The DNA damage response induces inflammation and senescence by inhibiting autophagy of GATA4

Kang, Chanhee; Xu, Qikai; Martin, Timothy D.; Li, Mamie Z.; Demaria, Marco; Aron, Liviu; Lu, Tao; Yankner, Bruce A.; Campisi, Judith; Elledge, Stephen J.

doi:10.1126/science.aaa5612

Cited by 701 publications

(661 citation statements)

References 66 publications

(107 reference statements)

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“…GATA4 was identified as the key mediator of SASP, which was activated by damaged DNA and able to influence multiple tissue‐remodeling in a context‐dependent manner 12. In this study, we observed increased cardiomyocytes with damaged DNA based on γ‐H2AX immunostaining in postinfarction hearts (Figure 2A).…”

Section: Resultssupporting

confidence: 50%

“…Masson staining and dual immunofluorescence staining were included to establish that cardiomyocytes underwent senescence after hypoxia. Regarding its functional role, SASP was important for senescence to participate in tissue remodeling that was maintained by transcription factor GATA4 12. In this study, we noticed an increase of GATA4 accumulation in the border zones, where the senescence markers are also highly expressed.…”

Section: Discussionsupporting

confidence: 55%

“…Upon DNA damage response, GATA4 is activated and in turn, initiates the secretion of inflammation factors by activating transcription factor NF‐kB 12. Furthermore, it was verified that GATA4‐mediated senescence and secretory phenotype are involved in multiple aging tissues including brain, skin, and liver 12. In this study, we investigated whether cardiomyocyte senescence participated in post‐AMI heart remodeling and whether the underlying mechanism is related to GATA4.…”

Section: Introductionmentioning

confidence: 90%

“…Mechanically, senescent cells can affect surrounding cells and play active roles in tissue remodeling by secreting such proteins as proinflammatory cytokines, chemokines, and growth factors (senescence‐associated secretory phenotype, SASP) 11. GATA‐binding factor 4 (GATA4) is required to maintain senescence and SASP 12. Upon DNA damage response, GATA4 is activated and in turn, initiates the secretion of inflammation factors by activating transcription factor NF‐kB 12.…”

Section: Introductionmentioning

confidence: 99%

“…GATA‐binding factor 4 (GATA4) is required to maintain senescence and SASP 12. Upon DNA damage response, GATA4 is activated and in turn, initiates the secretion of inflammation factors by activating transcription factor NF‐kB 12. Furthermore, it was verified that GATA4‐mediated senescence and secretory phenotype are involved in multiple aging tissues including brain, skin, and liver 12.…”

Section: Introductionmentioning

confidence: 99%

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Postinfarction Hearts Are Protected by Premature Senescent Cardiomyocytes Via GATA4‐Dependent CCN1 Secretion

Cui

Xue

Yang

et al. 2018

JAHA

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BackgroundStress‐induced cell premature senescence participates in a variety of tissue and organ remodeling by secreting such proteins as proinflammatory cytokines, chemokines, and growth factors. However, the role of cardiomyocyte senescence in heart remodeling after acute myocardial infarction has not been thoroughly elucidated to date. Therefore, we sought to clarify the impact of premature myocardial senescence on postinfarction heart function.Methods and ResultsSenescence markers, including p16INK 4a, p21CIP 1/ WAF 1, and SA‐β‐gal staining, were analyzed in several heart disease models by immunostaining. Both postinfarction mouse hearts and ischemic human myocardium demonstrated increased senescence markers. Additionally, senescence‐related secretory phenotype was activated after acute myocardial infarction, which upregulated senescence‐related secretory phenotype factors, including CCN family member 1 (CCN1), interleukin‐1α, tumor necrosis factor α, and monocyte chemoattractant protein‐1. In vivo, a tail vein injection of AAV9‐Gata4‐shRNA significantly attenuated senescence‐related secretory phenotype secretion and aggravated postinfarction heart dysfunction. Furthermore, among activated senescence‐related secretory phenotype factors, CCN1 administration reduced myofibroblast viability in vitro and rescued the deleterious effect of AAV9‐Gata4‐shRNA in vivo.ConclusionsMyocardial premature senescence was observed in the ischemic hearts and improved postinfarction heart function, partly through the GATA‐binding factor 4‐CCN1 pathway.

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Section: Resultssupporting

confidence: 50%

Section: Discussionsupporting

confidence: 55%

Section: Introductionmentioning

confidence: 90%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Postinfarction Hearts Are Protected by Premature Senescent Cardiomyocytes Via GATA4‐Dependent CCN1 Secretion

Cui

Xue

Yang

et al. 2018

JAHA

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Mitochondrial dysfunction and cell senescence: deciphering a complex relationship

2019

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Cellular senescence and mitochondrial dysfunction have both been defined as classical hallmarks of the ageing process. Here, we review the intricate relationship between the two. In the context of ageing, it is now well regarded that cellular senescence is a key driver in both ageing and the onset of a number of age‐related pathologies. Emerging evidence has pinpointed mitochondria as one of the key modulators in the development of the senescence phenotype, particularly the pro‐inflammatory senescence associated secretory phenotype (SASP). This review focuses on the contribution of homeostatic mechanisms, as well as of reactive oxygen species and mitochondrial metabolites in the senescence programme. Furthermore, we discuss emerging pathways and mitochondrial‐mediated mechanisms that may be influencing the SASP and, subsequently, explore how these may be exploited to open up new therapeutic avenues.

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Targeting cellular senescence to combat cancer and ageing

2022

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Senescence is a complex cellular process that is implicated in various physiological and pathological processes. It is characterized by a stable state of cell growth arrest and by a secretome of diverse pro‐inflammatory factors, chemokines and growth factors. In this review, we summarize the context‐dependent role of cellular senescence in ageing and in age‐related diseases, such as cancer. We discuss current approaches to targeting senescence to develop therapeutic strategies to combat cancer and to promote healthy ageing, and we outline our vision for future research directions for senescence‐based interventions in these fields.

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The DNA damage response induces inflammation and senescence by inhibiting autophagy of GATA4

Cited by 701 publications

References 66 publications

Postinfarction Hearts Are Protected by Premature Senescent Cardiomyocytes Via GATA4‐Dependent CCN1 Secretion

Postinfarction Hearts Are Protected by Premature Senescent Cardiomyocytes Via GATA4‐Dependent CCN1 Secretion

Mitochondrial dysfunction and cell senescence: deciphering a complex relationship

Targeting cellular senescence to combat cancer and ageing

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