2008
DOI: 10.1016/j.bmcl.2008.04.041
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Indirect oxidation of the antitumor agent procarbazine by tyrosinase—Possible application in designing anti-melanoma prodrugs

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Cited by 17 publications
(12 citation statements)
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“…Our results are consistent with recent studies that show that in urea or carbamate derivatives of dopamine the nitrogen atom is not sufficiently nucleophilic to effect the necessary cyclization that results in release of the antitumour agent [21,22]. …”
Section: Figure 1 Near Heresupporting
confidence: 93%
“…Our results are consistent with recent studies that show that in urea or carbamate derivatives of dopamine the nitrogen atom is not sufficiently nucleophilic to effect the necessary cyclization that results in release of the antitumour agent [21,22]. …”
Section: Figure 1 Near Heresupporting
confidence: 93%
“…Hyperpigmentation, such as melasma, ephelide, and lentigo in human skin and enzymatic browning in fruits and vegetables is not desirable. The occurrence of these phenomena has encouraged researchers to seek potent new safe tyrosinase inhibitors for use in anti-browning in farm products 40) and skin whitening for medicinal 41) and cosmetic purposes. 42) Recent expansion of the global market has resulted in an ever-growing demand for new products for depigmentation, cosmeceutical, and skin lightening purposes.…”
Section: Discussionmentioning
confidence: 99%
“…In particular, it has been demonstrated that tyrosinase is able to contribute to the oxidation of the hydrazine group in the anticancer agent procarbazine. 41 Tyrosinase is able to contribute via oxidation of substrates, namely, phenols such as quercetin, to reactive species. 42,43 These reactive o-quinone species are then able to oxidize the hydrazine linker on procarbazine and initiate procarbazine's antitumor activity.…”
Section: Tyrosinase-based Therapiesmentioning
confidence: 99%
“…42,43 These reactive o-quinone species are then able to oxidize the hydrazine linker on procarbazine and initiate procarbazine's antitumor activity. 41 Tyrosinase also mediates the release of cytotoxic agents from carbamate and urea prodrugs via a cyclization-drug release mechanism. 44 In murine models, tyrosinase-activated conditionally replicative adenoviruses have been reported to enhance prolongation of survival in mice with experimental brain tumors.…”
Section: Tyrosinase-based Therapiesmentioning
confidence: 99%