Publication | Open Access
Testosterone Stimulates Duox1 Activity through GPRC6A in Skin Keratinocytes
38
Citations
33
References
2014
Year
Duox1 ActivityMolecular PhysiologySignal TransductionEndocrine MechanismCutaneous BiologyPhysiologyH2o2 GenerationTestosterone-gprc6a ComplexCell DeathDermatologySkin HomeostasisEndocrinologyMedicineCell BiologyCell SignalingCellular PhysiologyExperimental DermatologyReproductive Endocrinology
Testosterone is an endocrine hormone with functions in reproductive organs, anabolic events, and skin homeostasis. We report here that GPRC6A serves as a sensor and mediator of the rapid action of testosterone in epidermal keratinocytes. The silencing of GPRC6A inhibited testosterone-induced intracellular calcium ([Ca(2+)]i) mobilization and H2O2 generation. These results indicated that a testosterone-GPRC6A complex is required for activation of Gq protein, IP3 generation, and [Ca(2+)]i mobilization, leading to Duox1 activation. H2O2 generation by testosterone stimulated the apoptosis of keratinocytes through the activation of caspase-3. The application of testosterone into three-dimensional skin equivalents increased the apoptosis of keratinocytes between the granular and stratified corneum layers. These results support an understanding of the molecular mechanism of testosterone-dependent apoptosis in which testosterone stimulates H2O2 generation through the activation of Duox1.
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