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Are therapeutic effects of antiacne agents mediated by activation of FoxO1 and inhibition of mTORC1?

Melnik, Bodo C. ; Schmitz, Gerd



Abstract

Acne pathogenesis has recently been linked to decreased nuclear FoxO1 levels and increased mTORC1 activity. This hypothesis postulates that antiacne agents either enhance nuclear FoxO activity or inhibit mTORC1. Benzoyl peroxide (BPO), by activation of oxidative stress-inducible kinases, increases nuclear FoxO levels promoting Sestrin3-mediated AMPK activation. Furthermore, BPO-derived ROS may ...

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