AI Article Synopsis

  • An ubiquinone derivative called pseudoalteromone A was isolated from marine species APmarine002 and ROA-050 and shown to have anti-melanogenesis effects.
  • Treatment with pseudoalteromone A significantly reduced melanin production and tyrosinase activity in various melanocyte cell lines, indicating its potential for skin-whitening.
  • Further analysis using a 3D pigmented skin model confirmed that pseudoalteromone A inhibits melanogenic gene expression, leading to its anti-melanogenic properties.

Article Abstract

An ubiquinone derivative, pseudoalteromone A (), has been isolated from two marine-derived spp., APmarine002 and ROA-050, and its anti-melanogenesis activity was investigated. The anti-melanogenic capacity of pseudoalteromone A was demonstrated by assessing the intracellular and extracellular melanin content and cellular tyrosinase activity in the B16 cell line, Melan-a mouse melanocyte cell line, and MNT-1 human malignant melanoma cell line. Treatment with pseudoalteromone A (40 μg/mL) for 72 h reduced α-melanocyte-stimulating hormone (α-MSH)-induced intracellular melanin production by up to 44.68% in B16 cells and 38.24% in MNT-1 cells. Notably, pseudoalteromone A induced a concentration-dependent reduction in cellular tyrosinase activity in B16 cell, and Western blot analyses showed that this inhibitory activity was associated with a significant decrease in protein levels of tyrosinase and tyrosinase-related protein 1 (Tyrp-1), suggesting that pseudoalteromone A exerts its anti-melanogenesis activity through effects on melanogenic genes. We further evaluated the skin-whitening effect of pseudoalteromone A in the three-dimensional (3D) pigmented-epidermis model, MelanoDerm, and visualized the 3D distribution of melanin by two-photon excited fluorescence imaging in this human skin equivalent. Collectively, our findings suggest that pseudoalteromone A inhibits tyrosinase activity and expression and that this accounts for its anti-melanogenic effects in melanocytes.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8618130PMC
http://dx.doi.org/10.3390/md19110612DOI Listing

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