Melander A, Bitzén P O, Faber O, Groop L
Department of Research in Primary Health Care, Lund University Health Sciences Centre, Dalby, Sweden.
Drugs. 1989 Jan;37(1):58-72. doi: 10.2165/00003495-198937010-00004.
Apart from the amelioration of symptoms, a major aim of the treatment of non-insulin-dependent diabetes mellitus (NIDDM, type 2 diabetes) should be the prevention of cardiovascular complications. These are associated with the chronic hyperglycaemia that is characteristic of NIDDM, and the risk of complications is already increased in subjects with impaired glucose tolerance (IGT). For these reasons, and because hyperglycaemia appears to be a self-perpetuating condition, treatment should be introduced as early as possible and should be aimed at normalisation of blood glucose. To enable early detection and intervention, screening is necessary. As diet regulation alone rarely suffices to normalise blood glucose, addition of sulphonylurea drugs is indicated in many cases. If introduced in the IGT phase, sulphonylureas drugs combined with diet regulation may postpone the development of IGT to manifest NIDDM, and may reduce the increased risk of cardiovascular morbidity and mortality. Sulphonylureas stimulate insulin release, possibly via interaction with receptors in the pancreatic B cells. In addition, such treatment enhances the reduced insulin action. This might be a primary effect but is also a consequence of the increased access to insulin and the subsequent reduction of hyperglycaemia. Sulphonylureas may enhance insulin availability by reducing insulin clearance. Effects on blood lipids are probably secondary phenomena. Fast and short acting sulphonylureas may improve the impaired meal-induced acute insulin release. If combined with weight-reducing diet regulation and introduced early, such treatment can maintain (near) normal blood glucose levels and an improved insulin action for several years without increasing basal insulin secretion, without chronic hyperinsulinaemia, and without weight increase. If not combined with diet regulation, sulphonylurea therapy is likely to fail. If introduced when NIDDM is advanced, the efficacy of these drugs is limited, with secondary failures developing at a rate of 5 to 10% per year. Continuous (24-hour-a-day) exposure to drug treatment could possibly desensitise the B cell to sulphonylurea stimulation. 'Second-generation' sulphonylurea drugs have a higher potency than 'first-generation' drugs, but this need not signify a greater clinical efficacy. The effect of several of these drugs may be increased if they are ingested half an hour before meal(s). Short acting sulphonylureas may be safer than long acting ones, which seem more likely to cause long lasting and fatal hypoglycaemia, at least in elderly patients.(ABSTRACT TRUNCATED AT 400 WORDS)
除了缓解症状外,非胰岛素依赖型糖尿病(NIDDM,2型糖尿病)治疗的一个主要目标应该是预防心血管并发症。这些并发症与NIDDM特有的慢性高血糖有关,而且糖耐量受损(IGT)的患者发生并发症的风险已经增加。基于这些原因,以及由于高血糖似乎是一种会自我持续的病症,治疗应尽早开始,并应以血糖正常化为目标。为了能够早期发现并进行干预,筛查是必要的。由于仅靠饮食调节很少能使血糖正常化,在许多情况下需要加用磺脲类药物。如果在IGT阶段就开始使用,磺脲类药物与饮食调节相结合可能会推迟IGT发展为显性NIDDM,并可能降低心血管疾病发病率和死亡率增加的风险。磺脲类药物可能通过与胰腺β细胞中的受体相互作用来刺激胰岛素释放。此外,这种治疗可增强降低的胰岛素作用。这可能是一种主要作用,但也是胰岛素可用性增加以及随后高血糖降低的结果。磺脲类药物可能通过减少胰岛素清除来提高胰岛素可用性。对血脂的影响可能是次要现象。速效和短效磺脲类药物可能会改善受损的餐时急性胰岛素释放。如果与减轻体重的饮食调节相结合并尽早开始,这种治疗可以在不增加基础胰岛素分泌、不导致慢性高胰岛素血症且不增加体重的情况下,维持(接近)正常血糖水平并改善胰岛素作用数年。如果不与饮食调节相结合,磺脲类药物治疗可能会失败。如果在NIDDM晚期开始使用,这些药物的疗效有限,每年会有5%至10%的继发失效情况发生。持续(一天24小时)接受药物治疗可能会使β细胞对磺脲类药物刺激产生脱敏。“第二代”磺脲类药物比“第一代”药物效力更高,但这并不一定意味着临床疗效更好。如果在饭前半小时服用,其中几种药物的效果可能会增强。短效磺脲类药物可能比长效磺脲类药物更安全,长效磺脲类药物似乎更有可能导致持久且致命的低血糖,至少在老年患者中是这样。(摘要截选至400词)
