部分过氧化物酶体增殖物激活受体(PPAR-γ)激动剂巴格列酮的降糖作用与不良反应的解离
Dissociation of antihyperglycaemic and adverse effects of partial perioxisome proliferator-activated receptor (PPAR-gamma) agonist balaglitazone.
作者信息
Larsen Philip J, Lykkegaard Kirsten, Larsen Leif K, Fleckner Jan, Sauerberg Per, Wassermann Karsten, Wulff Erik Max
机构信息
Department of Neuroscience, University of Copenhagen, The Panum Institute, Blegdamsvej 3, Denmark.
出版信息
Eur J Pharmacol. 2008 Oct 31;596(1-3):173-9. doi: 10.1016/j.ejphar.2008.08.004. Epub 2008 Aug 16.
Balaglitazone is a novel thiazolidinedione in clinical development for the treatment of type 2 diabetes. Common side effects associated with PPARgamma receptor agonists are weight gain, oedema and adipogenesis. Balaglitazone is a selective partial PPARgamma agonist and it has been speculated that such compounds have a more favourable safety margin than full agonists. We have compared impact of equi-efficacious antihyperglycaemic doses of balaglitazone with full PPARgamma agonist rosiglitazone on body fluid accumulation, cardiac enlargement, and adipogenesis. Equi-efficacious antihyperglycaemic doses (ED(90)) of balaglitazone (3 mg/kg/day) and rosiglitazone (6 mg/kg/day) were determined in male diabetic db/db mice. In adult male rats treated for up to 42 days, feeding, drinking, anthropometry, and plasma volumes were measured. Total plasma volume was measured with dye dilution technique. Compared to vehicle, rosiglitazone consistently increased food intake throughout the 42 day treatment period. In contrast, balaglitazone increased food intake in the last week of the experiment. However, both rosiglitazone and balaglitazone increased water intake. After 42 days, rosiglitazone treated rats displayed significantly elevated adiposity. Rosiglitazone increased total blood and plasma volumes throughout the treatment. Twenty-one days of balaglitazone treatment had no significant impact on blood or plasma volumes, whilst 42 days of balaglitazone increased plasma volume but to a significantly lesser extent than seen for rosiglitazone (vehicle: 46.1+/-1.5; balaglitazone: 50.8+/-1.21; rosiglitazone: 54.6+/-1.6 ml/kg). Heart weight was significantly elevated only in rosiglitazone treated animals. At doses inducing comparable antihyperglycaemic control, the full PPARgamma agonist, rosiglitazone, induces more pronounced body fluid retention and heart enlargement than seen for the partial PPARgamma agonist, balaglitazone. Thus, partial agonists may pose safer alternative to current anti-diabetic therapy with full PPARgamma agonist.
巴格列酮是一种正在临床开发用于治疗2型糖尿病的新型噻唑烷二酮类药物。与PPARγ受体激动剂相关的常见副作用包括体重增加、水肿和脂肪生成。巴格列酮是一种选择性部分PPARγ激动剂,据推测这类化合物的安全边际比完全激动剂更有利。我们比较了等效降糖剂量的巴格列酮与完全PPARγ激动剂罗格列酮对体液蓄积、心脏增大和脂肪生成的影响。在雄性糖尿病db/db小鼠中确定了巴格列酮(3毫克/千克/天)和罗格列酮(6毫克/千克/天)的等效降糖剂量(ED90)。在成年雄性大鼠中进行长达42天的治疗,测量进食量、饮水量、人体测量指标和血浆容量。用染料稀释技术测量总血浆容量。与赋形剂相比,罗格列酮在整个42天的治疗期间持续增加食物摄入量。相比之下,巴格列酮在实验的最后一周增加食物摄入量。然而,罗格列酮和巴格列酮均增加饮水量。42天后,罗格列酮治疗的大鼠出现明显的肥胖。罗格列酮在整个治疗过程中增加全血和血浆容量。巴格列酮治疗21天对血液或血浆容量没有显著影响,而巴格列酮治疗42天增加血浆容量,但增加程度明显低于罗格列酮(赋形剂:46.1±1.5;巴格列酮:50.8±1.21;罗格列酮:54.6±1.6毫升/千克)。仅在罗格列酮治疗的动物中,心脏重量显著增加。在诱导可比降糖控制的剂量下,完全PPARγ激动剂罗格列酮比部分PPARγ激动剂巴格列酮诱导更明显的体液潴留和心脏增大。因此,部分激动剂可能是目前使用完全PPARγ激动剂进行抗糖尿病治疗的更安全替代方案。
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