Estrogen promotes cutaneous wound healing via estrogen receptor β independent of its antiinflammatory activities

Laura Campbell, Elaine Emmerson, Faith Davies, Stephen C. Gilliver, Andre Krust, Pierre Chambon, Gillian S. Ashcroft, Matthew J. Hardman

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Post-menopausal women have an increased risk of developing a number of degenerative pathological conditions, linked by the common theme of excessive inflammation. Systemic estrogen replacement (in the form of hormone replacement therapy) is able to accelerate healing of acute cutaneous wounds in elderly females, linked to its potent antiinflammatory activity. However, in contrast to many other age-associated pathologies, the detailed mechanisms through which estrogen modulates skin repair, particularly the cell type-specific role of the two estrogen receptors, ERα and ERβ, has yet to be determined. Here, we use pharmacological activation and genetic deletion to investigate the role of both ERα and ERβ in cutaneous tissue repair. Unexpectedly, we report that exogenous estrogen replacement to ovariectomised mice in the absence of ERβ actually delayed wound healing. Moreover, healing in epidermal-specific ERβ null mice ( K14-cre/ERβL2/L2) largely resembled that in global ERβ null mice. Thus, the beneficial effects of estrogen on skin wound healing are mediated by epidermal ERβ, in marked contrast to most other tissues in the body where ERα is predominant. Surprisingly, agonists to both ERα and ERβ are potently antiinflammatory during skin repair, indicating clear uncoupling of inflammation and overall efficiency of repair. Thus, estrogen-mediated antiinflammatory activity is not the principal factor in accelerated wound healing. © 2010 Campbell et al.
    Original languageEnglish
    Pages (from-to)1825-1833
    Number of pages8
    JournalJournal of Experimental Medicine
    Volume207
    Issue number9
    DOIs
    Publication statusPublished - 30 Aug 2010

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