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A systematic review of the role of eculizumab in systemic lupus erythematosus-associated thrombotic microangiopathy

机译:系统审查生态生态狼疮在全身性红斑狼疮相关的血栓形成微疗病中的作用

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Lupus nephritis (LN) is a severe consequence of systemic lupus erythematosus (SLE) that affects approximately 40% of patients. Pathogenic immune complexes that are characteristic of LN deposit in the kidney and activate immune mediated pathways including the complement system. Complete remission rates in LN are approximately 44% highlighting the need for new treatment strategies in these patients. Eculizumab is a fully humanised IgG2/IgG4 monoclonal antibody directed at C5 and thus prevents the formation of the terminal complement complex. Eculizumab is successfully used in atypical haemolytic uraemic syndrome (aHUS) and paroxysomal nocturnal haemoglobinuria (PNH) but it is not standardly used in LN. The aim of this project was to determine whether there is any role for eculizumab as adjunctive therapy in LN. Using a predefined search strategy on Ovid MEDLINE and EMBASE the literature was reviewed systematically to identify studies in which eculizumab had been used to treat patients with SLE. All patients were included that were treated with complement inhibitors. Favourable outcome in this study was defined as resolution of symptoms that led to treatment, discharge from hospital or recovery of renal function. Patients were excluded if there was no outcome data or if complement inhibition was unrelated to their SLE. From 192 abstracts screened, 14 articles were identified, involving 30 patients. All SLE patients administered eculizumab were treated for thrombotic microangiopathy (TMA) secondary to LN diagnosed either histologically (66%) or as part of a diagnosis of aHUS (73%). 93% of patients had a favourable outcome in response to eculizumab treatment, of which 46% had a favourable outcome and successfully stopped treatment without relapse in symptoms during a median follow up of 7?months. Three patients (10%) reported adverse outcomes related to eculizumab therapy. Scientific evidence supports the involvement of complement in the pathogenesis of LN however the role of complement inhibition in clinical practice is limited to those with TMA features. This systematic review showed that in cases of LN complicated with TMA, eculizumab seems to be a very efficacious therapy. Further evidence is required to determine whether patients with refractory LN may benefit from adjunctive complement inhibition.
机译:狼疮肾炎(LN)是影响大约40%患者的系统性红斑狼疮(SLE)的严重后果。患有肾脏沉积物的病原免疫复合物,并激活包括补体系统的免疫介导的途径。 LN的完整缓解率约为44%,突出了这些患者的新治疗策略的需求。 Eculizumab是针对C5的完全人源化的IgG2 / IgG4单克隆抗体,从而防止末端互补复合物的形成。 Eculizumab以非典型溶血性血症综合征(Ahus)和阵发性夜间血红蛋白尿(PNH)成功地使用,但在LN中没有标准使用。该项目的目的是确定Eculizumab作为LN中的辅助治疗是否存在任何作用。使用预定的搜索策略在Ovid Medline上进行系统,系统地审查了文献,以鉴定生态蛋白已被用于治疗SLE患者的研究。将所有患者均被包括互补抑制剂处理的。本研究有利的结果被定义为导致治疗,从医院排出或肾功能恢复的症状的解决方案。如果没有结果数据或补蛋白与其SLE无关,则排除患者。从192年摘要筛选,鉴定了14篇文章,涉及30名患者。所有SLE患者均为血栓细胞病(TMA)治疗,缩小为LN诊断为组织学(66%)或作为AHUS诊断的一部分(73%)。 93%的患者响应生态治疗具有有利的结果,其中46%有一个有利的结果,并且在中位于7个月的中位后,在没有复发的情况下成功停止治疗。三名患者(10%)报告了与生态蛋白疗法有关的不利结果。科学证据支持补充在LN发病机制中的累及,但是补充抑制在临床实践中的作用仅限于TMA特征的作用。这种系统综述表明,在LN复杂的TMA的情况下,Eculizumab似乎是一个非常有效的治疗。需要进一步的证据来确定难治性LN的患者是否可以从辅助补体抑制中受益。

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