University Children's Hospital Tuebingen, Tuebingen, Germany.
Pediatr Nephrol. 2011 Aug;26(8):1325-9. doi: 10.1007/s00467-011-1879-9. Epub 2011 May 10.
Atypical hemolytic uremic syndrome (aHUS) in childhood is a rare disease associated with high morbidity and mortality. Most cases progress to end-stage renal failure. In approximately 50% of affected patients, mutations in genes encoding complement proteins are causative of the impairment in the regulation of the complement alternative pathway. This leads to deficient host cell protection and inappropriate complement activation on platelets and endothelial cells, particularly in the kidneys. Complement factor H (FH) heterozygosity induces unregulated activation of the membrane attack complex (MAC) C5b-9. Present therapeutic strategies for aHUS include lifelong plasmapheresis and renal dialysis. Unfortunately, kidney transplantation is frequently an unsatisfactory intervention due to the high rate of post-transplantation HUS recurrence, particularly in patients with FH mutation. Combined liver-kidney transplantation is also associated with poor outcome, mostly as a result of premature liver failure secondary to uncontrolled complement activation. Eculizumab is a complement C5 antibody that inhibits complement factor 5a (C5a) and the formation of the MAC. Thus, this antibody may be a promising new agent for patients with an aHUS undergoing kidney transplantation. We present the first case of a young patient with aHUS who received eculizumab as prophylactic treatment prior to a successful kidney transplantation.
儿童非典型溶血尿毒症综合征(aHUS)是一种罕见疾病,与高发病率和死亡率相关。大多数病例进展为终末期肾衰竭。在大约 50%的受影响患者中,编码补体蛋白的基因突变导致补体替代途径的调节受损。这导致宿主细胞保护不足和血小板及内皮细胞补体的不适当激活,尤其是在肾脏。补体因子 H(FH)杂合性诱导膜攻击复合物(MAC)C5b-9 的不受调节激活。目前针对 aHUS 的治疗策略包括终生血浆置换和肾脏透析。不幸的是,由于移植后 aHUS 复发率高,尤其是在 FH 突变患者中,肾移植常常是一种不理想的干预措施。肝肾联合移植也与不良结局相关,主要是由于不受控制的补体激活导致的早期肝功能衰竭。依库珠单抗是一种补体 C5 抗体,可抑制补体因子 5a(C5a)和 MAC 的形成。因此,这种抗体可能是接受肾移植的 aHUS 患者的一种有前途的新型药物。我们报告首例接受依库珠单抗预防性治疗成功进行肾移植的 aHUS 年轻患者。
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