Antiproliferative Effects of 1α-OH-vitD3 in Malignant Melanoma: Potential Therapeutic implications

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作者
Lucia Spath
Alessandra Ulivieri
Luca Lavra
Laura Fidanza
Marta Carlesimo
Maria Giubettini
Alessandra Narcisi
Emidio Luciani
Barbara Bucci
Daniela Pisani
Salvatore Sciacchitano
Armando Bartolazzi
机构
[1] Pathology Research Laboratory,
[2] Sant’Andrea University Hospital,undefined
[3] via di Grottarossa 1035,undefined
[4] 00189 Rome,undefined
[5] Italy ,undefined
[6] Laboratory of Biomedical Research,undefined
[7] Niccolò Cusano University Foundation,undefined
[8] Dermatology Unit,undefined
[9] Sant’Andrea University Hospital,undefined
[10] via di Grottarossa 1035,undefined
[11] 00189 Rome,undefined
[12] Italy ,undefined
[13] Internal Medicine Sant’Andrea University Hospital,undefined
[14] Molecular and Cellular Tumor Pathology Laboratory,undefined
[15] Cancer Center Karolinska,undefined
[16] Karolinska Hospital,undefined
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Early detection and surgery represent the mainstay of treatment for superficial melanoma, but for high risk lesions (Breslow’s thickness >0.75 mm) an effective adjuvant therapy is lacking. Vitamin D insufficiency plays a relevant role in cancer biology. The biological effects of 1α hydroxycholecalciferol on experimental melanoma models were investigated. 105 melanoma patients were checked for 25-hydroxycholecalciferol (circulating vitamin D) serum levels. Human derived melanoma cell lines and in vivo xenografts were used for studying 1α-hydroxycholecalciferol-mediated biological effects on cell proliferation and tumor growth. 99 out of 105 (94%) melanoma patients had insufficient 25-hydroxycholecalciferol serum levels. Interestingly among the six with vitamin D in the normal range, five had a diagnosis of in situ/microinvasive melanoma. Treatment with 1α-hydroxycholecalciferol induced antiproliferative effects on melanoma cells in vitro and in vivo, modulating the expression of cell cycle key regulatory molecules. Cell cycle arrest in G1 or G2 phase was invariably observed in vitamin D treated melanoma cells. The antiproliferative activity induced by 1α-hydroxycholecalciferol in experimental melanoma models, together with the discovery of insufficient 25-hydroxycholecalciferol serum levels in melanoma patients, provide the rationale for using vitamin D in melanoma adjuvant therapy, alone or in association with other therapeutic options.
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