Glutathione and Mercapturic Acid Conjugates of Sulofenur and Their Activity against a Human Colon Cancer Cell Line

Guan, Xiaoxu; Hoffman, Brianna N.; McFarland, Douglas C.; Gilkerson, Kysa K.; Dwivedi, Chandradhar; Erickson, Angela K.; Bebensee, Scott; Pellegrini, Jill

doi:10.1124/dmd.30.3.331

Cited by 21 publications

(17 citation statements)

References 26 publications

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“…Therefore, increased activity or abundance of GST may facilitate the formation and subsequent accumulation of such compounds. It is also important to note that quercetin can inhibit GST through the formation of oquinone (18,31) and other GSH, and mercapturic conjugates inhibit GSH reductase (28). Therefore, in tyrosinase expressing cells, quercetin may have multiple modes of interaction with drug detoxification proteins and may provide a means to interfere with drug resistance.…”

Section: Discussionmentioning

confidence: 99%

“…Therefore, Tyr + cells may also display elevated GST activity and a higher capacity to form conjugates. Various GSH and mercapturic acid conjugates have anticarcinogenic activity (28) and chemopreventative properties (29). The role of conjugate toxicity is further demonstrated by the induction of apoptosis in cells after the depletion of ralA binding protein 1, a transporter of GSH conjugates (30).…”

Section: Discussionmentioning

confidence: 99%

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Quercetin Selectively Inhibits Bioreduction and Enhances Apoptosis in Melanoma Cells That Overexpress Tyrosinase

Thangasamy

Sittadjody

Lanza-Jacoby

et al. 2007

Nutrition and Cancer

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Tyrosinase is expressed in melanoma cells and catalyzes the formation of 3,3',4',5,7-pentahydroxyflavone (quercetin) into reactive quinone species and subsequent glutathionyl adducts. Therefore, we examined the effect of quercetin metabolism on the glutathione (GSH) bioreduction pathway and cell viability in DB-1 melanoma cells that express varying levels of tyrosinase (Tyr+). In a cell-free system, GSH was significantly decreased by quercetin, which coincided with the formation of glutathionyl adducts. In Tyr+ clones, quercetin decreased bioreduction capacity and increased reactive oxygen species (ROS) to a greater degree compared to control cells. The antioxidant/electrophile response element-induced enzymes, glutathione-S-transferase (GST), and nicotinamide adenine dinucleotide phosphate:quinone oxidoreductase 1 were expressed at high levels in Tyr+ cells and contributed to pro-oxidant quercetin metabolism. The basal level of ROS and apoptosis was higher in Tyr+ cells and were selectively increased after exposure to quercetin. The increase in apoptosis following quercetin exposure was p53/Bax mediated and correlated with a decrease in GST-driven bioreduction capacity and an increase in ROS. In conclusion, quercetin can selectively sensitize Tyr+ expressing melanoma cells to apoptosis and may serve as an adjuvant to chemotherapy by enhancing cell death and interfering with GST-mediated drug resistance.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Quercetin Selectively Inhibits Bioreduction and Enhances Apoptosis in Melanoma Cells That Overexpress Tyrosinase

Thangasamy

Sittadjody

Lanza-Jacoby

et al. 2007

Nutrition and Cancer

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“…However, it was clearly demonstrated that SCPG is further processed through the mercapturic acid pathway to the corresponding N-acetylcysteine conjugate [ N -acetyl- S -( p -chlorophenylcarbamoyl)cysteine, NACC], which possesses comparable anticancer activity to the parent compound. The GSH- and cysteine-conjugates produced are susceptible to thiol exchange reactions and may act as carbamoylating agents towards biomacromolecules (Day et al, 1996; Guan et al, 2002). NACC, whose mechanism of action remains unclear, demonstrated selective anticancer activity, and low toxicity, which make NACC and its analogs promising anticancer agents (Chen et al, 2011).…”

Section: Bioactivation Of Cancer Compounds By Gstmentioning

confidence: 99%

Glutathione S-conjugates as prodrugs to target drug-resistant tumors

Ramsay

Dilda

2014

Front. Pharmacol.

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Living organisms are continuously exposed to xenobiotics. The major phase of enzymatic detoxification in many species is the conjugation of activated xenobiotics to reduced glutathione (GSH) catalyzed by the glutathione-S-transferase (GST). It has been reported that some compounds, once transformed into glutathione S-conjugates, enter the mercapturic acid pathway whose end products are highly reactive and toxic for the cell responsible for their production. The cytotoxicity of these GSH conjugates depends essentially on GST and gamma-glutamyl transferases (γGT), the enzymes which initiate the mercapturic acid synthesis pathway. Numerous studies support the view that the expression of GST and γGT in cancer cells represents an important factor in the appearance of a more aggressive and resistant phenotype. High levels of tumor GST and γGT expression were employed to selectively target tumor with GST- or γGT-activated drugs. This strategy, explored over the last two decades, has recently been successful using GST-activated nitrogen mustard (TLK286) and γGT-activated arsenic-based (GSAO and Darinaparsin) prodrugs confirming the potential of GSH-conjugates as anticancer drugs.

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“…Therefore, though urinary MAs are frequently used as biomarkers of internal dose, they are sometimes also classified as biomarker of effect [22]. Several recent and older examples of MAs used in the BM of human exposure or in biotransformation studies are: N-acetyl-S-(9,10-dihydro-9-hydroxy-10-phenanthryl)-L-cysteine, which originates from a polycyclic aromatic hydrocarbon, phenanthrene, present in cigarette smoke [23], four structurally different mercapturates derived from the herbicides atrazine, acetochlor, metolachlor, and alachlor [24], S-acetamidomethylmercapturic acid, in response to exposure to the industrial solvent N,N-dimethylacetamide [25], N-acetyl-S-(p-chloro- phenylcarbamoyl)cysteine, derives from the anticancer agent sulofenur [26], phenyl mercapturic acid, in response to benzene exposure in industry [27], 3,4-dihydroxybutylmercapturic acid as an environmental and biological monitoring indicator of non-occupational exposure to 1,3-dichloropropene [28], 3-chloro-2-hydroxypropylmercapturic acid and allylmercapturic acid as urinary biomarkers of human exposure to allyl chloride [29], and N-acetyl-S-(Z-and E-3-chloropropenyl-2)-L-cysteine as a biomarker for agricultural soil fumigant 1,3-dichloropropene [30]. In the first part of the studies summarized in this Review, attention is paid to MA derivatives of volatile anesthetics in humans, and whether they are applicable as biomarkers of effect.…”

Section: Mercapturic Acids: Potential Biomarkers Of Effectmentioning

confidence: 99%

Analyses of representative biomarkers of exposure and effect by chromatographic, mass spectrometric, and nuclear magnetic resonance techniques: Method development and application in life sciences

Orhan¹

2007

J of Separation Science

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Biomarkers are essential tools in monitoring studies, which include environmental monitoring, biological monitoring, biological effect monitoring, and health surveillance, as well as drug development processes. Their discovery, validation, and analysis require highly sensitive and selective analytical technologies. In this regard, gas and liquid chromatography, mass spectrometry, and nuclear magnetic resonance spectroscopy have facilitated great achievements in all these areas. In addition and closely related to biomarkers, the ongoing developments in these techniques promise a better understanding of the nature and mechanisms of toxic effects originating from various chemical, biological, or physical sources. This Review compiles studies performed on selected biomarkers with respect to both method development and application. Section 1 summarizes the concept of biomarkers; their application in various industrial/occupational, agricultural, drug developmental, and medical/clinical platforms. This section also focuses on biotransformation studies in close relation to biomarker discovery and validation, and on major techniques utilized in this area. In Section 2, biotransformation of volatile anesthetics in humans with a focus on mercapturic acid derivatives as potential biomarkers of effect is reviewed. The use of GC-ECD, GC/MS, and 19F-NMR in these studies is described. Section 3 focuses on the analysis of aldehydic lipid peroxidation degradation products by GC-ECD in mammalian cells in which oxidative stress induced chemically, and in humans after various challenges; anesthetic exposure, ischemia-reperfusion, and controlled endurance exercise. In Section 4, method development for protein and DNA oxidation products by LC-tandem MS and its application in mammalian cells and in humans are summarized. Possibilities, limitations, and future perspectives are discussed in Section 5.

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Glutathione and Mercapturic Acid Conjugates of Sulofenur and Their Activity against a Human Colon Cancer Cell Line

Cited by 21 publications

References 26 publications

Quercetin Selectively Inhibits Bioreduction and Enhances Apoptosis in Melanoma Cells That Overexpress Tyrosinase

Quercetin Selectively Inhibits Bioreduction and Enhances Apoptosis in Melanoma Cells That Overexpress Tyrosinase

Glutathione S-conjugates as prodrugs to target drug-resistant tumors

Analyses of representative biomarkers of exposure and effect by chromatographic, mass spectrometric, and nuclear magnetic resonance techniques: Method development and application in life sciences

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