Back to Search Start Over

The lysosomal proteome of senescent cells contributes to the senescence secretome.

Authors :
Rovira, Miguel
Sereda, Rebecca
Pladevall‐Morera, David
Ramponi, Valentina
Marin, Ines
Maus, Mate
Madrigal‐Matute, Julio
Díaz, Antonio
García, Fernando
Muñoz, Javier
Cuervo, Ana María
Serrano, Manuel
Source :
Aging Cell; Oct2022, Vol. 21 Issue 10, p1-21, 21p
Publication Year :
2022

Abstract

Senescent cells accumulate in tissues over time, favoring the onset and progression of multiple age‐related diseases. Senescent cells present a remarkable increase in lysosomal mass and elevated autophagic activity. Here, we report that two main autophagic pathways macroautophagy (MA) and chaperone‐mediated autophagy (CMA) are constitutively upregulated in senescent cells. Proteomic analyses of the subpopulations of lysosomes preferentially engaged in each of these types of autophagy revealed profound quantitative and qualitative changes in senescent cells, affecting both lysosomal resident proteins and cargo proteins delivered to lysosomes for degradation. These studies have led us to identify resident lysosomal proteins that are highly augmented in senescent cells and can be used as novel markers of senescence, such as arylsulfatase ARSA. The abundant secretome of senescent cells, known as SASP, is considered their main pathological mediator; however, little is known about the mechanisms of SASP secretion. Some secretory cells, including melanocytes, use the small GTPase RAB27A to perform lysosomal secretion. We found that this process is exacerbated in the case of senescent melanoma cells, as revealed by the exposure of lysosomal membrane integral proteins LAMP1 and LAMP2 in their plasma membrane. Interestingly, a subset of SASP components, including cytokines CCL2, CCL3, CXCL12, cathepsin CTSD, or the protease inhibitor SERPINE1, are secreted in a RAB27A‐dependent manner in senescent melanoma cells. Finally, proteins previously identified as plasma biomarkers of aging are highly enriched in the lysosomes of senescent cells, including CTSD. We conclude that the lysosomal proteome of senescent cells is profoundly reconfigured, and that some senescent cells can be highly active in lysosomal exocytosis. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
14749718
Volume :
21
Issue :
10
Database :
Complementary Index
Journal :
Aging Cell
Publication Type :
Academic Journal
Accession number :
159738154
Full Text :
https://doi.org/10.1111/acel.13707