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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Soluble factors influencing the neural stem cell niche in brain physiology, inflammation, and aging
Cory M. Willis,Alexandra M. Nicaise,Grzegorz Krzak,Rosana-Bristena Ionescu,Vassiliki Pappa,Andrea D'Angelo,Ravi Agarwal,Maria Repollés-de-Dalmau,Luca Peruzzotti-Jametti,Stefano Pluchino +9 more
TL;DR: In this paper , the authors highlight the main intrinsic and extrinsic regulators of neural stem cell function under homeostatic and inflammatory conditions including those trafficked within extracellular membrane vesicles.
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Shared genetic and epigenetic changes link aging and cancer.
TL;DR: In this article , a review of the genetic and epigenetic changes associated with normal aging and the mechanisms responsible for these changes is presented, highlighting the possible impacts of the normal aging process on malignant transformation.
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Periodontal Disease and Senescent Cells: New Players for an Old Oral Health Problem?
TL;DR: This review hypothesizes that sustained Gram-negative bacterial challenge, chronic inflammation itself, and the constant renewal of damaged tissues create a permissive environment for the abnormal accumulation of senescent cells, and proposes a model in which the dysfunctional presence of senescence may aggravate the initial immune reaction against pathogens.
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SASP-Dependent Interactions between Senescent Cells and Platelets Modulate Migration and Invasion of Cancer Cells.
Claudio Valenzuela,Ricardo Quintanilla,Alexandra Olate-Briones,Whitney Venturini,Daniel Mancilla,Angel Cayo,Rodrigo Moore-Carrasco,Nelson E. Brown +7 more
TL;DR: Overall, platelets have prominent effects on migration, while factors secreted by senescent cells tend to promote invasion, which likely reflects differences in the specific arrays of secreted senescence-associated factors, specific factors released by platelets upon activation, and the susceptibility of target cells to respond to these agents.
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The combination of mitogenic stimulation and DNA damage induces chondrocyte senescence
M.E. Copp,M.E. Copp,M.C. Flanders,M.C. Flanders,R. Gagliardi,Jessica M. Gilbertie,Garrett A. Sessions,S. Chubinskaya,Richard F. Loeser,Lauren V. Schnabel,Lauren V. Schnabel,Brian O. Diekman,Brian O. Diekman +12 more
TL;DR: Treatment of cartilage explants with mitogenic stimuli in the context of cellular damage reliably induces high levels of SA-β-gal activity and other senescence markers, which provides a physiologically relevant model system to investigate the mechanisms of senescences induction.
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