Silibinin inhibits ultraviolet B radiation-induced mitogenic and survival signaling, and associated biological responses in SKH-1 mouse skin

doi:10.1093/carcin/bgi096

Carcinogenesis Advance Access originally published online on April 14, 2005
Carcinogenesis 2005 26(8):1404-1413; doi:10.1093/carcin/bgi096

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Silibinin inhibits ultraviolet B radiation-induced mitogenic and survival signaling, and associated biological responses in SKH-1 mouse skin

Mallikarjuna Gu^1,, Sivanandhan Dhanalakshmi^1,, Sarumathi Mohan¹, Rana P. Singh¹ and Rajesh Agarwal^1,^2,^*

¹ Department of Pharmaceutical Sciences, School of Pharmacy and ² University of Colorado Cancer Center, University of Colorado Health Sciences Center, Denver, CO 80262, USA

^* To whom correspondence should be addressed. Tel: +1 303 315 1381; Fax: +1 303 315 6281; Email: Rajesh.Agarwal{at}UCHSC.edu

Ultraviolet B (UVB) radiation is a complete skin carcinogencausing DNA damage as a tumor-initiating event and activatingsignaling cascades that play a critical role in its tumor-promotingpotential. Recently we reported that a naturally occurring flavonoid,silibinin, protects UVB-induced skin damages and prevents photocarcinogenesis.Here we examined silibinin efficacy on acute and chronic UVB-causedmitogen-activated protein kinases (MAPKs) and AKT activationand associated biological responses in SKH-1 hairless mouseskin. A single UVB exposure at 180 mJ/cm² dose resulted in varyingdegrees of ERK1/2, JNK1/2, MAPK/p38 and AKT phosphorylationat various time-points in mouse skin; however, topical applicationof silibinin prior to or immediately after UVB exposure, orits dietary feeding strongly inhibited the activation of thesemolecules at all the time-points examined. Stronger effectsof silibinin towards inhibition of UVB-caused phosphorylationof MAPKs and AKT were also observed in a chronic UVB (180 mJ/cm²/dayfor 5 days) exposure protocol. Immunohistochemical analysisof chronically exposed skin sections showed that silibinin treatmentin all three protocols increases UVB-induced p53-positive cellsand decreases UVB-caused cell proliferation, apoptotic and sunburncells. These findings suggest that silibinin inhibits UVB-inducedMAPK and AKT signaling and increases p53 in mouse skin, andthat these effects of silibinin possibly lead to a decreasein UVB-caused proliferation and apoptosis, which might, in part,be responsible for its overall efficacy against photocarcinogenesis.

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