A plasma proteomic signature links secretome of senescent monocytes to aging- and obesity-related clinical outcomes in humans

Author:

Basisty Nathan1ORCID,Olinger Bradley1,Banarjee Reema1ORCID,Dey Amit1,Tsitsipatis Dimitrios2,Tanaka Toshiko3,Ram Anjana1ORCID,Nyunt Thedoe1ORCID,Daya Gulzar4ORCID,Peng Zhongsheng2,Cui Linna1,Candia Julián2ORCID,Simonsick Eleanor5,Gorospe Myriam6ORCID,Walker Keenan7ORCID,Ferrucci Luigi2ORCID

Affiliation:

1. National Institute on Aging, NIH

2. National Institute on Aging

3. Longitudinal Studies Section, Translational Gerontology Branch, National Institute on Aging, National Institutes of Health

4. NIH

5. National Institute on Aging, National Institutes of Health

6. National Institute on Aging/NIH

7. Laboratory of Behavioral Neuroscience, Intramural Research Program

Abstract

Abstract

Cellular senescence increases with age and contributes to age-related declines and pathologies. We identified circulating biomarkers of senescence associated with diverse clinical traits in humans to facilitate future non-invasive assessment of individual senescence burden and efficacy testing of novel senotherapeutics. Using a novel nanoparticle-based proteomic workflow, we profiled the senescence-associated secretory phenotype (SASP) in monocytes and examined these proteins in plasma samples (N = 1060) from the Baltimore Longitudinal Study of Aging (BLSA). Machine learning models trained on monocyte SASP associated with several age-related phenotypes in a test cohort, including body fat composition, blood lipids, inflammation, and mobility-related traits, among others. Notably, a subset of SASP-based predictions, including a ‘high impact’ SASP panel that predicts age- and obesity-related clinical traits, were validated in InCHIANTI, an independent aging cohort. These results demonstrate the clinical relevance of the circulating SASP and identify relevant biomarkers of senescence that could inform future clinical studies.

Publisher

Springer Science and Business Media LLC

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