The effects of graded caloric restriction: <scp>XII</scp>. Comparison of mouse to human impact on cellular senescence in the colon

Fontana, Luigi; Mitchell, Sharon E.; Wang, Boshi; Tosti, Valeria; Vliet, Thijmen van; Veronese, Nicola; Bertozzi, Beatrice; Early, Dayna S.; Maissan, Parcival; Speakman, John R.; Demaria, Marco

doi:10.1111/acel.12746

Cited by 52 publications

(30 citation statements)

References 20 publications

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“…Within the first group, studies in mice have shown that a 3-month, 26% calorically restricted diet started at adulthood can reduce the number of senescent cells in rapidly proliferating (intestinal) and slowly proliferating (hepatic) tissues [104]. A study of the human colonic mucosa showed that adults who had been voluntarily exposed to a 30% caloric restriction (with appropriate nutrition) for over 10 years had significantly reduced expression of p16 INK4a and reduced local concentrations of IL-6 [105]. A recent study in mice demonstrated that calorie restriction, even if started at adulthood, prevents fat deposition and the concomitant increase in telomere-associated DNA damage foci (TAF) in hepatocytes [106].…”

Section: How Can We Fight Cellular Senescence?mentioning

confidence: 99%

Cellular Senescence as a Therapeutic Target for Age-Related Diseases: A Review

et al. 2020

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Life expectancy has increased substantially over the last few decades, leading to a worldwide increase in the prevalence and burden of agingassociated diseases. Recent evidence has proven that cellular senescence contributes substantially to the development of these disorders. Cellular senescence is a state of cell cycle arrest with suppressed apoptosis and concomitant secretion of multiple bioactive factors (the senescence-associated secretory phenotype-SASP) that plays a physiological role in embryonic development and healing processes. However, DNA damage and oxidative stress that occur during aging cause the accumulation of senescent cells, which through their SASP bring about deleterious effects on multiple organ and systemic functions. Ablation of senescent cells through genetic or pharmacological means leads to improved life span and health span in animal models, and preliminary evidence suggests it may also have a positive impact on human health. Thus, strategies to reduce or eliminate the burden of senescent cells or their products have the potential to impact multiple clinical outcomes with a single intervention. In this review, we touch upon the basics of cell senescence and summarize the current state of development of therapies against cell senescence for human use.

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Section: How Can We Fight Cellular Senescence?mentioning

confidence: 99%

Cellular Senescence as a Therapeutic Target for Age-Related Diseases: A Review

et al. 2020

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“…Different studies have shown that CR reduce senescence markers in different mouse organs and human colon mucosa 9,[63][64][65][66] . One of the main inducers of senescence is cellular damage.…”

Section: Cr and Cellular Senescencementioning

confidence: 99%

Caloric restriction and cellular senescence

Fontana

Nehme

Demaria

2018

Mechanisms of Ageing and Development

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“…[ 98 , 99 ]), and has also been demonstrated to substantially improve proteostasis in aged nematodes [ 7 , 109 , 110 ]. In humans, caloric restriction was shown to improve proteostasis [ 111 ] and reduce markers of senescence [ 112 ]. Interestingly, specific dietary supplements have been shown to improve the proteostasis capacity in aged nematodes, including oleic acid [ 113 ] and arachidonic acid [ 110 ], which was found to modulate HSF1 function [ 114 ].…”

Section: Modulation Of Proteostasis To Improve Aging Healthmentioning

confidence: 99%

The aging proteostasis decline: From nematode to human

Meller

Shalgi

2021

Experimental Cell Research

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The aging proteostasis decline manifests in a failure of aging cells and organisms to properly respond to proteotoxic challenges. This proteostasis collapse has long been considered a hallmark of aging in nematodes, and has recently been shown to occur also in human cells upon entry to senescence, opening the way to exploring the phenomenon in the broader context of human aging. Cellular senescence is part of the normal human physiology of aging, with senescent cell accumulation as a prominent feature of aged tissues. Being highly resistant to cell death, senescent cells, as they accumulate, become pro-inflammatory and promote disease. Here we discuss the causes of human senescence proteostasis decline, in view of the current literature on nematodes, on the one hand, and senescence, on the other hand. We review two major aspects of the phenomenon: (1) the decline in transcriptional activation of stress-response pathways, and (2) impairments in proteasome function. We further outline potential underlying mechanisms of transcriptional proteostasis decline, focusing on reduced chromatin dynamics and compromised nuclear integrity. Finally, we discuss potential strategies for reinforcing proteostasis as a means to improve organismal health and address the relationship to senolytics.

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The effects of graded caloric restriction: XII. Comparison of mouse to human impact on cellular senescence in the colon

Cited by 52 publications

References 20 publications

Cellular Senescence as a Therapeutic Target for Age-Related Diseases: A Review

Cellular Senescence as a Therapeutic Target for Age-Related Diseases: A Review

Caloric restriction and cellular senescence

The aging proteostasis decline: From nematode to human

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