Abstract
Pre-mRNA processing factor 4B (PRP4) has previously been shown to induce epithelial-mesenchymal transition (EMT) and drug resistance in cancer cell lines. As melanin plays an important photoprotective role in the risk of sun-induced skin cancers, we have investigated whether PRP4 can induce drug resistance and regulate melanin biosynthesis in a murine melanoma (B16F10) cell line. Cells were incubated with a crucial melanogenesis stimulator, alpha-melanocyte-stimulating hormone, followed by transfection with PRP4. This resulted in the inhibition of the production of melanin via the downregulation of adenylyl cyclase-cyclic adenosine 3′,5′-monophosphate (AC)–(cAMP)–tyrosinase synthesis signaling pathway. Inhibition of melanin production by PRP4 leads to the promotion of carcinogenesis and induced drug resistance in B16F10 cells. Additionally, PRP4 overexpression upregulated the expression of β-arrestin 1 and desensitized the extracellular calcium-sensing receptor (CaSR), which in turn, inhibited the influx of extracellular Ca2+ ions. The decreased influx of Ca2+ was confirmed by a decreased expression level of calmodulin. We have demonstrated that transient receptor potential cation channel subfamily C member 1 was involved in the influx of CaSR-induced Ca2+ via a decreasing level of its expression. Furthermore, PRP4 overexpression downregulated the expression of AC, decreased the synthesis of cAMP, and modulated the actin cytoskeleton by inhibiting the expression of Ras homolog family member A (RhoA). Our investigation suggests that PRP4 inhibits the production of melanin in B16F10 cells, blocks the influx of Ca2+ through desensitization of CaSR, and modulates the actin cytoskeleton through downregulating the AC–cAMP pathway; taken together, these observations collectively lead to the promotion of skin carcinogenesis.
Highlights
The melanoma cell line B16F10 can produce melanin and displays metastatic behaviors
We have investigated the regulatory effect of Pre-mRNA processing factor 4B (PRP4) on melanin production in B16F10 cells and observed that PRP4 overexpression inhibited the production of melanin
We were curious to find the mechanism through which PRP4 promoted skin cancer, the effect of PRP4 on the melanin content of B16F10 cells was investigated in this study
Summary
The melanoma cell line B16F10 can produce melanin and displays metastatic behaviors. These cells are widely used to study melanogenesis and depigmentation [1], tumor metastasis [2], and cytotoxicity measurements of various substances in skin models [3]. Α-MSH binds to melanocortin 1 receptors, which produces cAMP, and cAMP phosphorylates the CREB transcription factor, which in turn promotes MITF activation. Melanosomes in dark skin show resistance to lysosomal degradation and remain intact throughout the epidermal layers. They form supranuclear caps in keratinocytes and melanocytes, and protect against ultraviolet radiations-induced damage [11,12]
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