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朊病毒病的治疗方法。

Therapeutic approaches for prion disorders.

作者信息

Ludewigs Heike, Zuber Chantal, Vana Karen, Nikles Daphne, Zerr Inga, Weiss Stefan

机构信息

Laboratorium für Molekulare Biologie, Genzentrum, Institut für Biochemie der LMU München, München, Germany.

出版信息

Expert Rev Anti Infect Ther. 2007 Aug;5(4):613-30. doi: 10.1586/14787210.5.4.613.

Abstract

Prion diseases are lethal for both humans and animals, and affected individuals die after several months following a rapid disease progression. Although researchers have attempted for decades to develop effective therapeutics for the therapy of human prion disorders, until now no efficient drug has been available on the market for transmissible spongiform encephalopathy (TSE) treatment or cure. Approximately 200 patients worldwide have died or suffer from variant Creutzfeldt-Jakob disease (CJD). Incidences for sporadic and familial CJD are approximately 1.5-2 per million per year and one per 10 million per year, respectively, in Europe. This review summarizes classical and modern trials for the development of effective anti-TSE drugs, introduces potential effective delivery systems, such as lentiviral and adeno-associated virus systems for antiprion components, including antibodies and siRNAs, and presents vaccination trials. Most of the antiprion drugs target prion protein PrP(c) and/or PrP(Sc). Alternative targets are receptors and coreceptors for PrP, that is, the 37/67-kDa laminin receptor and heparan sulfate proteoglycanes. We review clinical trials for the treatment of TSEs and describe hindrances and chances for a breakthrough in therapy of prion disorders.

摘要

朊病毒疾病对人类和动物都是致命的,患病个体在疾病快速进展后的几个月内死亡。尽管几十年来研究人员一直试图开发有效的疗法来治疗人类朊病毒疾病,但迄今为止,市场上还没有有效的药物可用于治疗或治愈传染性海绵状脑病(TSE)。全球约有200名患者死于变异型克雅氏病(CJD)或患有该病。在欧洲,散发性和家族性CJD的发病率分别约为每年每百万人口1.5 - 2例和每年每千万人口1例。本综述总结了开发有效抗TSE药物的经典和现代试验,介绍了潜在的有效递送系统,如用于抗朊病毒成分(包括抗体和小干扰RNA)的慢病毒和腺相关病毒系统,并介绍了疫苗试验。大多数抗朊病毒药物靶向朊病毒蛋白PrP(c)和/或PrP(Sc)。其他靶点是PrP的受体和共受体,即37/67-kDa层粘连蛋白受体和硫酸乙酰肝素蛋白聚糖。我们综述了治疗TSE的临床试验,并描述了朊病毒疾病治疗取得突破的障碍和机遇。

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