IGFBP5 is released by senescent cells and is internalized by healthy cells, promoting their senescence through interaction with retinoic receptors

Nicola Alessio; Domenico Aprile; Gianfranco Peluso; Valeria Mazzone; Deanira Patrone; Giovanni Di Bernardo; Umberto Galderisi

doi:10.1186/s12964-024-01469-1

Cell Communication and Signaling (Feb 2024)

IGFBP5 is released by senescent cells and is internalized by healthy cells, promoting their senescence through interaction with retinoic receptors

Nicola Alessio,
Domenico Aprile,
Gianfranco Peluso,
Valeria Mazzone,
Deanira Patrone,
Giovanni Di Bernardo,
Umberto Galderisi

Affiliations

Nicola Alessio: Department of Experimental Medicine, Luigi Vanvitelli Campania University
Domenico Aprile: Department of Experimental Medicine, Luigi Vanvitelli Campania University
Gianfranco Peluso: International Medical University UNICAMILLUS
Valeria Mazzone: Department of Experimental Medicine, Luigi Vanvitelli Campania University
Deanira Patrone: Department of Experimental Medicine, Luigi Vanvitelli Campania University
Giovanni Di Bernardo: Department of Experimental Medicine, Luigi Vanvitelli Campania University
Umberto Galderisi: Department of Experimental Medicine, Luigi Vanvitelli Campania University

DOI: https://doi.org/10.1186/s12964-024-01469-1
Journal volume & issue: Vol. 22, no. 1
pp. 1 – 17

Abstract

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Abstract Cells that are exposed to harmful genetic damage, either from internal or external sources, may undergo senescence if they are unable to repair their DNA. Senescence, characterized by a state of irreversible growth arrest, can spread to neighboring cells through a process known as the senescence-associated secretory phenotype (SASP). This phenomenon contributes to both aging and the development of cancer. The SASP comprises a variety of factors that regulate numerous functions, including the induction of secondary senescence, modulation of immune system activity, remodeling of the extracellular matrix, alteration of tissue structure, and promotion of cancer progression. Identifying key factors within the SASP is crucial for understanding the underlying mechanisms of senescence and developing effective strategies to counteract cellular senescence. Our research has specifically focused on investigating the role of IGFBP5, a component of the SASP observed in various experimental models and conditions. Through our studies, we have demonstrated that IGFBP5 actively contributes to promoting senescence and can induce senescence in neighboring cells. We have gained valuable insights into the mechanisms through which IGFBP5 exerts its pro-senescence effects. These mechanisms include its release following genotoxic stress, involvement in signaling pathways mediated by reactive oxygen species and prostaglandins, internalization via specialized structures called caveolae, and interaction with a specific protein known as RARα. By uncovering these mechanisms, we have advanced our understanding of the intricate role of IGFBP5 in the senescence process. The significance of IGFBP5 as a pro-aging factor stems from an in vivo study we conducted on patients undergoing Computer Tomography analysis. In these patients, we observed an elevation in circulating IGFBP5 levels in response to radiation-induced organismal stress. Globally, our findings highlight the potential of IGFBP5 as a promising therapeutic target for age-related diseases and cancer.

Published in Cell Communication and Signaling

ISSN: 1478-811X (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Cytology
Website: https://biosignaling.biomedcentral.com/

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Abstract

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