Enhanced insulin‐regulated phagocytic activities support extreme health span and longevity in multiple populations

Author:

Wu Deng1,Bi Xiaoman23,Li Peihu2,Xu Dahua2,Qiu Jianmin3,Li Kongning2ORCID,Zheng Shaojiang3,Chow Kim Hei‐Man1ORCID

Affiliation:

1. School of Life Sciences, Faculty of Science The Chinese University of Hong Kong Hong Kong

2. Key Laboratory of Tropical Translational Medicine of Ministry of Education, College of Biomedical Information and Engineering Hainan Medical University Haikou China

3. Key Laboratory of Tropical Cardiovascular Diseases Research of Hainan Province Tumor Institute of The First Affiliated Hospital, Hainan Women and Children Medical Center, Hainan Medical University Haikou China

Abstract

AbstractThe immune system plays a central role in many processes of age‐related disorders and it remains unclear if the innate immune system may play roles in shaping extreme longevity. By an integrated analysis with multiple bulk and single cell transcriptomic, so as DNA methylomic datasets of white blood cells, a previously unappreciated yet commonly activated status of the innate monocyte phagocytic activities is identified. Detailed analyses revealed that the life cycle of these monocytes is enhanced and primed to a M2‐like macrophage phenotype. Functional characterization unexpectedly revealed an insulin‐driven immunometabolic network which supports multiple aspects of phagocytosis. Such reprogramming is associated to a skewed trend of DNA demethylation at the promoter regions of multiple phagocytic genes, so as a direct transcriptional effect induced by nuclear‐localized insulin receptor. Together, these highlighted that preservation of insulin sensitivity is a key to healthy lifespan and extended longevity, via boosting the function of innate immune system in advanced ages.

Funder

Alzheimer's Association

Publisher

Wiley

Subject

Cell Biology,Aging

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