Circulating B Cell‐Derived Small RNA Delivered by Extracellular Vesicles: A Dialogue Mechanism for Long‐Range Targeted Renal Mitochondrial Injury in Obesity

Author:

Li Xiaqing12ORCID,Yang Wah34,Ma Ke12,Zheng Zirun12,Liu Xiayun12,Hu Bo1,Liu Huanhuan1,Zhao Qian5,Han Yi6,Xiao Zhangzhang17,Chen Ruichang8,Li Hongyue12,Huang Sibo9,Liu Jinfeng10,Wang Cunchuan34,Yin Lianghong111,Meng Yu1212

Affiliation:

1. Institute of Nephrology and Blood Purification The First Affiliated Hospital of Jinan University Jinan University Guangzhou Guangdong 510632 China

2. Nephrology department The Fifth Affiliated Hospital (Heyuan Shenhe People's Hospital) Jinan University Heyuan Guangdong 517000 China

3. Department of Obesity and Metabolic Disorders The First Affiliated Hospital of Jinan University Jinan University Guangzhou Guangdong 510632 China

4. Institute of Obesity and Metabolic Disorders Jinan University Guangzhou Guangdong 510632 China

5. Department of Infectious Diseases and Hepatology Center Nanfang Hospital Southern Medical University Guangzhou Guangdong 510400 China

6. Traditional Chinese Medicine Department People's Hospital of Yanjiang District Ziyang Sichuan 641300 China

7. Department of Nephrology Houjie Hospital of Dongguan Dongguan Guangdong 523945 China

8. Department of Emergency Medicine The First Affiliated Hospital of Jinan University Jinan University Guangzhou Guangdong 510632 China

9. Health Management Center The First Affiliated Hospital of Jinan University Jinan University Guangzhou Guangdong 510632 China

10. Department of Gastroenterology Binhaiwan Central Hospital of Dongguan Dongguan Guangdong 523000 China

11. Huangpu Institute of Materials Guangzhou Guangdong 510663 China

12. Nephrology Department and Guangdong Provincial Key Laboratory of Spine and Spinal Cord Reconstruction The Fifth Affiliated Hospital (Heyuan Shenhe People's Hospital) Jinan University Heyuan Guangdong 517000 China

Abstract

AbstractThe intricate processes that govern the interactions between peripatetic immune cells and distal renal injury in obesity are not fully understood. Employing transcriptomic analysis of circulating extracellular vesicles (EVs), a marked amplification of small RNA (miR‐3960) is discerned within CD3CD19+ B cells. This RNA is found to be preferentially augmented in kidney tissues, contrasting with its subdued expression in other organs. By synthesizing dual‐luciferase reporter assay with co‐immunoprecipitation analysis, it is pinpointed that miR‐3960 specifically targets the nuclear gene TRMT5, a pivotal actor in the methylation of mitochondrial tRNA. This liaison instigates aberrations in the post‐transcriptional modifications of mitochondrial tRNA, engendering deficiencies within the electron respiratory chain, primarily attributable to the diminution of the mitochondrial bioenergetic compound (NDUFA7) complex I. Such perturbations lead to a compromised mitochondrial respiratory capacity in renal tubular cells, thereby exacerbating tubular injury. In contrast, EV blockade or miR‐3960 depletion markedly alleviates renal tubular injury in obesity. This investigation unveils a hitherto unexplored pathway by which obesity‐induced circulating immune cells remotely manipulate mitochondrial metabolism in target organs. The strategic targeting of obese EVs or infiltrative immune cells and their specifically secreted RNAs emerges as a promising therapeutic avenue to forestall obesity‐related renal afflictions.

Funder

National Natural Science Foundation of China

Basic and Applied Basic Research Foundation of Guangdong Province

Publisher

Wiley

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