Bradley B. Jarrold
Early onset of senescence and imbalanced epidermal homeostasis across the decades in photoexposed human skin: Fingerprints of inflammaging
Jarrold, Bradley B.; Tan, Christina Yan Ru; Ho, Chin Yee; Soon, Ai Ling; Lam, TuKiet T.; Yang, Xiaojing; Nguyen, Calvin; Guo, Wei; Chew, Yap Ching; DeAngelis, Yvonne M.; Costello, Lydia; De Los Santos Gomez, Paola; Przyborski, Stefan; Bellanger, Sophie; Dreesen, Oliver; Kimball, Alexa B.; Oblong, John E.
Authors
Christina Yan Ru Tan
Chin Yee Ho
Ai Ling Soon
TuKiet T. Lam
Xiaojing Yang
Calvin Nguyen
Wei Guo
Yap Ching Chew
Yvonne M. DeAngelis
Lydia Costello
Paola De Los Santos Gomez paola.de-los-santos-gomez@durham.ac.uk
Academic Visitor
Professor Stefan Przyborski stefan.przyborski@durham.ac.uk
Deputy Provost
Sophie Bellanger
Oliver Dreesen
Alexa B. Kimball
John E. Oblong
Abstract
Inflammaging is a theory of ageing which purports that low-level chronic inflammation leads to cellular dysfunction and premature ageing of surrounding tissue. Skin is susceptible to inflammaging because it is the first line of defence from the environment, particularly solar radiation. To better understand the impact of ageing and photoexposure on epidermal biology, we performed a system biology-based analysis of photoexposed face and arm, and photoprotected buttock sites, from women between the ages of 20s to 70s. Biopsies were analysed by histology, transcriptomics, and proteomics and skin surface biomarkers collected from tape strips. We identified morphological changes with age of epidermal thinning, rete ridge pathlength loss and stratum corneum thickening. The SASP biomarkers IL-8 and IL-1RA/IL1-α were consistently elevated in face across age and cis/trans-urocanic acid were elevated in arms and face with age. In older arms, the DNA damage response biomarker 53BP1 showed higher puncti numbers in basal layers and epigenetic ageing were accelerated. Genes associated with differentiation and senescence showed increasing expression in the 30s whereas genes associated with hypoxia and glycolysis increased in the 50's. Proteomics comparing 60's vs 20's confirmed elevated levels of differentiation and glycolytic-related proteins. Representative immunostaining for proteins of differentiation, senescence and oxygen sensing/hypoxia showed similar relationships. This system biology-based analysis provides a body of evidence that young photoexposed skin is undergoing inflammaging. We propose the presence of chronic inflammation in young skin contributes to an imbalance of epidermal homeostasis that leads to a prematurely aged appearance during later life.
Citation
Jarrold, B. B., Tan, C. Y. R., Ho, C. Y., Soon, A. L., Lam, T. T., Yang, X., Nguyen, C., Guo, W., Chew, Y. C., DeAngelis, Y. M., Costello, L., De Los Santos Gomez, P., Przyborski, S., Bellanger, S., Dreesen, O., Kimball, A. B., & Oblong, J. E. (2022). Early onset of senescence and imbalanced epidermal homeostasis across the decades in photoexposed human skin: Fingerprints of inflammaging. Experimental Dermatology, 31(11), 1748-1760. https://doi.org/10.1111/exd.14654
Journal Article Type | Article |
---|---|
Acceptance Date | Jul 29, 2022 |
Online Publication Date | Aug 2, 2022 |
Publication Date | 2022-11 |
Deposit Date | Sep 6, 2022 |
Publicly Available Date | Aug 3, 2023 |
Journal | Experimental Dermatology |
Print ISSN | 0906-6705 |
Electronic ISSN | 1600-0625 |
Publisher | Wiley |
Peer Reviewed | Peer Reviewed |
Volume | 31 |
Issue | 11 |
Pages | 1748-1760 |
DOI | https://doi.org/10.1111/exd.14654 |
Public URL | https://durham-repository.worktribe.com/output/1195085 |
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