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脑室内注射尿皮质素3通过大鼠体内的促肾上腺皮质激素释放因子受体2抵消中枢酰基胃饥饿素诱导的摄食亢进和胃促动力作用。

Intracerebroventricular urocortin 3 counteracts central acyl ghrelin-induced hyperphagic and gastroprokinetic effects via CRF receptor 2 in rats.

作者信息

Yeh Chun, Ting Ching-Heng, Doong Ming-Luen, Chi Chin-Wen, Lee Shou-Dong, Chen Chih-Yen

机构信息

Division of Gastroenterology, Department of Internal Medicine, Cheng-Hsin General Hospital.

Department of Pathology, Mackay Memorial Hospital.

出版信息

Drug Des Devel Ther. 2016 Oct 3;10:3281-3290. doi: 10.2147/DDDT.S113195. eCollection 2016.

Abstract

PURPOSE

Urocortin 3 is a key neuromodulator in the regulation of stress, anxiety, food intake, gut motility, and energy homeostasis, while ghrelin elicits feeding behavior and enhances gastric emptying, adiposity, and positive energy balance. However, the interplays between urocortin 3 and ghrelin on food intake and gastric emptying remain uninvestigated.

METHODS

We examined the differential effects of central --octanoylated ghrelin, des-Gln-ghrelin, and urocortin 3 on food intake, as well as on charcoal nonnutrient semiliquid gastric emptying in conscious rats that were chronically implanted with intracerebroventricular (ICV) catheters. The functional importance of corticotropin-releasing factor (CRF) receptor 2 in urocortin 3-induced responses was examined by ICV injection of the selective CRF receptor 2 antagonist, astressin-B.

RESULTS

ICV infusion of urocortin 3 opposed central acyl ghrelin-elicited hyperphagia via CRF receptor 2 in satiated rats. ICV injection of --octanoylated ghrelin and des-Gln-ghrelin were equally potent in accelerating gastric emptying in fasted rats, whereas ICV administration of urocortin 3 delayed gastric emptying. In addition, ICV infusion of urocortin 3 counteracted central acyl ghrelin-induced gastroprokinetic effects via CRF receptor 2 pathway.

CONCLUSION

ICV-infused urocortin 3 counteracts central acyl ghrelin-induced hyperphagic and gastroprokinetic effects via CRF receptor 2 in rats. Our results clearly showed that enhancing ghrelin and blocking CRF receptor 2 signaling in the brain accelerated gastric emptying, which provided important clues for a new therapeutic avenue in ameliorating anorexia and gastric ileus found in various chronic wasting disorders.

摘要

目的

尿皮质素3是调节应激、焦虑、食物摄入、肠道蠕动和能量平衡的关键神经调节剂,而胃饥饿素可引发进食行为并增强胃排空、肥胖和正能量平衡。然而,尿皮质素3与胃饥饿素在食物摄入和胃排空方面的相互作用仍未得到研究。

方法

我们研究了中枢辛酰化胃饥饿素、去谷氨酰胺胃饥饿素和尿皮质素3对食物摄入的不同影响,以及对长期植入脑室内(ICV)导管的清醒大鼠木炭非营养半液体胃排空的影响。通过脑室内注射选择性促肾上腺皮质激素释放因子(CRF)受体2拮抗剂阿斯特辛-B,研究了CRF受体2在尿皮质素3诱导反应中的功能重要性。

结果

在饱腹大鼠中,脑室内注入尿皮质素3通过CRF受体2对抗中枢酰基胃饥饿素引起的摄食亢进。脑室内注射辛酰化胃饥饿素和去谷氨酰胺胃饥饿素在加速禁食大鼠胃排空方面同样有效,而脑室内给予尿皮质素3则延迟胃排空。此外,脑室内注入尿皮质素3通过CRF受体2途径抵消中枢酰基胃饥饿素诱导的胃促动力作用。

结论

脑室内注入尿皮质素3通过大鼠的CRF受体2抵消中枢酰基胃饥饿素诱导的摄食亢进和胃促动力作用。我们的结果清楚地表明,增强胃饥饿素并阻断大脑中的CRF受体2信号可加速胃排空,这为改善各种慢性消耗性疾病中出现的厌食和胃麻痹提供了一条新的治疗途径的重要线索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1ab/5055120/f02453411a74/dddt-10-3281Fig1.jpg

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