Elevated extracellular matrix protein 1 in circulating extracellular vesicles supports breast cancer progression under obesity conditions

被引:0
作者
Keyang Xu
Ai Fu
Zhaoyi Li
Liangbin Miao
Zhonghan Lou
Keying Jiang
Condon Lau
Tao Su
Tiejun Tong
Jianfeng Bao
Aiping Lyu
Hiu Yee Kwan
机构
[1] Hong Kong Baptist University,Centre for Cancer & Inflammation Research, School of Chinese Medicine
[2] Zhejiang Chinese Medical University,Hangzhou Xixi Hospital
[3] City University of Hong Kong,Department of Physics
[4] Guangzhou University of Chinese Medicine,International Institute for Translational Chinese Medicine, School of Pharmaceutical Science
[5] Hong Kong Baptist University,Department of Mathematics
[6] Hong Kong Baptist University,Institute of Systems Medicine and Health Sciences
[7] Hong Kong Baptist University,Institute of Research and Continuing Education
来源
Nature Communications | / 15卷
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摘要
The cargo content in small extracellular vesicles (sEVs) changes under pathological conditions. Our data shows that in obesity, extracellular matrix protein 1 (ECM1) protein levels are significantly increased in circulating sEVs, which is dependent on integrin-β2. Knockdown of integrin-β2 does not affect cellular ECM1 protein levels but significantly reduces ECM1 protein levels in the sEVs released by these cells. In breast cancer (BC), overexpressing ECM1 increases matrix metalloproteinase 3 (MMP3) and S100A/B protein levels. Interestingly, sEVs purified from high-fat diet-induced obesity mice (D-sEVs) deliver more ECM1 protein to BC cells compared to sEVs from control diet-fed mice. Consequently, BC cells secrete more ECM1 protein, which promotes cancer cell invasion and migration. D-sEVs treatment also significantly enhances ECM1-mediated BC metastasis and growth in mouse models, as evidenced by the elevated tumor levels of MMP3 and S100A/B. Our study reveals a mechanism and suggests sEV-based strategies for treating obesity-associated BC.
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