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一种用于犬自体移植模型中肾内输注免疫抑制剂的植入式泵。

An implantable pump for intrarenal infusion of immunosuppressants in a canine autotransplant model.

作者信息

Gruber S A, Cipolle R J, Canafax D M, Erdmann G R, Burke B A, Rabatin J T, Hynes P E, Ritz J A, Gould F H, Ascher N L

机构信息

Department of Surgery, University of Minnesota, Minneapolis 55455.

出版信息

Pharm Res. 1988 Dec;5(12):781-5. doi: 10.1023/a:1015940802451.

Abstract

We developed a canine renal allograft model utilizing implantable infusion pumps and biocompatible catheters to investigate the pharmacokinetics of local immunosuppressive drug administration. Seven mongrel dogs underwent bilateral nephrectomy and autotransplantation of one kidney to the iliac vessels. The proximal end of an infusion catheter directed into the iliac artery was tunneled to a subcutaneously placed programmable pump. A second, sampling catheter was placed with its tip in the iliac vein. Simultaneous regional (iliac vein) and systemic (jugular vein) venous concentrations of 6-mercaptopurine (6-MP), the immunosuppressive metabolite of azathioprine, were determined during a continuous 24-h intraarterial infusion (10 mg/kg/24 hr). The gradient between regional and systemic 6-MP concentrations was maximal initially when the pump was turned on, continuously decreased until steady state was reached, and disappeared immediately after the pump was turned off. The mean ratio of steady-state iliac vein to systemic 6-MP concentrations was 5.0 +/- 1.4, demonstrating a pharmacokinetic advantage of continuous intraarterial 6-MP infusion to the autotransplanted kidney. The novel canine renal allograft model described herein overcomes the technical limitations of earlier models and represents a foundational step in the design of intrarenal infusion patterns of immunosuppressive agents which we expect to prolong survival of the allotransplanted kidney with minimal systemic drug exposure and side effects.

摘要

我们开发了一种犬类肾移植模型,利用植入式输液泵和生物相容性导管来研究局部免疫抑制药物给药的药代动力学。七只杂种犬接受了双侧肾切除术,并将一侧肾脏自体移植到髂血管。一根导入髂动脉的输液导管近端通过皮下隧道连接到一个可程控泵。第二根采样导管的尖端置于髂静脉。在连续24小时动脉内输注(10毫克/千克/24小时)硫唑嘌呤的免疫抑制代谢产物6-巯基嘌呤(6-MP)期间,同时测定局部(髂静脉)和全身(颈静脉)静脉血中6-MP的浓度。泵开启时,局部与全身6-MP浓度之间的梯度最初最大,持续下降直至达到稳态,泵关闭后立即消失。稳态时髂静脉与全身6-MP浓度的平均比值为5.0±1.4,表明持续动脉内输注6-MP对自体移植肾脏具有药代动力学优势。本文所述的新型犬类肾移植模型克服了早期模型的技术局限性,代表了免疫抑制剂肾内输注模式设计的基础步骤,我们期望通过最小的全身药物暴露和副作用来延长同种异体移植肾脏的存活时间。

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