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接受环孢素A的犬节段性胰腺同种异体移植的延长。

Prolongation of segmental pancreatic allografts in dogs receiving cyclosporin A.

作者信息

Du Toit D F, Reece-Smith H, McShane P, Denton T, Morris P J

出版信息

Transplantation. 1982 Apr;33(4):432-7.

PMID:6176055
Abstract

This study showed that a heterotopic autotransplant of the tail of the pancreas was capable of maintaining adequate glucoregulatory function in pancreatectomized dogs, glucose tolerance test curves, and K values not differing from normal dogs 4 months after transplantation. Hyperinsulinemia in the fasting state was observed in the absence of hypoglycemia in autograft and allograft recipients. Intraductal Ethibloc injection produced total replacement of the exocrine gland at 4 months by fibrosis but with the preservation of islets. Cyclosporin A (Cy A, oral drinking solution) in a dose of 25 mg/kg/day given to recipients of heterotopic segmental allografts produced a slight but significant prolongation of graft survival, but a dose of 40 mg/kg/day resulted in indefinite graft survival (greater than 100 days) in five of eight allograft recipients. During intravenous glucose tolerance tests (IVGTTs), fasting hyperinsulinemia and significantly impaired glucose degradation (K values) was observed in long-term surviving allograft recipients 4 months after transplantation. In four long-term surviving pancreatic allograft recipients initially given 40 mg/kg/day, the dose of Cy A was gradually reduced after 4 months to a maintenance dose of 5 mg/kg/day by 6 months. On a dose of 5 mg/kg/day, three dogs rejected their grafts between 18 and 28 days after this schedule had commenced. Successful reversal of the hyperglycemia in two of three dogs that rejected their grafts was achieved by i.v. methylprednisolone and increased doses of Cy A. These results indicate that Cy A alone could significantly prolong the survival of canine pancreatic segmental allografts, but initially higher doses were required than that found to be effective in prolonging renal allograft survival in the dog.

摘要

本研究表明,胰腺尾部异位自体移植能够在胰腺切除的犬体内维持足够的糖调节功能,移植4个月后,葡萄糖耐量试验曲线和K值与正常犬无异。在自体移植和同种异体移植受体中,空腹状态下观察到高胰岛素血症,但无低血糖。导管内注射Ethibloc在4个月时可使外分泌腺完全被纤维组织替代,但胰岛得以保留。给异位节段性同种异体移植受体口服剂量为25mg/kg/天的环孢素A(Cy A)可使移植物存活时间略有但显著延长,而剂量为40mg/kg/天可使8只同种异体移植受体中的5只移植物无限期存活(超过100天)。在静脉葡萄糖耐量试验(IVGTTs)中,移植4个月后的长期存活同种异体移植受体出现空腹高胰岛素血症和葡萄糖降解显著受损(K值)。在最初给予40mg/kg/天的4只长期存活的胰腺同种异体移植受体中,4个月后Cy A剂量逐渐减少,到6个月时降至维持剂量5mg/kg/天。在剂量为5mg/kg/天时,3只犬在该方案开始后的18至28天之间排斥了移植物。通过静脉注射甲基强的松龙和增加Cy A剂量,3只排斥移植物的犬中有2只成功逆转了高血糖。这些结果表明,单独使用Cy A可显著延长犬胰腺节段性同种异体移植物的存活时间,但最初所需剂量高于在犬肾同种异体移植存活延长中发现的有效剂量。

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