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Epigenetic Regulation of Skin Cells in Natural Aging and Premature Aging Diseases
Donata Orioli, Elena Dellambra
Cells · 2018 · ▲ 142 citations
Telomere attrition
Epigenetic alterations
Mitochondrial dysfunction
Cellular senescence
Stem-cell exhaustion
Cell culture / in vitro
Human
Review
Abstract
Skin undergoes continuous renewal throughout an individual's lifetime relying on stem cell functionality. However, a decline of the skin regenerative potential occurs with age. The accumulation of senescent cells over time probably reduces tissue regeneration and contributes to skin aging. Keratinocytes and dermal fibroblasts undergo senescence(definition) in response to several intrinsic or extrinsic stresses, including telomere(definition) shortening, overproduction of reactive oxygen species, diet, and sunlight exposure. Epigenetic mechanisms directly regulate skin homeostasis and regeneration, but they also mark cell senescence and the natural and pathological aging processes. Progeroid syndromes represent a group of clinical and genetically heterogeneous pathologies characterized by the accelerated aging of various tissues and organs, including skin. Skin cells from progeroid patients display molecular hallmarks that mimic those associated with naturally occurring aging. Thus, investigations on progeroid syndromes strongly contribute to disclose the causal mechanisms that underlie the aging process. In the present review, we discuss the role of epigenetic pathways in skin cell regulation during physiologic and premature aging.
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- 10.3390/cells7120268
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- 2026-06-11 MST
Cite this
APA
Orioli, D., & Dellambra, E. (2018). Epigenetic Regulation of Skin Cells in Natural Aging and Premature Aging Diseases. <em>Cells</em>. https://doi.org/10.3390/cells7120268
Vancouver
Orioli D, Dellambra E. Epigenetic Regulation of Skin Cells in Natural Aging and Premature Aging Diseases. Cells. 2018. doi:10.3390/cells7120268.
BibTeX
@article{donata2018Epigen,
title = {Epigenetic Regulation of Skin Cells in Natural Aging and Premature Aging Diseases},
author = {Donata Orioli and Elena Dellambra},
journal = {Cells},
year = {2018},
doi = {10.3390/cells7120268},
}
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