Triglochin maritima Extracts Exert Anti-Melanogenic Properties via the CREB/MAPK Pathway in B16F10 Cells.

IF 4.9 2区 医学 Q1 CHEMISTRY, MEDICINAL Marine Drugs Pub Date : 2024-11-27 DOI:10.3390/md22120532
Won-Hwi Lee, Yuna Ha, Jeong-In Park, Won Bae Joh, Mira Park, Jang Kyun Kim, Hee-Kyung Jeon, Youn-Jung Kim
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Abstract

Triglochin maritima, a salt-tolerant plant, has demonstrated antioxidant effects, the ability to prevent prostate enlargement, antifungal properties, and skin moisturizing benefits. This study aimed to explore the anti-melanogenic potential of the 70% ethanol extract of T. maritima (TME) along with its ethyl acetate (TME-EA) and water (TME-A) fractions. TME (10-200 µg/mL), TME-EA (1-15 µg/mL), and TME-A (100-1000 µg/mL) were prepared and applied to B16F10 cells with or without α-MSH for 72 h. MTT assays were used to assess cytotoxicity, and anti-melanogenesis activity was determined by measuring melanin content, conducting a tyrosinase activity assay, and evaluating the expression of melanogenesis-related genes and proteins via RT-PCR and Western blotting. HPLC-PDA was used to analyze TME and TME-EA. The IC20 cytotoxicity values of TME, TME-A, and TME-EA without α-MSH, were 198.426 μg/mL, 1000 μg/mL, and 18.403 μg/mL, respectively. TME and TME-EA significantly decreased melanin and tyrosinase activity in α-MSH-stimulated B16F10 cells, with TME-EA showing comparable effects to arbutin, while TME-A showed no influence. TME-EA down-regulated melanogenesis genes (Tyr, Trp1, Dct, Mitf, Mc1r) and reduced CREB, p-38, and JNK phosphorylation while increasing ERK phosphorylation, suggesting the CREB/MAPK pathway's role in the anti-melanogenic effect. Luteolin was identified as a potential active ingredient. TME-EA may serve as an effective cosmeceutical for hyperpigmentation improvement due to its anti-melanogenic properties.

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三叶甘油三酯提取物通过CREB/MAPK途径在B16F10细胞中发挥抗黑素生成的作用。
三叶甘油三酯是一种耐盐植物,具有抗氧化作用、防止前列腺肿大、抗真菌特性和皮肤保湿功效。本研究旨在探讨海参70%乙醇提取物(TME)及其乙酸乙酯(TME- ea)和水(TME- a)组分的抗黑素生成潜力。制备TME(10-200µg/mL)、TME- ea(1-15µg/mL)和TME- a(100-1000µg/mL),分别作用于α-MSH或不含α-MSH的B16F10细胞72 h。采用MTT法评估细胞毒性,通过测定黑色素含量、酪氨酸酶活性、RT-PCR和Western blotting检测黑素生成相关基因和蛋白的表达来检测抗黑素生成活性。采用HPLC-PDA分析TME和TME- ea。不含α-MSH的TME、TME- a和TME- ea的IC20细胞毒值分别为198.426 μg/mL、1000 μg/mL和18.403 μg/mL。TME和TME- ea显著降低α- msh刺激的B16F10细胞的黑色素和酪氨酸酶活性,其中TME- ea与熊果苷的作用相当,而TME- a没有影响。TME-EA下调黑色素生成基因(Tyr、Trp1、Dct、Mitf、Mc1r),降低CREB、p-38和JNK磷酸化,增加ERK磷酸化,提示CREB/MAPK通路在抗黑色素生成作用中发挥作用。木犀草素是一种潜在的活性成分。由于其抗黑素的特性,TME-EA可以作为一种有效的药妆改善色素沉着。
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来源期刊
Marine Drugs
Marine Drugs 医学-医药化学
CiteScore
9.60
自引率
14.80%
发文量
671
审稿时长
1 months
期刊介绍: Marine Drugs (ISSN 1660-3397) publishes reviews, regular research papers and short notes on the research, development and production of drugs from the sea. Our aim is to encourage scientists to publish their experimental and theoretical research in as much detail as possible, particularly synthetic procedures and characterization information for bioactive compounds. There is no restriction on the length of the experimental section.
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