Enzyme Replacement Therapy for Genetic Disorders Associated with Enzyme Deficiency

酶替代疗法 溶酶体贮存障碍 溶酶体贮存病 遗传增强 基质还原疗法 生物 干细胞疗法 基因 干细胞 计算生物学 疾病 医学 生物化学 遗传学 病理
作者
Marlene Estevão Marchetti,Serena Faggiano,Andrea Mozzarelli
出处
期刊:Current Medicinal Chemistry [Bentham Science]
卷期号:29 (3): 489-525 被引量:4
标识
DOI:10.2174/0929867328666210526144654
摘要

Mutations in human genes might lead to the loss of functional proteins, causing diseases. Among these genetic disorders, a large class is associated with the deficiency in metabolic enzymes, resulting in both an increase in the concentration of substrates and a loss in the metabolites produced by the catalyzed reactions. The identification of therapeutic actions based on small molecules represents a challenge to medicinal chemists because the target is missing. Alternative approaches are biology-based, ranging from gene and stem cell therapy, CRISPR/Cas9 technology, distinct types of RNAs, and enzyme replacement therapy (ERT). This review will focus on the latter approach that since the 1990s has been successfully applied to cure many rare diseases, most of them being lysosomal storage diseases or metabolic diseases. So far, a dozen enzymes have been approved by FDA/EMA for lysosome storage disorders and only a few for metabolic diseases. Enzymes for replacement therapy are mainly produced in mammalian cells and some in plant cells and yeasts and are further processed to obtain active, highly bioavailable, less degradable products. Issues still under investigation for the increase in ERT efficacy are the optimization of the interaction of the enzymes with cell membrane and internalization, the reduction in immunogenicity, and the overcoming of blood-brain barrier limitations when neuronal cells need to be targeted. Overall, ERT has demonstrated its efficacy and safety in the treatment of many genetic rare diseases, both saving newborn lives and improving patients' life quality, and represents a very successful example of targeted biologics.
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