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Bace1 依赖性淀粉样蛋白加工调节肥胖小鼠下丘脑中瘦素的敏感性。

Bace1-dependent amyloid processing regulates hypothalamic leptin sensitivity in obese mice.

机构信息

Division of Molecular and Clinical Medicine, School of Medicine, Ninewells Hospital & Medical School, Dundee, DD1 9SY, UK.

School of Life Sciences, University of Dundee, Dundee, DD1 5EH, UK.

出版信息

Sci Rep. 2018 Jan 8;8(1):55. doi: 10.1038/s41598-017-18388-6.

DOI:10.1038/s41598-017-18388-6
PMID:29311632
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5758523/
Abstract

Obesity places an enormous medical and economic burden on society. The principal driver appears to be central leptin resistance with hyperleptinemia. Accordingly, a compound that reverses or prevents leptin resistance should promote weight normalisation and improve glucose homeostasis. The protease Bace1 drives beta amyloid (Aβ) production with obesity elevating hypothalamic Bace1 activity and Aβ production. Pharmacological inhibition of Bace1 reduces body weight, improves glucose homeostasis and lowers plasma leptin in diet-induced obese (DIO) mice. These actions are not apparent in ob/ob or db/db mice, indicating the requirement for functional leptin signalling. Decreasing Bace1 activity normalises hypothalamic inflammation, lowers PTP1B and SOCS3 and restores hypothalamic leptin sensitivity and pSTAT3 response in obese mice, but does not affect leptin sensitivity in lean mice. Raising central Aβ levels in the early stage of DIO increases hypothalamic basal pSTAT3 and reduces the amplitude of the leptin pSTAT3 signal without increased inflammation. Thus, elevated Aβ promotes hypothalamic leptin resistance, which is associated with diminished whole-body sensitivity to exogenous leptin and exacerbated body weight gain in high fat fed mice. These results indicate that Bace1 inhibitors, currently in clinical trials for Alzheimer's disease, may be useful agents for the treatment of obesity and associated diabetes.

摘要

肥胖给社会带来了巨大的医疗和经济负担。主要驱动因素似乎是中枢瘦素抵抗伴高瘦素血症。因此,一种能够逆转或预防瘦素抵抗的化合物应该能够促进体重正常化和改善葡萄糖稳态。蛋白酶 Bace1 驱动β淀粉样蛋白(Aβ)的产生,肥胖会增加下丘脑 Bace1 活性和 Aβ的产生。用 Bace1 的药理学抑制剂治疗可降低体重、改善葡萄糖稳态并降低饮食诱导肥胖(DIO)小鼠的血浆瘦素水平。在 ob/ob 或 db/db 小鼠中,这些作用并不明显,表明需要功能性瘦素信号。降低 Bace1 活性可使下丘脑炎症正常化、降低 PTP1B 和 SOCS3,并恢复肥胖小鼠下丘脑瘦素敏感性和 pSTAT3 反应,但对瘦小鼠的瘦素敏感性没有影响。在 DIO 的早期阶段升高中枢 Aβ水平会增加下丘脑基础 pSTAT3,减少瘦素 pSTAT3 信号的幅度,而不会增加炎症。因此,升高的 Aβ促进了下丘脑的瘦素抵抗,这与全身对外源瘦素的敏感性降低以及高脂肪喂养小鼠体重增加加剧有关。这些结果表明,目前正在临床试验中用于治疗阿尔茨海默病的 Bace1 抑制剂可能是治疗肥胖症和相关糖尿病的有用药物。

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