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Mapping epidermal and dermal cellular senescence in human skin aging. | LitMetric

AI Article Synopsis

  • Single-cell RNA sequencing and spatial transcriptomics provide deep insights into the cellular processes involved in skin aging and regeneration, focusing on irreversibly stalled cells known as senescent cells.
  • The research highlighted that photoaging, primarily from UV exposure, leads to a higher accumulation of senescent cells compared to normal aging, as demonstrated by a curated gene set named SenSkin™.
  • Findings indicate that senescent melanocytes increase melanin production, leading to uneven pigmentation, while senescent dermal fibroblasts result in decreased collagen and elastic fiber production, affecting overall skin health.

Article Abstract

Single-cell RNA sequencing and spatial transcriptomics enable unprecedented insight into cellular and molecular pathways implicated in human skin aging and regeneration. Senescent cells are individual cells that are irreversibly cell cycle arrested and can accumulate across the human lifespan due to cell-intrinsic and -extrinsic stressors. With an atlas of single-cell RNA-sequencing and spatial transcriptomics, epidermal and dermal senescence and its effects were investigated, with a focus on melanocytes and fibroblasts. Photoaging due to ultraviolet light exposure was associated with higher burdens of senescent cells, a sign of biological aging, compared to chronological aging. A skin-specific cellular senescence gene set, termed SenSkin™, was curated and confirmed to be elevated in the context of photoaging, chronological aging, and non-replicating CDKN1A+ (p21) cells. In the epidermis, senescent melanocytes were associated with elevated melanin synthesis, suggesting haphazard pigmentation, while in the dermis, senescent reticular dermal fibroblasts were associated with decreased collagen and elastic fiber synthesis. Spatial analysis revealed the tendency for senescent cells to cluster, particularly in photoaged skin. This work proposes a strategy for characterizing age-related skin dysfunction through the lens of cellular senescence and suggests a role for senescent epidermal cells (i.e., melanocytes) and senescent dermal cells (i.e., reticular dermal fibroblasts) in age-related skin sequelae.

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Source
http://dx.doi.org/10.1111/acel.14358DOI Listing

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