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具有协同光热和药理作用的脂肪细胞靶向纳米复合物用于对抗肥胖及相关代谢综合征

Adipocyte-Targeted Nanocomplex with Synergistic Photothermal and Pharmacological Effects for Combating Obesity and Related Metabolic Syndromes.

作者信息

Zhang Yuanyuan, Zeng Xiaojiao, Wu Fan, Yang Xiaopeng, Che Tingting, Zheng Yin, Li Jie, Zhang Yufei, Zhang Xinge, Wu Zhongming

机构信息

NHC Key Laboratory of Hormones and Development, Chu Hsien-I Memorial Hospital and Tianjin Institute of Endocrinology, Tianjin Medical University, Tianjin 300134, China.

Tianjin Key Laboratory of Metabolic Diseases, Tianjin Medical University, Tianjin 300134, China.

出版信息

Nanomaterials (Basel). 2024 Aug 19;14(16):1363. doi: 10.3390/nano14161363.

Abstract

Obesity is a global epidemic which induces a multitude of metabolic disorders. Browning of white adipose tissue (WAT) has emerged as a promising therapeutic strategy for promoting weight loss and improving associated metabolic syndromes in people with obesity. However, current methods of inducing white adipose tissue browning have limited applicability. We developed a nanocomplex pTSL@(P+I), which is a temperature-sensitive liposome (TSL) surface-conjugated with an adipocyte-targeting peptide (p) and loaded with both browning-promoting agents (P) and photosensitizing agents (I). This nanocomplex exhibits adipocyte targeting, as well as synergistic pharmacological and photothermal properties to promote browning. pTSL@(P+I) effectively upregulates UCP1 and COX5B expression by activating the transcription axis of PPARγ/PGC1α and HSF1/PGC1α, thereby promoting white adipose tissue browning and reducing obesity. This novel nanocomplex exhibited a uniform spherical shape, with an average diameter of approximately 200 nm. Additionally, the nanocomplexes exhibited remarkable photothermal properties and biocompatibility. Further, when adipocytes were treated with pTSL@(P+I), their triglyceride content decreased remarkably and intracellular mitochondrial activity increased significantly. When applied to diet-induced obesity (DIO) mice, the nanocomplex exhibited significant efficacy, demonstrating a notable 14.4% reduction in body weight from the initial measurement, a decreased fat/lean mass ratio of 20.8%, and no statistically significant disparities ( > 0.05) in associated side effects when compared to the control group. In summary, implementation of the targeted nanocomplex pTSL@(P+I) to enhance energy expenditure by stimulating white adipose tissue browning offers a promising therapeutic approach for the treatment of obesity and related metabolic syndromes.

摘要

肥胖是一种全球性流行病,会引发多种代谢紊乱。白色脂肪组织(WAT)的褐色化已成为一种有前景的治疗策略,可促进肥胖人群体重减轻并改善相关代谢综合征。然而,目前诱导白色脂肪组织褐色化的方法适用性有限。我们开发了一种纳米复合物pTSL@(P+I),它是一种温度敏感脂质体(TSL),表面偶联了脂肪细胞靶向肽(p),并负载了促褐色化剂(P)和光敏剂(I)。这种纳米复合物具有脂肪细胞靶向性,以及促进褐色化的协同药理和光热特性。pTSL@(P+I)通过激活PPARγ/PGC1α和HSF1/PGC1α转录轴有效上调UCP1和COX5B表达,从而促进白色脂肪组织褐色化并减轻肥胖。这种新型纳米复合物呈均匀球形,平均直径约为200纳米。此外,纳米复合物表现出显著的光热特性和生物相容性。进一步研究发现,用pTSL@(P+I)处理脂肪细胞后,其甘油三酯含量显著降低,细胞内线粒体活性显著增加。将该纳米复合物应用于饮食诱导肥胖(DIO)小鼠时,显示出显著疗效,与初始测量值相比体重显著降低了14.4%,脂肪/瘦体重比降低了20.8%,与对照组相比相关副作用无统计学显著差异(>0.05)。总之,采用靶向纳米复合物pTSL@(P+I)通过刺激白色脂肪组织褐色化来增加能量消耗,为肥胖及相关代谢综合征的治疗提供了一种有前景的治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/de89/11357138/eca75df79428/nanomaterials-14-01363-sch001.jpg

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