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Everolimus improves memory and learning while worsening depressive- and anxiety-like behavior in an animal model of depression

机译:埃弗洛米斯改善了记忆和学习,同时在抑郁症的动物模型中恶化和焦虑的行为恶化

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Everolimus (EVR) is an orally-administered rapamycin analog that selectively inhibits the mammalian target of rapamycin (mTOR) kinase (mainly mTORC1 and likely mTORC2) and the related signaling pathway. mTOR is a serine/threonine protein kinase regulating multiple important cellular functions; dysfunction of mTOR signaling has also been implicated in the pathophysiology of several neurological, neurodegenerative, developmental and cognitive disorders. EVR is widely used as an anti-neoplastic therapy and more recently in children with tuberous sclerosis complex (TSC). However, no clear correlation exists between EVR use and development of central side effects e.g. depression, anxiety or cognitive impairment. We studied the effects of a 3 weeks administration of EVR in mice chronically treated with betamethasone 21-phosphate disodium (BTM) as a model of depression and cognitive decline. EVR treatment had detrimental effects on depressive- and anxiety-like behavior while improving cognitive performance in both control (untreated) and BTM-treated mice. Such effects were accompanied by an increased hippocampal neurogenesis and synaptogenesis. Our results therefore might support the proposed pathological role of mTOR dysregulation in depressive disorders and confirm some previous data on the positive effects of mTOR inhibition in cognitive decline. We also show that EVR, possibly through mTOR inhibition, may be linked to the development of anxiety. The increased hippocampal neurogenesis by EVR might explain its ability to improve cognitive function or protect from cognitive decline. Our findings suggest some caution in the use of EVR, particularly in the developing brain; patients should be carefully monitored for their psychiatric/neurological profiles in any clinical situation where an mTOR inhibitor and in particular EVR is used e.g. cancer treatment, TSC or immunosuppression. (C) 2016 Elsevier Ltd. All rights reserved.
机译:everolimus(EVR)是口服施用的雷帕霉素类似物,其选择性地抑制雷帕霉素(MTOR)激酶(主要是MTORC1和可能MTORC2)的哺乳动物靶标和相关信号通路。 MTOR是一种丝氨酸/苏氨酸蛋白激酶调节多重重要的细胞功能; MTOR信号传导的功能障碍也涉及几种神经系统,神经变性,发育和认知障碍的病理生理学。 EVR广泛用作抗肿瘤治疗,最近在患有结核硬化复合体(TSC)的儿童中。然而,EVR使用与中央副作用的开发之间不存在明确的相关性。抑郁,焦虑或认知障碍。我们研究了3周给予慢性处理的小鼠EVR的效果为β塞米松21-磷酸二钠(BTM)作为抑郁和认知下降的模型。 EVR治疗对抑郁和焦虑的行为有不利影响,同时提高控制(未处理)和BTM处理的小鼠中的认知性能。这种效果伴有海马神经发生增加和突触术。因此,我们的结果可能支持MTOR失调在抑郁症中的拟议病理作用,并确认一些关于MTOR抑制在认知下降中的积极影响的数据。我们还表明,EVR可能通过MTOR抑制,可能与焦虑的发展联系起来。 EVR的海马神经发生增加可能解释其改善认知功能或免受认知下降的能力。我们的研究结果表明,在使用EVR时,特别是在开发大脑中的谨慎;在使用MTOR抑制剂和特别EVR的任何临床情况下,应仔细监测患者的精神病/神经系统谱。癌症治疗,TSC或免疫抑制。 (c)2016 Elsevier Ltd.保留所有权利。

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