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Curcumin-induced melanoma cell death is associated with mitochondrial permeability transition pore (mPTP) opening
Authors:Ying Qiu  Teng Yu  Wei Wang  Kun Pan  Dongmei Shi  Hui Sun
Institution:1. Department of Dermatology, Shandong Ji-ning No.1 People’s Hospital, Ji-ning City, Shandong Province 272011, PR China;2. Department of Dermatology, The Skin Disease Hospital of Ji-ning City, Ji-ning City, Shandong Province 272011, PR China
Abstract:Here we studied the role of mitochondrial permeability transition pore (mPTP) opening in curcumin’s cytotoxicity in melanoma cells. In cultured WM-115 melanoma cells, curcumin induced mitochondrial membrane potential (MPP) decrease, cyclophilin-D (CyPD)-adenine nucleotide translocator 1 (ANT-1) (two mPTP components) mitochondrial association and cytochrome C release, indicating mPTP opening. The mPTP blocker sanglifehrin A (SfA) and ANT-1 siRNA-depletion dramatically inhibited curcumin-induced cytochrome C release and WM-115 cell death. CyPD is required for curcumin-induced melanoma cell death. The CyPD inhibitor cyclosporin A (CsA) or CyPD siRNA-depletion inhibited curcumin-induced WM-115 cell death and apoptosis, while WM-115 cells with CyPD over-expression were hyper-sensitive to curcumin. Finally, we found that C6 ceramide enhanced curcumin-induced cytotoxicity probably through facilitating mPTP opening, while CsA and SfA as well as CyPD and ANT-1 siRNAs alleviated C6 ceramide’s effect on curcumin in WM-115 cells. Together, these results suggest that curcumin-induced melanoma cell death is associated with mPTP opening.
Keywords:ANT-1  adenine nucleotide translocator 1  CyPD  cyclophilin-D  CsA  cyclosporin A  mPTP  mitochondrial permeability transition pore  MPP  mitochondrial membrane potential  SfA  sanglifehrin A
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