The senescence-associated secretory phenotype is potentiated by feedforward regulatory mechanisms involving Zscan4 and TAK1

Zhang, Boyi; Fu, Da; Xu, Qixia; Cong, Xianling; Wu, Chunyan; Zhong, Xiaoming; Ma, Yu‐Shui; Lv, Zhongwei; Chen, Fei; Liu, Han; Qian, Min; Chin, Y. Eugene; Lam, Eric W.‐F.; Chiao, Paul J.; Sun, Yu

doi:10.1038/s41467-018-04010-4

Cited by 115 publications

(116 citation statements)

References 51 publications

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“…The biological effect of AREG is mainly mediated through its binding and activation of EGFR (also ErbB1), a widely expressed transmembrane RTK (Avraham & Yarden, ). By comparison of multiple cell lines and anticancer treatments, we showed that stromal cells are more ready to express AREG than cancer cells upon treatment by DDA agents that cause typical DNA lesions, instead of NDDA treatments that do not target DNA, a feature that is indeed shared by most of the SASP factors (Zhang et al, ). Intriguingly, AREG can be alternatively delivered via extracellular vesicles such as exosomes in the treatment‐naïve settings of multiple myeloma, non‐small‐cell lung cancer, and chronic myelogenous leukemia, each case activating the EGFR pathway in recipient cells without chemotherapy or SASP engagement in the TME (Corrado et al, ; Raimondo et al, ; Taverna et al, ).…”

Section: Discussionmentioning

confidence: 99%

“…In contrast to intrinsic resistance, which re‐exists in cancer cells before initiation of treatments, acquired resistance arises in the course of therapies and is frequently supported by the tumor‐adjacent stroma (Junttila & de Sauvage, ). For instance, cancer resistance can be driven by a treatment‐damaged TME, which is pathologically fueled by the SASP (Sun et al, , ; Zhang et al, ). Originally discovered as an essential biological feature of senescent cells, the SASP is now established as an important contributor in the development of multiple aging‐related complications, including atherosclerosis, osteoarthritis, physical frailty, and systemic inflammation (Childs et al, ; Demaria et al, ; Jeon et al, ; Zhu et al, ).…”

Section: Discussionmentioning

confidence: 99%

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Targeting amphiregulin (AREG) derived from senescent stromal cells diminishes cancer resistance and averts programmed cell death 1 ligand (PD‐L1)‐mediated immunosuppression

et al. 2019

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Aging is characterized by a progressive loss of physiological integrity, while cancer represents one of the primary pathological factors that severely threaten human lifespan and healthspan. In clinical oncology, drug resistance limits the efficacy of most anticancer treatments, and identification of major mechanisms remains a key to solve this challenging issue. Here, we highlight the multifaceted senescence‐associated secretory phenotype (SASP), which comprises numerous soluble factors including amphiregulin (AREG). Production of AREG is triggered by DNA damage to stromal cells, which passively enter senescence in the tumor microenvironment (TME), a process that remarkably enhances cancer malignancy including acquired resistance mediated by EGFR. Furthermore, paracrine AREG induces programmed cell death 1 ligand (PD‐L1) expression in recipient cancer cells and creates an immunosuppressive TME via immune checkpoint activation against cytotoxic lymphocytes. Targeting AREG not only minimized chemoresistance of cancer cells, but also restored immunocompetency when combined with classical chemotherapy in humanized animals. Our study underscores the potential of in vivo SASP in driving the TME‐mediated drug resistance and shaping an immunosuppressive niche, and provides the proof of principle of targeting major SASP factors to improve therapeutic outcome in cancer medicine, the success of which can substantially reduce aging‐related morbidity and mortality.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Targeting amphiregulin (AREG) derived from senescent stromal cells diminishes cancer resistance and averts programmed cell death 1 ligand (PD‐L1)‐mediated immunosuppression

et al. 2019

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“…As stromal cells represent the major non-cancerous mesenchymal components providing structural architecture within the tissue of most solid tumors, we chose to employ a primary normal human prostate stromal cell line, namely PSC27, to initiate the study. Composed of predominantly fibroblasts but with a minor percentage of non-fibroblast cell lineages including endothelial cells and smooth muscle cells, PSC27 develops a typical SASP after exposure to stressful insults such as cytotoxic chemotherapy or ionizing radiation [23][24][25] . We treated these cells with a pre-optimized sub-lethal dose of bleomycin (BLEO), resulting in enhanced senescence-associated βgalactosidase (SA-β-Gal) staining positivity, decreased BrdU incorporation, and elevated DNA damage foci several days afterwards ( Fig.…”

Section: Senescent Stromal Cells Generate An Increased Number Of Evsmentioning

confidence: 99%

“…Animals were sacrificed at end of the 8th week post tumor xenografting, with tumor volume measurement, tissue staining and histological examination performed as previously described 23 .…”

Section: Preclinical Studiesmentioning

confidence: 99%

Senescent stromal cells promote cancer resistance through SIRT1 loss-potentiated overproduction of small extracellular vesicles

Liu

Long

Li³

et al. 2020

Preprint

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ABSTRACTCellular senescence is a potent tumor-suppressive program that prevents neoplastic events. Paradoxically, senescent cells develop an inflammatory secretome, termed the senescence-associated secretory phenotype (SASP) and implicated in age-related pathologies including cancer. Here we report that senescent cells actively synthesize and release small extracellular vesicles (sEVs) with a distinctive size distribution. Mechanistically, SIRT1 loss supports accelerated sEV production despite enhanced proteome-wide ubiquitination, a process correlated with ATP6V1A downregulation and defective lysosomal acidification. Once released, senescent stromal sEVs significantly alter the expression profile of recipient cancer cells and enhance their aggressiveness, specifically drug resistance mediated by expression of ATP binding cassette subfamily B member 4 (ABCB4). Targeting SIRT1 with an agonist SRT2104 prevents development of cancer resistance through restraining sEV production by senescent stromal cells. In clinical oncology, sEVs in peripheral blood of posttreatment cancer patients are readily detectable by routine biotechniques, presenting a novel biomarker to monitor therapeutic efficacy and to predict long term outcome. Together, our study identifies a distinct mechanism supporting pathological activities of senescent cells, and provides a novel avenue to circumvent advanced human malignancies by co-targeting cancer cells and their surrounding microenvironment, which contributes to drug resistance via secretion of sEVs from senescent stromal cells.

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“…Given the remarkable benefit of targeting KDM4 in the treatment-damaged TME, we subsequently evaluated longer time consequences by comparing the survival terms of animals subject to different treatment modalities in a time-extended manner. Development of a bulky disease was considered once the tumor burden was prominent (e.g., when the size exceeds 2000 mm 3 ), an approach reported previously 39,40 . Mice receiving MIT/ML324 co-treatment exhibited the most prolonged median survival duration, acquiring a minimally 50% longer survival than the group treated by MIT alone (Fig.…”

Section: Upregulated Kdm4a/b Expression Is Accompanied By Decreased Hmentioning

confidence: 99%

KDM4 Orchestrates Epigenomic Remodeling of Senescent Cells and Potentiates the Senescence-Associated Secretory Phenotype

Zhang

Long

et al. 2020

Preprint

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Cellular senescence restrains the expansion of neoplastic cells through several layers of regulation, including epigenetic decoration of chromatin structure and functional modulation of bioactive components. Here we report that expression of the histone H3-specific demethylase KDM4 is upregulated in human stromal cells upon cellular senescence. In clinical oncology, upregulated KDM4 and diminished H3K9/H3K36 methylation are correlated with adverse survival of cancer patients post-chemotherapy. Global chromatin accessibility mapping via ATAC-seq and expression profiling through RNA-seq reveal extensive reorganization of chromosomes and spatiotemporal reprogramming of the transcriptomic landscape, events responsible for development of the senescence-associated secretory phenotype (SASP). Selectively targeting KDM4 dampens the SASP of senescent stromal cells and enhances the apoptotic index of cancer cells in the treatment-damaged tumor microenvironment (TME), together prolonging overall survival of experimental animals. Our study supports the dynamic change of H3K9/H3K36 methylation marks during cellular senescence, identifies an unusually permissive chromatin state, unmasks KDM4 as a key modulator of the SASP, and presents a novel therapeutic avenue to manipulate cellular senescence and curtail age-related pathologies.

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The senescence-associated secretory phenotype is potentiated by feedforward regulatory mechanisms involving Zscan4 and TAK1

Cited by 115 publications

References 51 publications

Targeting amphiregulin (AREG) derived from senescent stromal cells diminishes cancer resistance and averts programmed cell death 1 ligand (PD‐L1)‐mediated immunosuppression

Targeting amphiregulin (AREG) derived from senescent stromal cells diminishes cancer resistance and averts programmed cell death 1 ligand (PD‐L1)‐mediated immunosuppression

Senescent stromal cells promote cancer resistance through SIRT1 loss-potentiated overproduction of small extracellular vesicles

KDM4 Orchestrates Epigenomic Remodeling of Senescent Cells and Potentiates the Senescence-Associated Secretory Phenotype

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