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阿卡波糖:一种α-葡萄糖苷酶抑制剂。

Acarbose: an alpha-glucosidase inhibitor.

作者信息

Martin A E, Montgomery P A

机构信息

Drug Information Service, University of Michigan Health System (UMHS), Ann Arbor, USA.

出版信息

Am J Health Syst Pharm. 1996 Oct 1;53(19):2277-90; quiz 2336-7. doi: 10.1093/ajhp/53.19.2277.

Abstract

The chemistry, pharmacology, pharmacokinetics, and clinical efficacy of acarbose, a new antidiabetic agent, are reviewed. Acarbose reversibly inhibits intestinal alpha-glucosidases, enzymes responsible for the metabolism of complex carbohydrates into absorbable monosaccharide units. This action results in a diminished and delayed rise in blood glucose following a meal, resulting in a reduction in post-prandial hyperglycemia, area under the glucose concentration-time curve, and glycosylated hemoglobin. Other effects include a reduction in postprandial insulin and variable changes in plasma lipid concentrations. In placebo-controlled trials, acarbose caused significant improvements in glycemic control indicators, including glycosylated hemoglobin. Acarbose has demonstrated additional glycemic control when added to other antidiabetic therapies, including sulfonylureas and insulin. Efficacy of acarbose appears to be comparable to or slightly less than that of sulfonylureas or metformin, although it has not been compared with maximal dose of these agents. The most commonly reported adverse drug reactions with acarbose are abdominal pain, diarrhea, and flatulence, which tend to lessen with time. Acarbose may affect the bioavailability of metformin and may be less effective when used in conjunction with intestinal adsorbents and digestive enzyme preparations. Concurrent use with hypoglycemic agents (sulfonylureas and insulin) may cause an increased frequency of hypoglycemia. Acarbose should not be used in individuals with certain intestinal disorders, including inflammatory bowel disease. The dosage should start at 25 mg one to three times daily given with the first bite of each main meal and should be adjusted to a maximum of 50 mg three times daily for patients weighing up to 60 kg or 100 mg three times daily for heavier patients. Acarbose may be considered for first-line antidiabetic therapy in certain patients and may be useful as combination therapy in selected instances. Acarbose is efficacious in improving metabolic control in non-insulin-dependent diabetes mellitus. Further evaluation of its effects on the long-term complications of diabetes is needed.

摘要

本文综述了新型抗糖尿病药物阿卡波糖的化学、药理学、药代动力学及临床疗效。阿卡波糖可逆性抑制肠道α-葡萄糖苷酶,该酶负责将复合碳水化合物代谢为可吸收的单糖单元。这一作用导致餐后血糖升高幅度减小且延迟,从而降低餐后高血糖、葡萄糖浓度-时间曲线下面积及糖化血红蛋白水平。其他作用包括降低餐后胰岛素水平以及血浆脂质浓度的可变变化。在安慰剂对照试验中,阿卡波糖使血糖控制指标(包括糖化血红蛋白)有显著改善。阿卡波糖与其他抗糖尿病疗法(包括磺脲类药物和胰岛素)联合使用时,显示出额外的血糖控制效果。阿卡波糖的疗效似乎与磺脲类药物或二甲双胍相当或略低,尽管尚未与这些药物的最大剂量进行比较。阿卡波糖最常报告的药物不良反应是腹痛、腹泻和胃肠胀气,这些症状往往会随时间减轻。阿卡波糖可能会影响二甲双胍的生物利用度,与肠道吸附剂和消化酶制剂联合使用时可能效果较差。与降糖药物(磺脲类药物和胰岛素)同时使用可能会增加低血糖的发生频率。阿卡波糖不应在患有某些肠道疾病(包括炎症性肠病)的个体中使用。剂量应从每餐第一口饭时服用25mg,每日1至3次开始,对于体重达6kg的患者,最大可调整至每日3次,每次50mg;对于体重更重的患者,最大可调整至每日3次,每次100mg。在某些患者中,阿卡波糖可被视为一线抗糖尿病治疗药物,在特定情况下也可作为联合治疗药物。阿卡波糖在改善非胰岛素依赖型糖尿病的代谢控制方面是有效的。需要进一步评估其对糖尿病长期并发症的影响。

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