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明尼苏达抗淋巴细胞球蛋白与环孢素在尸体肾移植中的序贯使用。

Sequential use of Minnesota antilymphoblast globulin and cyclosporine in cadaveric renal transplantation.

作者信息

Kupin W L, Venkatachalam K K, Oh H K, Dienst S, Levin N W

出版信息

Transplantation. 1985 Dec;40(6):601-4. doi: 10.1097/00007890-198512000-00005.

Abstract

The use of Cyclosporine (CsA) immediately after renal transplantation may be associated with an increased incidence and duration of acute tubular necrosis (ATN) and permanent primary graft nonfunction. To avoid this potential interaction we treated recipients of primary cadaveric grafts initially with azathioprine (AZA), methylprednisolone (MP), and 5 daily doses of Minnesota antilymphoblast globulin (MAG) (postoperative days 3-7). AZA was discontinued and CsA started on day 6 if the graft was functioning by then. If ATN persisted beyond day 6, AZA and MAG (maximum 12 doses) were continued and CsA withheld until graft function was established (group 1-33 patients). This protocol is compared to our previous regimen of MAG (14 doses over the first 3 weeks), AZA and MP (group 2-68 primary cadaveric graft recipients). Improved one-year graft survival (81% vs. 60%, P less than 0.05) and patient survival (93% vs. 81%, P less than 0.05) were seen in group 1. The incidence and duration of ATN did not differ in the two groups. During the first year after transplantation more patients in group 1 were completely free of rejection episodes (40% vs. 20%, P less than 0.05) and the number of rejection episodes per patient was also lower in this group (1.0 +/- 15 vs. 1.6 +/- 49, P less than 0.05). The incidence of infections was not different in the two groups. No tumors have developed in either group. We conclude that in primary cadaveric renal transplantation the initial administration of a short course of MAG followed by CsA therapy results in excellent graft and patient survival while avoiding the potential adverse effect of CsA on an allograft already subjected to preservation injury.

摘要

肾移植后立即使用环孢素(CsA)可能会增加急性肾小管坏死(ATN)的发生率和持续时间以及永久性原发性移植物无功能的发生风险。为避免这种潜在的相互作用,我们对初次接受尸体肾移植的受者最初采用硫唑嘌呤(AZA)、甲泼尼龙(MP)以及5天剂量的明尼苏达抗淋巴细胞球蛋白(MAG)进行治疗(术后第3 - 7天)。如果到第6天时移植物功能良好,则停用AZA并开始使用CsA。如果ATN持续超过第6天,则继续使用AZA和MAG(最多12剂)并停用CsA,直至移植物功能恢复(第1组 - 33例患者)。该方案与我们之前使用MAG(前3周内14剂)、AZA和MP的方案进行了比较(第2组 - 68例初次接受尸体肾移植的受者)。第1组患者1年移植物存活率(81%对60%,P < 0.05)和患者存活率(93%对81%,P < 0.05)均有所提高。两组中ATN的发生率和持续时间无差异。移植后第一年,第1组中更多患者完全没有排斥反应(40%对20%,P < 0.05),且该组每位患者的排斥反应次数也更低(1.0±1.5对1.6±4.9,P < 0.05)。两组感染发生率无差异。两组均未发生肿瘤。我们得出结论,在初次尸体肾移植中,先短期使用MAG然后进行CsA治疗,可使移植物和患者获得良好的存活率,同时避免CsA对已遭受保存损伤的同种异体移植物产生潜在的不良影响。

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