首页> 外文会议>International Symposium on Amyloidosis >THE USE OF SEQUENTIAL LIVING DONOR KIDNEY AND AUTOLOGOUS STEM CELL TRANSPLANTATION FOR PATIENTS WITH PRIMARY (AL) AMYLOIDOSIS AND ADVANCED RENAL FAILURE
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THE USE OF SEQUENTIAL LIVING DONOR KIDNEY AND AUTOLOGOUS STEM CELL TRANSPLANTATION FOR PATIENTS WITH PRIMARY (AL) AMYLOIDOSIS AND ADVANCED RENAL FAILURE

机译:使用顺序活体供体肾和自体干细胞移植患者对原发性(Al)淀粉样蛋白病和晚期肾功能衰竭的患者

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Patients with primary (AL) amyloidosis and renal failure have limited life expectancy on dialysis and face higher risk during autologous siem cell transplantation (ASCT). We have pursued a novel strategy of living donor kidney transplant (KTx) prior to ASCT for these patients. Clinical and laboratory outcomes of all 7 patients accepted for this protocol at Mayo Clinic between Dec 1999 and Feb 2003 were reviewed. Five of the 7 were on dialysis prior to KTx. AH 7 patients underwent living donor KTx and experienced good initial graft function. Immunosuppression was tacrolimus (n = 4), cyclosporine (n = 2), or sirolimus (n = 1) in combination with mycophenolate mofetil and prednisone. Five patients subsequently underwent ASCT, 4 with good outcome. For these 4 patients, stem cell harvest was carried out prior to KTx for 3 and after KTx for 1. Average times to neutrophil and platelet engraftment were 15.5 and 23.5 days respectively. The fifth developed progressive hepatic amyloidosis after KTx and was advised against ASCT, died following ASCT elsewhere. Two did not undergo ASCT. One died of a demyelinating disease 4 weeks after KTx. The other has thus far elected not to undergo ASCT and has minimal recurrent disease after 3 years. Living donor KTx followed by ASCT is a feasible approach for AL patients with advanced renal impairment. Prudent patient selection is crucial as KTx will delay ASCT. Stem cell engraftment was not impaired by triple-drug immunosuppression.
机译:患有原发性(Al)淀粉样蛋白病和肾功能衰竭的患者对透析的预期寿命有限,并且在自体Siem细胞移植(ASCT)期间面临更高的风险。在ASCT之前,我们在这些患者之前追求了一种新的活性肾移植(KTX)策略。综述了1999年12月至2003年12月至2003年2月在2003年12月间在Mayo Clinic接受本议定书的所有7例患者的临床和实验室结果。在KTX之前,7中的五个是透析。 AH 7患者接受过生活供体KTX并经历了良好的初始移植功能。免疫抑制与凝集素(n = 4),环孢菌素(n = 2),或西罗莫司(n = 1)与霉酚酸酯mofeetil和泼尼松组合。五名患者随后接受了ASCT,4名良好的结果。对于这4名患者,干细胞收获在KTX之前进行3,在KTX之前进行1. kTx。对于中性粒细胞和血小板植入的平均分别为15.5和23.5天。第五个在KTX后发育了进步性肝脏淀粉样蛋白症,并在其他地方ASCT acceSCTSCT ASCT。两个没有接受ASCT。在KTX后4周死于脱髓鞘疾病。迄今为止,另一个人在3年后甚至在ASCT和疾病中具有最小的复发性疾病。生活捐赠者KTX随后是ASCT是肾脏损伤晚期患者的可行方法。谨慎的患者选择至关重要,因为KTX将延迟ASCT。干细胞植入不受三重药物免疫抑制损害。

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