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Inulavosin and its benzo-derivatives, melanogenesis inhibitors, target the copper loading mechanism to the active site of tyrosinase

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dc.contributor.author Fujita, H.
dc.contributor.author Menezes, J.C.J.M.D.S.
dc.contributor.author Santos, S.M.
dc.contributor.author Yokota, S.
dc.contributor.author Kamat, S.P.
dc.contributor.author Cavaleiro, J.A.S.
dc.contributor.author Motokawa, T.
dc.contributor.author Kato, T.
dc.contributor.author Mochizuki, M.
dc.contributor.author Fujiwara, T.
dc.contributor.author Fujii, Y.
dc.contributor.author Tanaka, Y.
dc.date.accessioned 2015-06-04T04:22:27Z
dc.date.available 2015-06-04T04:22:27Z
dc.date.issued 2014
dc.identifier.citation Pigment Cell and Melanoma Research. 27(3); 2014; 376-386. en_US
dc.identifier.uri http://dx.doi.org/10.1111/pcmr.12225
dc.identifier.uri http://irgu.unigoa.ac.in/drs/handle/unigoa/3054
dc.description.abstract Tyrosinase, a melanosomal membrane protein containing copper, is a key enzyme for melanin synthesis in melanocytes. Inulavosin inhibits melanogenesis by enhancing a degradation of tyrosinase in lysosomes. However, the mechanism by which inulavosin redirects tyrosinase to lysosomes is yet unknown. The analyses of structure-activity relationship of inulavosin and its benzo-derivatives reveal that the hydroxyl and the methyl groups play a critical role in their inhibitory activity. Intriguingly, the docking studies to tyrosinase suggest that the compounds showing inhibitory activity bind through hydrophobic interactions to the cavity of tyrosinase below which the copper-binding sites are located. This cavity is proposed to be required for the association with a chaperon that assists in copper loading to tyrosinase in Streptomyces antibioticus. Inulavosin and its benzo-derivatives may compete with the copper chaperon and result in a lysosomal mistargeting of apo-tyrosinase that has a conformational defect. en_US
dc.publisher Wiley en_US
dc.subject Chemistry en_US
dc.title Inulavosin and its benzo-derivatives, melanogenesis inhibitors, target the copper loading mechanism to the active site of tyrosinase en_US
dc.type Journal article en_US
dc.identifier.impf y


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