耐量没有有害影响(对照组[K = 1.81 ± 0.24,n = 8]与CsA治疗组[K = 1.76 ± 0.20,n = 8,P = 无显著性差异])。低剂量CsA可确保MHC相容的WF(n = 7,MST大于115天)和MHC不相容的BN(n = 9,MST大于117天,P = 无显著性差异)胰腺移植物在自发性糖尿病BB/Wor宿主中永久存活。11名存活超过100天的受体中有3名在停用CsA后似乎永久接受了他们的同种异体移植物。当用供体皮肤进行攻击时,其胰腺移植被排斥证明了免疫活性。用CsA治疗的血管化胰腺同种异体移植物似乎比胰岛移植更不易发生复发性糖尿病。低剂量CsA可保护BB大鼠的血管化胰腺同种异体移植物免受排斥和复发性糖尿病的影响。

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