Title : Chemical Reactivity Window Determines Prodrug Efficiency toward Glutathione Transferase Overexpressing Cancer Cells.

Pub. Date : 2016 Jun 6

PMID : 27093577






1 Functional Relationships(s)
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1 DNS-DOX, however, effectively killed GSTP1 (20 nmol/min/mg) and MGST1 (450 nmol/min/mg) overexpressing cells as did the less reactive 4-mononitrobenzenesulfonyl doxorubicin (MNS-DOX) in a MGST1-dependent manner (1.5 nmol/min/mg) as shown previously. 4-mononitrobenzenesulfonyl doxorubicin microsomal glutathione S-transferase 1 Homo sapiens