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[低磷酸酯酶症:目前有哪些治疗方法?]

[Hypophosphatasia : What is currently available for treatment?].

作者信息

Schmidt T, Amling M, Barvencik F

机构信息

Institut für Osteologie und Biomechanik, Universitätsklinikum Hamburg-Eppendorf, Lottestr. 59, 22529, Hamburg, Deutschland.

出版信息

Internist (Berl). 2016 Dec;57(12):1145-1154. doi: 10.1007/s00108-016-0147-2.

Abstract

This review presents the current knowledge on the diagnosis and treatment of hypophosphatasia, a rare genetic disease, caused by mutations in the tissue non-specific alkaline phosphatase (TNSALP) gene. The clinical spectrum of hypophosphatasia is highly variable ranging from lethal infantile forms to mild forms diagnosed in adults. Although the disease rarely occurs, correct diagnosis is important to provide appropriate treatment and to avoid worsening by use of harmful drugs such as bisphosphonates. Low serum values of alkaline phosphatase (ALP) is the main feature of HPP, but by itself not sufficient for diagnosis, as it can occur under different conditions. Diagnosis can be established by the combination of reduced levels of ALP, elevated ALP substrates (PLP, PEA, PPi) and typical symptoms and can be confirmed by genetic testing of ALPL mutations. Enzyme replacement therapy is now available for affected patients with onset of the disease during childhood and adolescence. Early results of enzyme replacement therapy are encouraging. However, a multidisciplinary approach remains the core of the treatment including nutritional support, monitoring of vitamin D, calcium and phosphate levels, physical therapy and regular dental care.

摘要

本综述介绍了关于低磷酸酯酶症诊断和治疗的当前知识,低磷酸酯酶症是一种由组织非特异性碱性磷酸酶(TNSALP)基因突变引起的罕见遗传病。低磷酸酯酶症的临床谱差异很大,从致死性婴儿型到成人诊断出的轻型。尽管该疾病很少见,但正确诊断对于提供适当治疗以及避免使用双膦酸盐等有害药物导致病情恶化很重要。血清碱性磷酸酶(ALP)值低是低磷酸酯酶症的主要特征,但仅凭此不足以诊断,因为在不同情况下也可能出现。通过ALP水平降低、ALP底物(PLP、PEA、PPi)升高和典型症状相结合可确立诊断,并可通过ALPL突变的基因检测予以证实。酶替代疗法现可用于儿童期和青春期发病的受影响患者。酶替代疗法的早期结果令人鼓舞。然而,多学科方法仍然是治疗的核心,包括营养支持、监测维生素D、钙和磷酸盐水平、物理治疗以及定期口腔护理。

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