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向啮齿动物外周和中枢给予 Xenin 和神经降压素可抑制食物摄入。

Peripheral and central administration of xenin and neurotensin suppress food intake in rodents.

作者信息

Cooke Jennifer H, Patterson Michael, Patel Sejal R, Smith Kirsty L, Ghatei Mohammad A, Bloom Stephen R, Murphy Kevin G

机构信息

Department of Investigative Medicine, Hammersmith Hospital, Imperial College, London, UK.

出版信息

Obesity (Silver Spring). 2009 Jun;17(6):1135-43. doi: 10.1038/oby.2008.652. Epub 2009 Feb 12.

Abstract

Xenin is a 25-amino acid peptide highly homologous to neurotensin. Xenin and neurotensin are reported to have similar biological effects. Both reduce food intake when administered centrally to fasted rats. We aimed to clarify and compare the effects of these peptides on food intake and behavior. We confirm that intracerebroventricular (ICV) administration of xenin or neurotensin reduces food intake in fasted rats, and demonstrate that both reduce food intake in satiated rats during the dark phase. Xenin reduced food intake more potently than neurotensin following ICV administration. ICV injection of either peptide in the dark phase increased resting behavior. Xenin and neurotensin stimulated the release of corticotrophin-releasing hormone (CRH) from ex vivo hypothalamic explants, and administration of alpha-helical CRH attenuated their effects on food intake. Intraperitoneal (IP) administration of xenin or neurotensin acutely reduced food intake in fasted mice and ad libitum fed mice in the dark phase. However, chronic continuous or twice daily peripheral administration of xenin or neurotensin to mice had no significant effect on daily food intake or body weight. These studies confirm that ICV xenin or neurotensin can acutely reduce food intake and demonstrate that peripheral administration of xenin and neurotensin also reduces food intake. This may be partly mediated by changes in hypothalamic CRH release. The lack of chronic effects on body weight observed in our experiments suggests that xenin and neurotensin are unlikely to be useful as obesity therapies.

摘要

Xenin是一种与神经降压素高度同源的25个氨基酸的肽。据报道,Xenin和神经降压素具有相似的生物学效应。对禁食大鼠进行中枢给药时,两者均能减少食物摄入量。我们旨在阐明并比较这些肽对食物摄入和行为的影响。我们证实,脑室内(ICV)注射Xenin或神经降压素可减少禁食大鼠的食物摄入量,并证明两者均可减少饱足大鼠在黑暗期的食物摄入量。脑室内注射后,Xenin比神经降压素更有效地减少食物摄入量。在黑暗期脑室内注射任何一种肽均可增加静息行为。Xenin和神经降压素刺激离体下丘脑外植体释放促肾上腺皮质激素释放激素(CRH),而注射α-螺旋CRH可减弱它们对食物摄入的影响。腹腔内(IP)注射Xenin或神经降压素可急性减少禁食小鼠和自由进食小鼠在黑暗期的食物摄入量。然而,对小鼠进行慢性连续或每日两次外周注射Xenin或神经降压素对每日食物摄入量或体重没有显著影响。这些研究证实,脑室内注射Xenin或神经降压素可急性减少食物摄入量,并表明外周注射Xenin和神经降压素也可减少食物摄入量。这可能部分是由下丘脑CRH释放的变化介导的。我们的实验中观察到对体重缺乏慢性影响,这表明Xenin和神经降压素不太可能用作肥胖症治疗药物。

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