Abstract
Melanoma is highly metastatic, and understanding of its molecular mechanism is urgently needed for the development of therapeutic targets and prognostic assessment for metastatic melanoma. SIRT1 is a nicotinamide adenine dinucleotide (NAD+)-dependent protein deacetylase, belonging to the mammalian sirtuin family. It has been reported that SIRT1 is associated with metastasis in various cancers. However, the molecular mechanism of SIRT1 in melanoma metastasis remains to be clarified. Here we report that SIRT1 induces the epithelial–mesenchymal transition (EMT) by accelerating E-cadherin degradation via autophagy and facilitates melanoma metastasis. Initially, we found that SIRT1 expression was frequently elevated in metastatic melanoma compared with primary melanoma. In addition, SIRT1 induced the EMT and promoted cell migration and invasion by decreasing E-cadherin expression. Further work demonstrated that SIRT1 accelerated the autophagic degradation of E-cadherin through deacetylation of Beclin 1. In addition, inhibition of autophagy recovered E-cadherin expression and suppressed cell migration and invasion by delaying the degradation of E-cadherin in SIRT1-overexpressing cells. Overall, our findings reveal a novel molecular mechanism for SIRT1 in melanoma metastasis, indicating that SIRT1 may serve as a viable therapeutic target for metastatic melanoma.
Highlights
Melanoma is a lethal skin cancer that is highly metastatic[1,2]
SIRT1 expression is frequently elevated in metastatic melanoma Previous research has shown that SIRT1 expression is upregulated in human melanoma cells and tissues[32]
These results suggest that SIRT1 expression is elevated in metastatic melanoma
Summary
Melanoma is a lethal skin cancer that is highly metastatic[1,2]. Tumor metastasis poses a major barrier to the effective treatment of melanoma. There is no efficacious treatment for metastatic melanoma. Tumor metastasis is facilitated by the epithelial–mesenchymal transition (EMT). The EMT is a dynamic and reversible phenotypic switching process that enables polarized epithelial cells to gain characteristics of mesenchymal cell phenotypes as well as enhanced migratory and invasive capacities[4,5,6,7]. The EMT converts benign tumors into invasive, metastatic tumors and plays an important role in promoting tumor progression and metastasis[8]. Loss of expression of E-cadherin, a cell–cell adhesion molecule that is mainly expressed in epithelial cells, is the foundation for the activation of the EMT9,10. There are many transcription factors that work as Official journal of the Cell Death Differentiation Association
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