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Lixisenatide: clinical profile and available evidence

机译:利西拉来:临床概况和现有证据

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摘要

Incretin-based therapies, which exploit the physiological actions of GLP-1, have attracted interest as a novel therapeutic option for Type 2 diabetes. In particular, GLP-1 receptor agonists provide significant improvements in HbA1c, with a low risk of hypoglycemia, as well as improvements in a wide spectrum of extraglycemic factors. These drugs can be categorized as either short- or long-acting compounds. Their efficacy on glucose homeostasis and safety profiles seems to be significantly affected by pharmacokinetics, thus enabling incretin-based therapy to be tailored for each patient affected by Type 2 diabetes. This review gives an overview of pharmacological, preclinical and clinical evidence of the most recently developed short-acting GLP-1 receptor agonist lixisenatide. Medline was searched for English-language articles that evaluated pharmacodynamics, pharmacokinetics, metabolism and mechanism of action of lixisenatide. An extensive Medline and Embase search for 'lixisenatide' and 'glucagon-like peptide-1 receptor agonist' was performed, collecting all randomized clinical trial data for humans. Completed but still unpublished trials were identified through a search of the www.clinicaltrials.gov website. US FDA and EMA reviews were also searched for data from unpublished trials. The most relevant papers and meeting abstracts published up to June 2013 were identified for inclusion in this review.
机译:利用肠溶素的疗法利用GLP-1的生理作用,已引起人们的兴趣,将其作为2型糖尿病的新型治疗选择。尤其是,GLP-1受体激动剂可显着改善HbA1c,降低低血糖风险,并改善广泛的血糖外因子。这些药物可以分为短效或长效化合物。它们对葡萄糖稳态和安全性的功效似乎受到药代动力学的显着影响,因此可以为每位受2型糖尿病影响的患者量身定制基于肠降血糖素的疗法。这篇综述概述了最近开发的短效GLP-1受体激动剂利西拉来的药理,临床前和临床证据。在Medline中搜索了英语文章,这些文章评估了利西拉来的药效学,药代动力学,代谢和作用机理。进行了广泛的Medline和Embase搜索,以寻找“ lixisenatide”和“胰高血糖素样肽1受体激动剂”,收集了人类的所有随机临床试验数据。通过访问www.clinicaltrials.gov网站,可以确定已完成但尚未发表的试验。还搜索了美国FDA和EMA审查中未发表试验的数据。确定了截至2013年6月的最相关论文和会议摘要,以纳入本次审查。

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