Bin Sawad Aseel, Pothukuchy Arti, Badeaux Mark, Hodson Victoria, Bubb Gillian, Lindsley Kristina, Uyei Jennifer, Diaz George A
Aeglea BioTherapeutics, Inc. Austin Texas USA.
Health Economics and Outcomes Research - Evidence Synthesis IQVIA, Inc. San Francisco California USA.
JIMD Rep. 2022 Mar 25;63(4):330-340. doi: 10.1002/jmd2.12283. eCollection 2022 Jul.
Arginase 1 deficiency (ARG1-D) is a rare, progressive and debilitating urea cycle disorder characterized by clinical manifestations including spasticity, seizures, developmental delay, and intellectual disability. The aim of this systematic review was to identify and summarize the natural history of ARG1-D and the unmet needs of patients.
A comprehensive search of published case reports was undertaken to identify patients with ARG1-D regardless of interventions, comparisons, or outcomes. MEDLINE, EMBASE, Cochrane Central Register of Controlled Trials, and other evidence-based medicine literature databases were searched on 20 April 2020. Quality was assessed using the Joanna Briggs Institute (JBI) Critical Appraisal Checklist. (PROSPERO registration: CRD42020212142.).
One hundred and fifty seven ARG1-D patients were included from 111 publications (good overall quality based on JBI's Checklist); 84 (53.5%) were males. Motor deficits (including spasticity), intellectual disability, and seizures were reported in >50% of the cases. Mean age (SD) at diagnosis was 6.4 years and the laboratory findings most commonly reported to support diagnosis included elevated plasma arginine (81.5%), mutation in gene through genetic testing (60%), and absence/reduction of red blood cell arginase activity (51%). Reported management approaches mainly included dietary protein restriction (68%), nitrogen scavengers (45%), and essential amino acid supplements (21%). Author-reported clinical improvement was documented for 26% of patients, 15% deteriorated, and 19% had limited or no change; notably, no indication of clinical outcome was reported for 40% cases.
This review illustrates a significant burden of disease and highlights a considerable unmet need for clinically effective treatment options for patients with ARG1-D.
精氨酸酶1缺乏症(ARG1-D)是一种罕见的、进行性且使人衰弱的尿素循环障碍,其临床表现包括痉挛、癫痫发作、发育迟缓以及智力残疾。本系统评价的目的是确定并总结ARG1-D的自然病史以及患者未满足的需求。
对已发表的病例报告进行全面检索,以确定患有ARG1-D的患者,而不考虑干预措施、对照或结果。于2020年4月20日检索了MEDLINE、EMBASE、Cochrane对照试验中心注册库以及其他循证医学文献数据库。使用乔安娜·布里格斯研究所(JBI)批判性评价清单评估质量。(国际前瞻性系统评价注册平台注册号:CRD42020212142。)
从111篇出版物中纳入了157例ARG1-D患者(根据JBI清单,总体质量良好);84例(53.5%)为男性。超过50%的病例报告有运动缺陷(包括痉挛)、智力残疾和癫痫发作。诊断时的平均年龄(标准差)为6.4岁,最常报告用于支持诊断的实验室检查结果包括血浆精氨酸升高(81.5%)、通过基因检测发现基因中的突变(60%)以及红细胞精氨酸酶活性缺乏/降低(51%)。报告的管理方法主要包括饮食蛋白质限制(68%)、氮清除剂(45%)和必需氨基酸补充剂(21%)。作者报告26%的患者有临床改善记录,15%病情恶化,19%病情有限改善或无变化;值得注意的是,40%的病例未报告临床结局情况。
本评价表明了该疾病的重大负担,并凸显了ARG1-D患者对临床有效治疗方案存在相当大的未满足需求。
