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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Effects of long-term administration of recombinant human protein C in xenografted primates.
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Effects of long-term administration of recombinant human protein C in xenografted primates.

机译:长期施用重组人蛋白C在异种灵长类动物中的作用。

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BACKGROUND: The role potential of recombinant human activated protein C (rhaPC), a recently developed molecule with anticoagulant and antiinflammatory properties, in prolonging survival in immunosuppressed primate recipients of porcine renal xenografts has been evaluated. METHODS: rhaPC was administered daily for 5 days (24 mug/kg/hr; group A; n = 3) or throughout the postoperative period (8-24 mug/kg/hr; group B; n = 2; or 24-48 mug/kg/hr; group C; n = 4). Animals in group D (n = 2) received rhaPC daily (24 mug/kg/hr) combined with recombinant human antithrombin (84 U/kg every 8 hr). Two animals served as control (group E). RESULTS: The results indicate that rhaPC is protective against fibrin deposition early after transplantation but does not prevent fibrin deposition and the occurrence of acute humoral xenograft rejection (AHXR) later on. Animals in the study survived between 8 and 55 days. At the dose used, rhaPC is able to prevent fibrin deposition in the graft in the first 2 weeks after xenotransplantation, except when it is administered in conjunction with antithrombin. However, rhaPC did not prevent the eventual occurrence of AHXR in primate recipients of porcine xenografts. CONCLUSIONS: In this pig to primate model, rhaPC confers a short advantage in the prevention of early perioperative xenograft damage but does not represent an effective strategy for preventing AHXR.
机译:背景:已经评估了重组人活化蛋白C(rhaPC)(一种新近开发的具有抗凝血和抗炎特性的分子)在延长免疫抑制的猪肾异种移植灵长类动物受体体内的存活中的潜在作用。方法:rhaPC每天给药5天(24杯/千克/小时; A组; n = 3);或在整个术后期间(8-24杯/千克/小时; B组; n = 2;或24-48杯子/千克/小时; C组; n = 4)。 D组(n = 2)的动物每天接受rhaPC(24杯/千克/小时)联合重组人抗凝血酶(每8小时84 U /千克)。两只动物作为对照(E组)。结果:结果表明,rhaPC在移植后早期可防止纤维蛋白沉积,但不能防止纤维蛋白沉积和随后发生的急性体液异种移植排斥反应(AHXR)。该研究中的动物存活了8至55天。在异剂量移植后的头两周内,rhaPC能够以所用的剂量防止纤维蛋白沉积在移植物中,除非与抗凝血酶联用时除外。但是,rhaPC不能阻止猪异种移植的灵长类动物接受者最终发生AHXR。结论:在这种猪到灵长类动物模型中,rhaPC在预防早期围手术期异种移植损伤方面具有短暂的优势,但不能代表预防AHXR的有效策略。

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