Hyperphosphatemia induces senescence in human endothelial cells by increasing endothelin‐1 production

Olmos, Gemma; Martínez-Miguel, Patricia; Alcalde-Estévez, Elena; Medrano, Diana; Sosa, Patricia; Rodríguez‐Mañas, Leocadio; Naves-Díaz, Manuel; Rodríguez‐Puyol, Diego; Ruiz-Torres, María Piedad; López‐Ongil, Susana

doi:10.1111/acel.12664

Cited by 37 publications

(36 citation statements)

References 44 publications

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“…Surprisingly, AP-1, which is generally characterized as pro-mitotic, has also been reported as increased in senescent pEOCs [36]. Recently, however, the ROS-mediated induction of AP-1 has been causatively connected with the initiation of senescence in endothelial cells [37]. AP-1 induction has also been suggested as an essential element of signaling cascade in Ras-induced senescence of fibroblasts [38].…”

Section: Discussionmentioning

confidence: 99%

Deciphering the Molecular Mechanism of Spontaneous Senescence in Primary Epithelial Ovarian Cancer Cells

Pakuła

Mały

Uruski

et al. 2020

Cancers

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Spontaneous senescence of cancer cells remains a puzzling and poorly understood phenomenon. Here we comprehensively characterize this process in primary epithelial ovarian cancer cells (pEOCs). Analysis of tumors from ovarian cancer patients showed an abundance of senescent cells in vivo. Further, serially passaged pEOCs become senescent after a few divisions. These senescent cultures display trace proliferation, high expression of senescence biomarkers (SA-β-Gal, γ-H2A.X), growth-arrest in the G1 phase, increased level of cyclins D1, D2, decreased cyclin B1, up-regulated p16, p21, and p53 proteins, eroded telomeres, reduced activity of telomerase, predominantly non-telomeric DNA damage, activated AKT, AP-1, and ERK1/2 signaling, diminished JNK, NF-κB, and STAT3 pathways, increased formation of reactive oxygen species, unchanged activity of antioxidants, increased oxidative damage to DNA and proteins, and dysfunctional mitochondria. Moreover, pEOC senescence is inducible by normal peritoneal mesothelium, fibroblasts, and malignant ascites via the paracrine activity of GRO-1, HGF, and TGF-β1. Collectively, pEOCs undergo spontaneous senescence in a mosaic, telomere-dependent and telomere-independent manner, plausibly in an oxidative stress-dependent mechanism. The process may also be activated by extracellular stimuli. The biological and clinical significance of pEOC senescence remains to be explored.

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Section: Discussionmentioning

confidence: 99%

Deciphering the Molecular Mechanism of Spontaneous Senescence in Primary Epithelial Ovarian Cancer Cells

Pakuła

Mały

Uruski

et al. 2020

Cancers

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“…ET-1 also contributes to the fibrotic phenotype, inducing the expression of collagen, FN and CCN2 in fibroblasts isolated from fibrotic lesions [27]. Moreover, ET-1 has been reported to induce cellular senescence in cultured vascular endothelial cells [28].…”

Section: Agingmentioning

confidence: 99%

“…sarcopenia. ET-1 has been associated to the development of fibrosis in different cell and tissue contexts [22,24,27,29], even it can induce cellular senescence in human endothelial cells [28], but the role of ET-1 in skeletal muscle aging has never been described before. For this reason, we decided to study its effects on cultured muscle cells using a well-described experimental cellular model; mouse myoblast C2C12 cells [30].…”

Section: Agingmentioning

confidence: 99%

Endothelin-1 induces cellular senescence and fibrosis in cultured myoblasts. A potential mechanism of aging-related sarcopenia

Alcalde-Estévez

Asenjo-Bueno

Sosa

et al. 2020

Aging

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The loss of muscular mass and strength is an inevitable aging related phenomenon, named sarcopenia. The mechanisms involved in its origin and progression remain to be clearly elucidated. Malnutrition, decreased physical exercise and the decline in sex steroid hormone production and in insulin sensitivity play an important role in sarcopenia [1]. Sarcopenic muscles suffer profound changes in their architecture, exhibiting both reduced fiber size and reduced fiber number, especially of the type II fibers, reduced number of satellite cells www.aging-us.com

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“…Senescence also occurs with aging in both major arterial cell types, endothelium (103,104) and VSMCs (105)(106)(107). Endothelial NO produced by eNOS normally maintains VSMCs in a nondividing, contractile state and suppresses thrombogenic and inflammatory signaling in endothelium.…”

Section: Senescent Cells Drive Age-related Cardiovascular Diseasesmentioning

confidence: 99%

Senescent cells: a therapeutic target for cardiovascular disease

Childs¹,

Hu²,

Deursen³

2018

Journal of Clinical Investigation

145

122

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Cellular senescence, a major tumor-suppressive cell fate, has emerged from humble beginnings as an in vitro phenomenon into recognition as a fundamental mechanism of aging. In the process, senescent cells have attracted attention as a therapeutic target for age-related diseases, including cardiovascular disease (CVD), the leading cause of morbidity and mortality in the elderly. Given the aging global population and the inadequacy of current medical management, attenuating the health care burden of CVD would be transformative to clinical practice. Here, we review the evidence that cellular senescence drives CVD in a bimodal fashion by both priming the aged cardiovascular system for disease and driving established disease forward. Hence, the growing field of senotherapy (neutralizing senescent cells for therapeutic benefit) is poised to contribute to both prevention and treatment of CVD.

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Hyperphosphatemia induces senescence in human endothelial cells by increasing endothelin‐1 production

Cited by 37 publications

References 44 publications

Deciphering the Molecular Mechanism of Spontaneous Senescence in Primary Epithelial Ovarian Cancer Cells

Deciphering the Molecular Mechanism of Spontaneous Senescence in Primary Epithelial Ovarian Cancer Cells

Endothelin-1 induces cellular senescence and fibrosis in cultured myoblasts. A potential mechanism of aging-related sarcopenia

Senescent cells: a therapeutic target for cardiovascular disease

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