Melanosomal localization is required for GIF-2115/2250 to inhibit melanogenesis in B16F10 melanoma cells

IF 2.7 4区 医学 Q2 DERMATOLOGY International Journal of Cosmetic Science Pub Date : 2024-02-07 DOI:10.1111/ics.12949
Ayumi Sakurai, Kyoka Kawaguchi, Miyu Watanabe, Sayaka Okajima, Saho Furukawa, Kenichi Koga, Kentaro Oh-Hashi, Yoko Hirata, Kyoji Furuta, Hiroshi Takemori
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Abstract

Objective

Tyrosinase inhibitors suppress melanogenesis in melanocytes. During a screening for tyrosinase inhibitors, however, we noticed some discrepancies in inhibitory efficacies between melanocytes and in vitro assays. The compound (S)-N-{3-[4-(dimethylamino)phenyl]propyl}-N-methyl-indan-1-amine (GIF-2115) exerts antioxidative stress activity upon accumulation in late endosomes and lysosomes. GIF-2115 was also identified as a potent antimelanogenic reagent in B16F10 mouse melanoma cells. GIF-2115 inhibited the activity of mushroom tyrosinase and the lysates of B16F10 cells. However, structure–activity relationship studies indicated that GIF-2238, which lacks the benzene ring in the aminoindan structure of GIF-2115, inhibited tyrosinase activity in vitro but did not inhibit melanogenesis in B16F10 cells. The aim of the present study is to show the importance of the intracellular distribution of tyrosinase inhibitors in exerting their antimelanogenic activity in melanocytes.

Methods

The intracellular distribution of compounds was monitored by linking with the fluorescent group of 7-nitro-2,1,3-benzoxadiazole (NBD). To mislocalize GIF-2115 to mitochondria, the mitochondria-preferring fluoroprobe ATTO565 was used.

Results

We reconfirmed the localization of GIF-2250 (GIF-2115-NBD) not only to matured but also to early-stage melanosomes. Although GIF-2286 (GIF-2238-NBD) maintained tyrosinase inhibitory activity, it did not show specific intracellular localization. Moreover, when GIF-2115 was linked with ATTO565, the resultant compound GIF-2265 did not inhibit melanogenesis in B16F10 cells, despite its strong tyrosinase inhibitory activity.

Conclusion

These results suggest that melanosomal localization is essential for the antimelanogenic activity of GIF-2115, and GIF-2115 derivatives may be new guides for drugs to endosomes and lysosomes as well as melanosomes.

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GIF-2115/2250 抑制 B16F10 黑色素瘤细胞的黑色素生成需要黑体定位。
目的酪氨酸酶抑制剂可抑制黑色素细胞中的黑色素生成。然而,在筛选酪氨酸酶抑制剂的过程中,我们注意到黑色素细胞和体外试验的抑制效果存在一些差异。化合物(S)-N-{3-[4-(二甲基氨基)苯基]丙基}-N-甲基-茚满-1-胺(GIF-2115)在晚期内体和溶酶体中积累后具有抗氧化活性。在 B16F10 小鼠黑色素瘤细胞中,GIF-2115 也被鉴定为一种有效的抗黑色素生成试剂。GIF-2115 可抑制蘑菇酪氨酸酶和 B16F10 细胞裂解物的活性。然而,结构-活性关系研究表明,GIF-2238 缺乏 GIF-2115 氨基茚满结构中的苯环,它能抑制体外酪氨酸酶的活性,但不能抑制 B16F10 细胞的黑色素生成。本研究旨在说明酪氨酸酶抑制剂在黑色素细胞中发挥抗黑色素生成活性的细胞内分布的重要性:方法:通过与7-硝基-2,1,3-苯并噁二唑(NBD)的荧光基团连接来监测化合物在细胞内的分布。为了将 GIF-2115 错定位到线粒体,使用了线粒体优先荧光探针 ATTO565:结果:我们再次证实了 GIF-2250 (GIF-2115-NBD)不仅存在于成熟的黑色素体中,也存在于早期黑色素体中。虽然GIF-2286(GIF-2238-NBD)保持着抑制酪氨酸酶的活性,但它并没有显示出特定的细胞内定位。此外,当 GIF-2115 与 ATTO565 连接时,生成的化合物 GIF-2265 虽然具有很强的酪氨酸酶抑制活性,但并不能抑制 B16F10 细胞的黑色素生成:这些结果表明,黑色素体定位对 GIF-2115 的抗黑色素生成活性至关重要,GIF-2115 衍生物可能是药物进入内体和溶酶体以及黑色素体的新途径。
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来源期刊
CiteScore
4.60
自引率
4.30%
发文量
73
期刊介绍: The Journal publishes original refereed papers, review papers and correspondence in the fields of cosmetic research. It is read by practising cosmetic scientists and dermatologists, as well as specialists in more diverse disciplines that are developing new products which contact the skin, hair, nails or mucous membranes. The aim of the Journal is to present current scientific research, both pure and applied, in: cosmetics, toiletries, perfumery and allied fields. Areas that are of particular interest include: studies in skin physiology and interactions with cosmetic ingredients, innovation in claim substantiation methods (in silico, in vitro, ex vivo, in vivo), human and in vitro safety testing of cosmetic ingredients and products, physical chemistry and technology of emulsion and dispersed systems, theory and application of surfactants, new developments in olfactive research, aerosol technology and selected aspects of analytical chemistry.
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