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通过高灵敏度激酶测定法证实,致癌激酶PAK1的微量水平在黑色素瘤细胞中具有血清/血小板衍生生长因子依赖性的“致黑色素生成”作用。

The serum/PDGF-dependent "melanogenic" role of the minute level of the oncogenic kinase PAK1 in melanoma cells proven by the highly sensitive kinase assay.

作者信息

Be Tu Pham Thi, Nguyen Binh Cao Quan, Tawata Shinkichi, Yun Cheong-Yong, Kim Eung Gook, Maruta Hiroshi

机构信息

PAK Research Center, University of the Ryukyus.

出版信息

Drug Discov Ther. 2017 Jan 15;10(6):314-322. doi: 10.5582/ddt.2016.01062. Epub 2016 Oct 17.

DOI:10.5582/ddt.2016.01062
PMID:27746419
Abstract

We previously demonstrated that the oncogenic kinase PAK4, which both melanomas and normal melanocytes express at a very high level, is essential for their melanogenesis. In the present study, using the highly sensitive "Macaroni-Western" (IP-ATP-Glo) kinase assay, we investigated the melanogenic potential of another oncogenic kinase PAK1, which melanoma (B16F10) cells express only at a very minute level. After transfecting melanoma cells with PAK1-shRNA for silencing PAK1 gene, melanin content, tyrosinase activity, and kinase activity of PAK1 were compared between the wild-type and transfectants. We found that (i) PAK1 is significantly activated by melanogenic hormones such as IBMX (3-isobutyl-1-methyl xanthine) and α-MSH (melanocyte-stimulating hormone), (ii) silencing the endogenous PAK1 gene in melanoma cells through PAK1-specific shRNA reduces both melanin content and tyrosinase activity in the presence of both serum and melanogenic hormones to the basal level, (iii) the exogenously added wild-type PAK1 in the melanoma cells boosts the α-MSH-inducible melanin level by several folds without affecting the basal, and (iv) α-MSH/IBMX-induced melanogenesis hardly takes place in the absence of either serum or PAK1, clearly indicating that PAK1 is essential mainly for serum- and α-MSH/IBMX-dependent melanogenesis, but not the basal, in melanoma cells. The outcome of this study might provide the first scientific basis for explaining why a wide variety of herbal PAK1-blockers such as CAPE (caffeic acid phenethyl ester), curcumin and shikonin in cosmetics are useful for skin-whitening.

摘要

我们之前证明,致癌激酶PAK4在黑色素瘤和正常黑素细胞中均高表达,对它们的黑色素生成至关重要。在本研究中,我们使用高灵敏度的“通心粉免疫印迹法”(IP-ATP-Glo)激酶检测法,研究了另一种致癌激酶PAK1的黑色素生成潜力,PAK1在黑色素瘤(B16F10)细胞中仅微量表达。在用PAK1-shRNA转染黑色素瘤细胞以沉默PAK1基因后,比较了野生型和转染细胞之间的黑色素含量、酪氨酸酶活性以及PAK1的激酶活性。我们发现:(i)PAK1被诸如异丁基甲基黄嘌呤(IBMX)和α-促黑素(α-MSH)等黑色素生成激素显著激活;(ii)通过PAK1特异性shRNA沉默黑色素瘤细胞中的内源性PAK1基因,在有血清和黑色素生成激素存在的情况下,可将黑色素含量和酪氨酸酶活性均降低至基础水平;(iii)向黑色素瘤细胞中外源添加野生型PAK1可使α-MSH诱导的黑色素水平提高数倍,且不影响基础水平;(iv)在没有血清或PAK1的情况下,α-MSH/IBMX诱导的黑色素生成几乎不发生,这清楚地表明PAK1主要对黑色素瘤细胞中依赖血清和α-MSH/IBMX的黑色素生成至关重要,而对基础黑色素生成并非如此。本研究结果可能为解释为何化妆品中多种草药PAK1阻滞剂(如咖啡酸苯乙酯(CAPE)、姜黄素和紫草素)对皮肤美白有用提供首个科学依据。

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