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Xenin-25[Lys13PAL]:一种新型长效酰化的xenin-25类似物,具有潜在的抗糖尿病作用。

Xenin-25[Lys13PAL]: a novel long-acting acylated analogue of xenin-25 with promising antidiabetic potential.

作者信息

Gault V A, Martin C M A, Flatt P R, Parthsarathy V, Irwin N

机构信息

SAAD Centre for Pharmacy and Diabetes, School of Biomedical Sciences, University of Ulster, Coleraine, BT52 1SA, UK.

出版信息

Acta Diabetol. 2015 Jun;52(3):461-71. doi: 10.1007/s00592-014-0681-0. Epub 2014 Nov 6.

Abstract

AIMS

Xenin-25 is co-secreted with glucose-dependent insulinotropic polypeptide (GIP) from intestinal K-cells following a meal. Xenin-25 is believed to play a key role in glucose homoeostasis and potentiate the insulinotropic effect of GIP.

METHODS

This study investigated the effects of sub-chronic administration of the stable and longer-acting xenin-25 analogue, xenin-25[Lys(13)PAL] (25 nmol/kg), in diabetic mice fed with a high-fat diet.

RESULTS

Initial studies confirmed the significant persistent glucose-lowering (p < 0.05) and insulin-releasing (p < 0.05) actions of xenin-25[Lys(13)PAL] compared with native xenin-25. Interestingly, xenin-25 retained significant glucose-lowering activity in GIP receptor knockout mice. Twice-daily intraperitoneal (i.p.) injection of xenin-25[Lys(13)PAL] for 14 days had no significant effect on food intake or body weight in high-fat-fed mice. Non-fasting glucose and insulin levels were also unchanged, but overall glucose levels during an i.p. glucose tolerance and oral nutrient challenge were significantly (p < 0.05) lowered by xenin-25[Lys(13)PAL] treatment. These changes were accompanied by significant improvements in i.p. (p < 0.05) and oral (p < 0.001) nutrient-stimulated insulin concentrations. No appreciable changes in insulin sensitivity were observed between xenin-25[Lys(13)PAL] and saline-treated high-fat mice. However, xenin-25[Lys(13)PAL] treatment restored notable sensitivity to the biological actions of exogenous GIP injection. Consumption of O2, production of CO2, respiratory exchange ratio and energy expenditure were not altered by 14-day twice-daily treatment with xenin-25[Lys(13)PAL]. In contrast, ambulatory activity was significantly (p < 0.05 to p < 0.001) increased during the dark phase in xenin-25[Lys(13)PAL] mice compared with high-fat controls.

CONCLUSIONS

These data indicate that sustained administration of a stable analogue of xenin-25 exerts a spectrum of beneficial metabolic effects in high-fat-fed mice.

摘要

目的

进食后,肠K细胞会将异种肽-25与葡萄糖依赖性促胰岛素多肽(GIP)共同分泌。据信,异种肽-25在葡萄糖稳态中起关键作用,并增强GIP的促胰岛素作用。

方法

本研究调查了对高脂饮食喂养的糖尿病小鼠亚慢性给予稳定且长效的异种肽-25类似物异种肽-25[赖氨酸(13)聚丙交酯](25 nmol/kg)的效果。

结果

初步研究证实,与天然异种肽-25相比,异种肽-25[赖氨酸(13)聚丙交酯]具有显著的持续降糖作用(p < 0.05)和促胰岛素释放作用(p < 0.05)。有趣的是,异种肽-25在GIP受体敲除小鼠中仍保留显著的降糖活性。对高脂喂养的小鼠每日腹腔注射(i.p.)两次异种肽-25[赖氨酸(13)聚丙交酯],持续14天,对其食物摄入量或体重无显著影响。非空腹血糖和胰岛素水平也未改变,但在腹腔注射葡萄糖耐量试验和口服营养刺激试验期间,异种肽-25[赖氨酸(13)聚丙交酯]治疗显著(p < 0.05)降低了总体血糖水平。这些变化伴随着腹腔注射(p < 0.05)和口服(p < 0.001)营养刺激胰岛素浓度的显著改善。在异种肽-25[赖氨酸(13)聚丙交酯]和生理盐水处理的高脂小鼠之间,未观察到胰岛素敏感性有明显变化。然而,异种肽-25[赖氨酸(13)聚丙交酯]治疗恢复了对外源性GIP注射生物作用的显著敏感性。每日两次用异种肽-25[赖氨酸(13)聚丙交酯]治疗14天,未改变氧气消耗、二氧化碳产生、呼吸交换率和能量消耗。相反,与高脂对照组相比,异种肽-25[赖氨酸(13)聚丙交酯]处理的小鼠在黑暗期的活动显著增加(p < 0.05至p < 0.001)。

结论

这些数据表明,持续给予稳定的异种肽-25类似物对高脂喂养的小鼠具有一系列有益的代谢作用。

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