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一种新型胰多肽类似物对胰岛细胞谱系的有益影响。

The Beneficial Impact of a Novel Pancreatic Polypeptide Analogue on Islet Cell Lineage.

作者信息

Zhu Wuyun, Tanday Neil, Flatt Peter R, Irwin Nigel

机构信息

Diabetes Research Centre, Schools of Biomedical Science and Pharmacy, Ulster University, Co. Londonderry, Coleraine BT52 1SA, UK.

出版信息

Int J Mol Sci. 2025 Apr 29;26(9):4215. doi: 10.3390/ijms26094215.

Abstract

(Proline3)PP, or (P)PP, is an enzymatically stable, neuropeptide Y4 receptor (NPY4R)-selective, pancreatic polypeptide (PP) analogue with established weight-lowering and pancreatic islet morphology benefits in obesity-diabetes. In the current study, we now investigate the impact of twice-daily (P)PP administration (25 nmol/kg) for 11 days on islet cell lineage, using streptozotocin (STZ) diabetic Ins1;Rosa26-eYFP and Glu;Rosa26-eYFP transgenic mice with enhanced yellow fluorescent protein (eYFP) labelling of beta-cell and alpha-cells, respectively. (P)PP had no obvious impact on body weight or blood glucose levels in STZ-diabetic mice at the dose tested, but did return food intake towards control levels in Ins1Rosa26-eYFP mice. Notably, pancreatic insulin content was augmented by (P)PP treatment in both Ins1Rosa26-eYFP and Glu;Rosa26-eYFP mice, alongside enhanced beta-cell area and reduced alpha-cell area. Beneficial (P)PP-induced changes on islet morphology were consistently associated with decreased beta-cell apoptosis, while (P)PP also augmented beta-cell proliferation in Ins1Rosa26-eYFP mice. Alpha-cell turnover rates were returned towards healthy control levels by (P)PP intervention in both mouse models. In terms of islet cell lineage, increased transition of alpha- to beta-cells as well as decreased beta- to alpha-cell differentiation were shown to contribute towards the enhancement of beta-cell area in (P)PP-treated mice. Together these data reveal, for the first time, sustained NPY4R activation positively modulates beta-cell turnover, as well as islet cell plasticity, to help preserve pancreatic islet architecture following STZ-induced metabolic stress.

摘要

(脯氨酸3)胰多肽,即(P)PP,是一种酶稳定的、神经肽Y4受体(NPY4R)选择性的胰多肽(PP)类似物,在肥胖 - 糖尿病中具有既定的减肥和胰岛形态益处。在当前研究中,我们现在使用链脲佐菌素(STZ)诱导的糖尿病Ins1;Rosa26 - eYFP和Glu;Rosa26 - eYFP转基因小鼠,分别对β细胞和α细胞进行增强型黄色荧光蛋白(eYFP)标记,研究每日两次给予(P)PP(25 nmol/kg)持续11天对胰岛细胞谱系的影响。在所测试的剂量下,(P)PP对STZ糖尿病小鼠的体重或血糖水平没有明显影响,但确实使Ins1Rosa26 - eYFP小鼠的食物摄入量恢复到对照水平。值得注意的是,在Ins1Rosa26 - eYFP和Glu;Rosa26 - eYFP小鼠中,(P)PP治疗均增加了胰腺胰岛素含量,同时β细胞面积增加,α细胞面积减少。(P)PP诱导的对胰岛形态的有益变化始终与β细胞凋亡减少相关,而(P)PP还增加了Ins1Rosa26 - eYFP小鼠中的β细胞增殖。在两种小鼠模型中,(P)PP干预使α细胞周转率恢复到健康对照水平。就胰岛细胞谱系而言,在(P)PP处理的小鼠中,α细胞向β细胞的转变增加以及β细胞向α细胞的分化减少,均有助于β细胞面积的增加。这些数据首次共同揭示,持续的NPY4R激活可正向调节β细胞更新以及胰岛细胞可塑性,以帮助在STZ诱导的代谢应激后维持胰岛结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a8d/12071604/f7f1df93ed20/ijms-26-04215-g001.jpg

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