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低磷酸酯酶症的酶替代疗法——当前范例。

Enzyme replacement therapy for hypophosphatasia-The current paradigm.

机构信息

Bioengineering and Molecular Medicine Laboratory, The Children's Hospital at Westmead and Westmead Institute for Medical Research, Westmead, New South Wales, Australia.

Children's Hospital at Westmead Clinical School, University of Sydney, Camperdown, New South Wales, Australia.

出版信息

Clin Endocrinol (Oxf). 2024 Dec;101(6):593-601. doi: 10.1111/cen.15063. Epub 2024 Jul 14.

Abstract

Hypophosphatasia (HPP) is a rare, inherited, and systemic disorder characterized by impaired skeletal mineralization and low tissue nonspecific serum alkaline phosphatase (TNSALP) activity. It is caused by either autosomal recessive or dominant-negative mutations in the gene that encodes TNSALP. The phenotype of HPP is very broad including abnormal bone mineralization, disturbances of calcium and phosphate metabolism, pain, recurrent fracture, short stature, respiratory impairment, developmental delay, tooth loss, seizures, and premature death. Other than supportive care, there has been no disease-specific treatment available for those with HPP. Asfotase alfa is a fully humanized, recombinant enzyme replacement therapy for the management of HPP. It is available in several countries for the treatment of the more severe forms of HPP, namely perinatal and infantile HPP. This review will summarize the preclinical data on asfotase alfa and highlight the data from clinical trials and case reports. These data show the transformative nature of asfotase alfa when administered as part of an interdisciplinary treatment model.

摘要

低磷酸酯酶症(HPP)是一种罕见的、遗传性的、全身性疾病,其特征是骨骼矿化受损和组织非特异性血清碱性磷酸酶(TNSALP)活性降低。它是由编码 TNSALP 的基因的常染色体隐性或显性负突变引起的。HPP 的表型非常广泛,包括异常的骨矿化、钙和磷代谢紊乱、疼痛、反复骨折、身材矮小、呼吸功能障碍、发育迟缓、牙齿缺失、癫痫发作和早逝。除了支持性护理外,目前还没有针对 HPP 的特定疾病治疗方法。阿法特酶是一种用于 HPP 管理的完全人源化重组酶替代疗法。它在几个国家被批准用于治疗更严重的 HPP 形式,即围产期和婴儿期 HPP。这篇综述将总结阿法特酶的临床前数据,并重点介绍临床试验和病例报告的数据。这些数据显示了阿法特酶在作为多学科治疗模式的一部分时的变革性。

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