A complex secretory program orchestrated by the inflammasome controls paracrine senescence
Juan Carlos Acosta,Ana Banito,Torsten Wuestefeld,Athena Georgilis,Peggy Janich,Jennifer P. Morton,Dimitris Athineos,Tae-Won Kang,Felix Lasitschka,Mindaugas Andrulis,Gloria Pascual,Kelly J. Morris,Sadaf Khan,Hong Jin,Gopuraja Dharmalingam,Ambrosius P. Snijders,Thomas L. Carroll,David Capper,Catrin Pritchard,Gareth J. Inman,Thomas Longerich,Owen J. Sansom,Salvador Aznar Benitah,Lars Zender,Jesús Gil +24 more
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TLDR
It is demonstrated that the SASP can cause paracrine senescence and impact on tumour suppression andSenescence in vivo and TGF-β ligands play a major role by regulating p15INK4b and p21CIP1.Abstract:
Oncogene-induced senescence (OIS) is crucial for tumour suppression. Senescent cells implement a complex pro-inflammatory response termed the senescence-associated secretory phenotype (SASP). The SASP reinforces senescence, activates immune surveillance and paradoxically also has pro-tumorigenic properties. Here, we present evidence that the SASP can also induce paracrine senescence in normal cells both in culture and in human and mouse models of OIS in vivo. Coupling quantitative proteomics with small-molecule screens, we identified multiple SASP components mediating paracrine senescence, including TGF-β family ligands, VEGF, CCL2 and CCL20. Amongst them, TGF-β ligands play a major role by regulating p15(INK4b) and p21(CIP1). Expression of the SASP is controlled by inflammasome-mediated IL-1 signalling. The inflammasome and IL-1 signalling are activated in senescent cells and IL-1α expression can reproduce SASP activation, resulting in senescence. Our results demonstrate that the SASP can cause paracrine senescence and impact on tumour suppression and senescence in vivo.read more
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A Senescence-Centric View of Aging: Implications for Longevity and Disease
TL;DR: Recent evidence that implicates cellular senescence as a central regulatory mechanism of the aging process is discussed, and mechanisms by which senescent cells drive aging and diseases are described.
Journal ArticleDOI
Whole Chromosome Instability induces senescence and promotes SASP.
Grasiella A. Andriani,Vinnycius Pereira Almeida,Francesca Faggioli,Maurizio Mauro,Wanxia Li Tsai,Laura Santambrogio,Alexander Y. Maslov,Massimo Gadina,Judith Campisi,Jan Vijg,Cristina Montagna +10 more
TL;DR: The findings suggest that W-CIN triggers premature senescence, presumably to prevent the propagation of cells with an abnormal DNA content, and that aneuploid cells that accumulate during aging in some mammalian tissues potentially contribute to age-related pathologies and inflammation through SASP secretion.
Journal ArticleDOI
Ageing induced vascular smooth muscle cell senescence in atherosclerosis
Anna K. Uryga,Martin R. Bennett +1 more
TL;DR: The evidence for accelerated biological ageing in atherosclerosis is summarized, the functional consequences of cell ageing on cells comprising the plaque, and the causal role that VSMC senescence plays in atherogenesis are summarized.
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“Social Life” of Senescent Cells: What Is SASP and Why Study It?
TL;DR: The present article aims to describe the "social" life of senescent cells: basically, SASP constitution, molecular mechanisms of its regulation, and its functional role.
Journal ArticleDOI
Autophagy and Senescence in Cancer Therapy
TL;DR: An understanding of the relationship between autophagy induction and the senescence secretory phenotype in both tumor cells and fibroblasts is likely to be relevant to current clinical efforts to exploit autophagic inhibition as a therapeutic strategy for enhancing the response of malignancies to chemotherapy or radiotherapy.
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