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首页> 外文期刊>Pigment cell & melanoma research >Manassantin B inhibits melanosome transport in melanocytes by disrupting the melanophilin-myosin Va interaction
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Manassantin B inhibits melanosome transport in melanocytes by disrupting the melanophilin-myosin Va interaction

机译:Manassantin B通过破坏黑素蛋白-肌球蛋白Va相互作用来抑制黑素细胞中的黑素体转运

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摘要

Human skin hyperpigmentation disorders occur when the synthesis and/or distribution of melanin increases. The distribution of melanin in the skin is achieved by melanosome transport and transfer. The transport of melanosomes, the organelles where melanin is made, in a melanocyte precedes the transfer of the melanosomes to a keratinocyte. Therefore, hyperpigmentation can be regulated by decreasing melanosome transport. In this study, we found that an extract of Saururus chinensis Baill (ESCB) and one of its components, manassantin B, inhibited melanosome transport in Melan-a melanocytes and normal human melanocytes (NHMs). Manassantin B disturbed melanosome transport by disrupting the interaction between melanophilin and myosin Va. Manassantin B is neither a direct nor an indirect inhibitor of tyrosinase. The total melanin content was not reduced when melanosome transport was inhibited in a Melan-a melanocyte monoculture by manassantin B. Manassantin B decreased melanin content only when Melan-a melanocytes were co-cultured with SP-1 keratinocytes or stimulated by α-MSH. Therefore, we propose that specific inhibitors of melanosome transport, such as manassantin B, are potential candidate or lead compounds for the development of agents to treat undesirable hyperpigmentation of the skin.
机译:当黑色素的合成和/或分布增加时,就会发生人的皮肤色素沉着异常。黑色素在皮肤中的分布是通过黑素体的运输和转移来实现的。在黑素细胞中黑素体(制造黑色素的细胞器)的运输先于黑素体向角质形成细胞的转移。因此,可以通过减少黑素体转运来调节色素沉着过度。在这项研究中,我们发现金龙属(Saururus chinensis Baill)(ESCB)的提取物及其成分之一(manassantin B)抑制了Melan-a黑素细胞和正常人黑素细胞(NHMs)中黑素体的运输。 Manassantin B通过破坏黑色素和肌球蛋白Va之间的相互作用来干扰黑素体的运输。ManassantinB既不是酪氨酸酶的直接抑制剂,也不是其间接抑制剂。当通过Manassantin B抑制Melan-a黑色素细胞单次培养中的黑素体转运时,总黑色素含量不会降低。ManassantinB仅在Melan-a黑色素细胞与SP-1角质形成细胞共培养或受到α-MSH刺激时才降低黑色素含量。因此,我们提出黑素体转运的特异性抑制剂,例如马纳森汀B,是潜在的候选化合物或潜在化合物,可用于开发治疗皮肤不良色素沉着的药物。

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