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The HSP co-inducer BGP-15 can prevent the metabolic side effects of the atypical antipsychotics

机译:HSP协同诱导剂BGP-15可以预防非典型抗精神病药的代谢副作用

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Weight gain and dysfunction of glucose and lipid metabolism are well-known side effects of atypical antipsychotic drugs (AAPD). Here, we address the question whether a heat-shock protein (HSP) co-inducer, insulin sensitizer drug candidate, BGP-15, can prevent AAPD-induced glucose, lipid, and weight changes. We also examined how an AAPD alters HSP expression and whether BGP-15 alters that expression. Four different experiments are reported on the AAPD BGP-15 interventions in a human trial of healthy men, a rodent animal model, and an in vitro adipocyte cell culture system. Olanzapine caused rapid insulin resistance in healthy volunteers and was associated with decreased level of HSP72 in peripheral mononuclear blood cells. Both changes were restored by the administration of BGP-15. In Wistar rats, weight gain and insulin resistance induced by clozapine were abolished by BGP-15. In 3T3L1 adipocytes, clozapine increased intracellular fat accumulation, and BGP-15 inhibited this process. Taken together, our results indicate that BGP-15 inhibits multiple metabolic side effects of atypical antipsychotics, and this effect is likely to be related to its HSP co-inducing ability.
机译:体重增加以及葡萄糖和脂质代谢的功能障碍是非典型抗精神病药物(AAPD)的众所周知的副作用。在这里,我们解决了一个问题,即热休克蛋白(HSP)协同诱导剂,胰岛素增敏剂候选物BGP-15是否可以防止AAPD诱导的葡萄糖,脂质和体重变化。我们还检查了AAPD如何更改HSP表达以及BGP-15是否更改该表达。在针对健康男人的人类试验,啮齿动物模型和体外脂肪细胞培养系统的AAPD BGP-15干预措施中,报道了四个不同的实验。奥氮平在健康志愿者中引起快速的胰岛素抵抗,并与外周单个核血细胞中HSP72水平降低有关。两项更改均通过BGP-15的管理得以恢复。在Wistar大鼠中,BGP-15消除了氯氮平诱导的体重增加和胰岛素抵抗。在3T3L1脂肪细胞中,氯氮平增加了细胞内脂肪的积累,而BGP-15抑制了这一过程。综上所述,我们的结果表明BGP-15抑制了非典型抗精神病药的多种代谢副作用,并且这种作用可能与其HSP协同诱导能力有关。

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