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经皮光热-药物疗法重塑脂肪组织治疗肥胖和代谢紊乱。

Transdermal Photothermal-Pharmacotherapy to Remodel Adipose Tissue for Obesity and Metabolic Disorders.

机构信息

School of Chemical and Biomedical Engineering, Nanyang Technological University, 637457, Singapore.

Affiliated Tumor Hospital, Guangxi Medical University, Nanning 530021, P.R. China.

出版信息

ACS Nano. 2022 Feb 22;16(2):1813-1825. doi: 10.1021/acsnano.1c06410. Epub 2022 Jan 3.

Abstract

Despite the increasing prevalence of obesity, the current medications, which act indirectly on the central nervous system to suppress appetite or on the gastrointestinal tract to inhibit fat absorption, suffer from poor effectiveness and side effects. Here, we developed a transdermal mild photothermal therapy directly acting on the root of evil (subcutaneous white adipose depot) to induce its ameliorating remodeling (browning, lipolysis, and apoptosis), based on the injectable thermoresponsive hydrogel encapsulated with copper sulfide nanodots. Further, combining pharmaceutical therapy with codelivery of mirabegron leads to a strong therapeutic synergy. This method not only ensures high effectiveness and low side effects due to localized and targeted application but also remotely creates significant improvements in systemic metabolism. Specifically, as compared to the untreated group, it totally inhibits obesity development in high-fat-diet fed mice (15% less in body weight) with decreased masses of both subcutaneous (40%) and visceral fats (54%), reduced serum levels of cholesterol (54%)/triglyceride (18%)/insulin (74%)/glucose (45%), and improved insulin sensitivity (65% less in insulin resistance index). This self-administrable method is amenable for long-term home-based treatment. Finally, multiple interconnected signaling pathways are revealed, providing mechanistic insights to develop effective strategies to combat obesity and associated metabolic disorders.

摘要

尽管肥胖症的患病率不断上升,但目前的药物通过间接作用于中枢神经系统来抑制食欲,或通过作用于胃肠道来抑制脂肪吸收,其效果和副作用都不尽如人意。在这里,我们基于包封硫化铜纳米点的可注射温敏水凝胶,开发了一种直接作用于病根(皮下白色脂肪库)的透皮温和光热疗法,以诱导其改善重塑(褐色、脂肪分解和细胞凋亡)。此外,将药物治疗与米拉贝隆的共递送相结合,可产生强烈的治疗协同作用。这种方法不仅由于局部和靶向应用而确保了高效性和低副作用,而且还能远程显著改善全身代谢。具体来说,与未治疗组相比,它完全抑制了高脂肪饮食喂养的小鼠的肥胖发展(体重减轻 15%),同时皮下脂肪(减少 40%)和内脏脂肪(减少 54%)、血清胆固醇(减少 54%)/甘油三酯(减少 18%)/胰岛素(减少 74%)/葡萄糖(减少 45%)水平降低,胰岛素敏感性提高(胰岛素抵抗指数降低 65%)。这种自我管理的方法适用于长期家庭治疗。最后,揭示了多个相互关联的信号通路,为开发有效策略来对抗肥胖症和相关代谢紊乱提供了机制见解。

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