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Targeting Wolman Disease and Cholesteryl Ester Storage Disease: Disease Pathogenesis and Therapeutic Development

机译:针对Wolman疾病和胆固醇酯存储疾病:疾病发病机理和治疗发展

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摘要

Wolman disease (WD) and cholesteryl ester storage disease (CESD) are lysosomal storage diseases (LSDs) caused by a deficiency in lysosomal acid lipase (LAL) due to mutations in the LIPA gene. This enzyme is critical to the proper degradation of cholesterol in the lysosome. LAL function is completely lost in WD while some residual activity remains in CESD. Both are rare diseases with an incidence rate of less than 1/100,000 births for WD and approximate 2.5/100,000 births for CESD. Clinical manifestation of WD includes hepatosplenomegaly, calcified adrenal glands, severe malabsorption and a failure to thrive. As in CESD, histological analysis of WD tissues reveals the accumulation of triglycerides (TGs) and esterified cholesterol (EC) in cellular lysosomes. However, the clinical presentation of CESD is less severe and more variable than WD. This review is to provide an overview of the disease pathophysiology and the current state of therapeutic development for both of WD and CESD. The review will also discuss the application of patient derived iPSCs for further drug discovery.
机译:沃尔曼疾病(WD)和胆固醇酯存储疾病(CESD)是由LIPA基因突变引起的溶酶体酸性脂肪酶(LAL)缺乏引起的溶酶体存储疾病(LSD)。该酶对溶酶体中胆固醇的适当降解至关重要。 WD中的LAL功能完全消失,而CESD中仍保留了一些剩余的活动。两者都是罕见疾病,WD的发病率低于1 / 100,000例,CESD的发病率约为2.5 / 100,000例。 WD的临床表现包括肝脾肿大,肾上腺钙化,严重的吸收不良和to壮。与CESD一样,对WD组织的组织学分析表明,甘油三酸酯(TGs)和酯化胆固醇(EC)在细胞溶酶体内积聚。但是,与WD相比,CESD的临床表现不那么严重,而且变化更大。本综述旨在概述WD和CESD的疾病病理生理学和治疗发展的当前状态。该综述还将讨论患者衍生的iPSC在进一步药物开发中的应用。

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