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瑞格列奈对餐时血糖调节的综述:是解决2型糖尿病治疗中低血糖问题的方法吗?

Review of prandial glucose regulation with repaglinide: a solution to the problem of hypoglycaemia in the treatment of Type 2 diabetes?

作者信息

Nattrass M, Lauritzen T

机构信息

University Hospital Birmingham NHS Trust, Selly Oak Hospital, UK.

出版信息

Int J Obes Relat Metab Disord. 2000 Sep;24 Suppl 3:S21-31. doi: 10.1038/sj.ijo.0801422.

Abstract

Type 2 diabetes mellitus is characterised by abnormal beta-cell function (present at the time of diagnosis) that is often associated with insulin resistance. An important and consistent pathophysiological finding is the failure to produce adequate increments in insulin secretion in response to carbohydrate intake. Therefore, insulin secretagogue therapy, particularly when focused on prandial glucose regulation, is a logical approach to treatment because it addresses one of the most fundamental pathophysiological aspects of the disease. However, the traditional secretagogues-the sulphonylureas--have long been associated with the unwanted effect of hypoglycaemia. This is particularly likely to occur when drugs with lengthy plasma half-lives, prolonged drug-receptor interactions, active metabolites or a reliance on renal clearance are used. The problem is most prevalent in elderly patients, where sulphonylurea-induced hypoglycaemia may be related to failure to comply with strict mealtimes or the need for supplementary food intake, often in the context of compromised renal function. Data from large-scale outcome studies demonstrate that when tight glycaemic control is achieved through aggressive antidiabetic therapy, late diabetic complications can be significantly reduced. However, the pursuit of stricter HbA1c targets with more aggressive interventions may increase the risk of hypoglycaemia. This is an irony because the clinical need to avoid hypoglycaemia and patients' apprehension of it present barriers to the achievement of beneficial glycaemic targets. However, an increased risk of hypoglycaemia may not be inevitable with insulin secretagogue therapy. The recently introduced carbamoylmethyl benzoic acid derivative, repaglinide, has pharmacological properties that are well suited to its intended role as a prandial glucose regulator. When taken prior to main meals, the rapid onset and relatively short duration of action of repaglinide aid disposal of the mealtime glucose load, without continued stimulation of pancreatic beta-cells in the postprandial fasting period. Repaglinide is also characterised by hepatic metabolism and elimination, which is an advantage in the context of impaired renal function. Prandial glucose regulation with repaglinide selectively increases insulin secretion, and hence limits glucose excursions, in the prandial phase. If a meal is omitted, so too is the corresponding dose. This more flexible approach to the management of Type 2 diabetes has a number of advantages when compared with the fixed daily dosing regimens of sulphonylureas, among them a reduced risk of hypoglycaemia--a benefit that is particularly marked in the context of missed or irregular meals.

摘要

2型糖尿病的特征是β细胞功能异常(诊断时即存在),且常与胰岛素抵抗相关。一个重要且一致的病理生理发现是,机体无法对碳水化合物摄入产生足够的胰岛素分泌增量。因此,胰岛素促分泌剂治疗,尤其是专注于餐时血糖调节时,是一种合理的治疗方法,因为它解决了该疾病最基本的病理生理问题之一。然而,传统的促分泌剂——磺脲类药物——长期以来一直与低血糖这一不良作用相关。当使用血浆半衰期长、药物-受体相互作用时间延长、有活性代谢产物或依赖肾脏清除的药物时,这种情况尤其容易发生。这个问题在老年患者中最为普遍,在老年患者中,磺脲类药物引起的低血糖可能与未能严格遵守进餐时间或需要补充食物摄入有关,这通常发生在肾功能受损的情况下。大规模结局研究的数据表明,通过积极的抗糖尿病治疗实现严格的血糖控制时,糖尿病晚期并发症可显著减少。然而,采用更积极的干预措施追求更严格的糖化血红蛋白(HbA1c)目标可能会增加低血糖风险。这颇具讽刺意味,因为避免低血糖的临床需求以及患者对低血糖的担忧成为实现有益血糖目标的障碍。然而,胰岛素促分泌剂治疗不一定会增加低血糖风险。最近推出的氨甲酰甲基苯甲酸衍生物瑞格列奈具有一些药理特性,非常适合其作为餐时血糖调节剂的预期作用。在主餐前服用时,瑞格列奈起效迅速且作用持续时间相对较短,有助于处理餐时的葡萄糖负荷,而不会在餐后禁食期持续刺激胰腺β细胞。瑞格列奈还具有经肝脏代谢和清除的特点,在肾功能受损的情况下这是一个优势。瑞格列奈进行餐时血糖调节可在餐时选择性增加胰岛素分泌,从而限制血糖波动。如果遗漏一餐,相应剂量也可不服用。与磺脲类药物固定的每日给药方案相比,这种更灵活的2型糖尿病管理方法有许多优点,其中包括低血糖风险降低——在错过或不规律进餐的情况下,这一益处尤为明显。

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