Boyu Liu, Lei Zhu, Lei Lei, Huifang Li, Rui Cong, Jinfan Hou, Jiehui Zhao, Pengwei Li, Yiwei Tang, Zhigui Su, Jiasheng Tu, Lei Jiang
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引用次数: 0
Abstract
The accumulation of atherosclerosis plaques within arterial walls leads to cardiovascular events. Lipid‐laden macrophages, known as foam cells play a pivotal role in atherosclerotic plaque progression by disrupting cholesterol homeostasis and facilitating inflammation. This study presents a rational and multivalent nanoplatform (siTTENPs) for atherosclerosis treatment. siTTENPs can form electrostatic complexes with the nucleic acid siTRPM2, thereby reducing oxidized low‐density lipoprotein (oxLDL) uptake by foam cells and alleviating inflammation. Concurrently, β‐cyclodextrin (β‐CD) modified siTTENPs facilitate cholesterol clearance, further re‐establishing lipid homeostasis. The nanometer size and S2P peptide (CRTLLTVRKC) modification endow these particles with specific targeting capabilities toward lesional macrophages, thereby enhancing their anti‐atherosclerotic efficacy. Consequently, the siTTENPs delivery system effectively inhibits pathological cholesterol internalization while simultaneously promoting cholesterol efflux mechanisms and reducing inflammation. This therapeutic intervention leads to significant regression of atherosclerotic plaque. This study introduces an innovative therapeutic strategy aimed at improving cholesterol homeostasis, with promising implications for the treatment of atherosclerosis.
期刊介绍:
Advanced Materials, one of the world's most prestigious journals and the foundation of the Advanced portfolio, is the home of choice for best-in-class materials science for more than 30 years. Following this fast-growing and interdisciplinary field, we are considering and publishing the most important discoveries on any and all materials from materials scientists, chemists, physicists, engineers as well as health and life scientists and bringing you the latest results and trends in modern materials-related research every week.