Aging-related defects in macrophage function are driven by MYC and USF1 transcriptional programs

doi:10.1016/j.celrep.2024.114073

. 2024 Apr 23;43(4):114073.

doi: 10.1016/j.celrep.2024.114073. Epub 2024 Apr 4.

Aging-related defects in macrophage function are driven by MYC and USF1 transcriptional programs

Affiliations

¹ Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK; Healthy Lifespan Institute, University of Sheffield, Sheffield, UK.
² Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK.
³ Department of Cardiovascular Sciences, University of Leicester, Leicester, UK; National Institute for Healthcare Research, Leicester Biomedical Research Centre, Glenfield Hospital, Leicester, UK.
⁴ School of Biosciences, University of Sheffield, Sheffield, UK.
⁵ Healthy Lifespan Institute, University of Sheffield, Sheffield, UK; Department of Autonomic Control and Systems Engineering, University of Sheffield, Sheffield, UK.
⁶ Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK; Healthy Lifespan Institute, University of Sheffield, Sheffield, UK. Electronic address: h.l.wilson@sheffield.ac.uk.
⁷ Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK; Healthy Lifespan Institute, University of Sheffield, Sheffield, UK; Biological Research Centre, Szeged, Hungary. Electronic address: e.kiss-toth@sheffield.ac.uk.

PMID: 38578825
DOI: 10.1016/j.celrep.2024.114073

Free article

Aging-related defects in macrophage function are driven by MYC and USF1 transcriptional programs

Charlotte E Moss et al. Cell Rep. 2024.

Free article

. 2024 Apr 23;43(4):114073.

doi: 10.1016/j.celrep.2024.114073. Epub 2024 Apr 4.

Authors

Affiliations

¹ Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK; Healthy Lifespan Institute, University of Sheffield, Sheffield, UK.
² Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK.
³ Department of Cardiovascular Sciences, University of Leicester, Leicester, UK; National Institute for Healthcare Research, Leicester Biomedical Research Centre, Glenfield Hospital, Leicester, UK.
⁴ School of Biosciences, University of Sheffield, Sheffield, UK.
⁵ Healthy Lifespan Institute, University of Sheffield, Sheffield, UK; Department of Autonomic Control and Systems Engineering, University of Sheffield, Sheffield, UK.
⁶ Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK; Healthy Lifespan Institute, University of Sheffield, Sheffield, UK. Electronic address: h.l.wilson@sheffield.ac.uk.
⁷ Division of Clinical Medicine, School of Medicine and Population Health, University of Sheffield, Sheffield, UK; Healthy Lifespan Institute, University of Sheffield, Sheffield, UK; Biological Research Centre, Szeged, Hungary. Electronic address: e.kiss-toth@sheffield.ac.uk.

PMID: 38578825
DOI: 10.1016/j.celrep.2024.114073

Abstract

Macrophages are central innate immune cells whose function declines with age. The molecular mechanisms underlying age-related changes remain poorly understood, particularly in human macrophages. We report a substantial reduction in phagocytosis, migration, and chemotaxis in human monocyte-derived macrophages (MDMs) from older (>50 years old) compared with younger (18-30 years old) donors, alongside downregulation of transcription factors MYC and USF1. In MDMs from young donors, knockdown of MYC or USF1 decreases phagocytosis and chemotaxis and alters the expression of associated genes, alongside adhesion and extracellular matrix remodeling. A concordant dysregulation of MYC and USF1 target genes is also seen in MDMs from older donors. Furthermore, older age and loss of either MYC or USF1 in MDMs leads to an increased cell size, altered morphology, and reduced actin content. Together, these results define MYC and USF1 as key drivers of MDM age-related functional decline and identify downstream targets to improve macrophage function in aging.

Keywords: CP: Immunology; MYC; USF1; aging; innate immune function; longevity; macrophage; monocyte; upstream stimulatory factor.

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Conflict of interest statement

Declaration of interests The authors declare no competing interests.

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Aging-related defects in macrophage function are driven by MYC and USF1 transcriptional programs

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Aging-related defects in macrophage function are driven by MYC and USF1 transcriptional programs

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