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Featured researches published by Phong X. Nguyen.


Toxicology and Applied Pharmacology | 2014

Flavin-containing monooxygenase S-oxygenation of a series of thioureas and thiones

Marilyn C. Henderson; Lisbeth K. Siddens; Sharon K. Krueger; J. Fred Stevens; Karen M. Kedzie; Wenkui K. Fang; Todd M. Heidelbaugh; Phong X. Nguyen; Ken Chow; Michael E. Garst; Daniel W. Gil; David E. Williams

Mammalian flavin-containing monooxygenase (FMO) is active towards many drugs with a heteroatom having the properties of a soft nucleophile. Thiocarbamides and thiones are S-oxygenated to the sulfenic acid which can either react with glutathione and initiate a redox-cycle or be oxygenated a second time to the unstable sulfinic acid. In this study, we utilized LC-MS/MS to demonstrate that the oxygenation by hFMO of the thioureas under test terminated at the sulfenic acid. With thiones, hFMO catalyzed the second reaction and the sulfinic acid rapidly lost sulfite to form the corresponding imidazole. Thioureas are often pulmonary toxicants in mammals and, as previously reported by our laboratory, are excellent substrates for hFMO2. This isoform is expressed at high levels in the lung of most mammals, including non-human primates. Genotyping to date indicates that individuals of African (up to 49%) or Hispanic (2-7%) ancestry have at least one allele for functional hFMO2 in lung, but not Caucasians nor Asians. In this study the major metabolite formed by hFMO2 with thioureas from Allergan, Inc. was the sulfenic acid that reacted with glutathione. The majority of thiones were poor substrates for hFMO3, the major form in adult human liver. However, hFMO1, the major isoform expressed in infant and neonatal liver and adult kidney and intestine, readily S-oxygenated thiones under test, with Kms ranging from 7 to 160 μM and turnover numbers of 30-40 min(-1). The product formed was identified by LC-MS/MS as the imidazole. The activities of the mouse and human FMO1 and FMO3 orthologs were in good agreement with the exception of some thiones for which activity was much greater with hFMO1 than mFMO1.


Archive | 2008

4-(substituted cycloalkylmethyl) imidazole-2-thiones, 4-(substituted cycloalkenylmethyl) imidazole-2-thiones, 4-(substituted cycloalkylmethyl) imidazol-2-ones and 4-(substituted cycloalkenylmethyl) imidazol-2-ones and related compounds

Ken Chow; Todd M. Heidelbaugh; Daniel W. Gil; Michael E. Garst; Larry A. Wheeler; Phong X. Nguyen; Dario G. Gomez


Archive | 2003

4-substituted imidazole-2-thiones and imidazol-2-ones as agonists of the alpha-2b and alpha-2c adrenergic receptors

Ken Chow; Todd M. Heidelbaugh; Daniel W. Gil; Michael E. Garst; Larry A. Wheeler; Phong X. Nguyen; Dario G. Gomez


Journal of Organic Chemistry | 2003

A convenient synthesis of 7-Halo-1-indanones and 8-Halo-1-tetralones

Phong X. Nguyen; Evelyn G. Corpuz; Todd M. Heidelbaugh; Ken Chow; Michael E. Garst


Archive | 2004

4-(2-Methyl-5,6,7,8-tetrahydro-quinolin-7-ylmethyl)-1,3-dihydro-imidazole-2-thione as specific alpha2B agonist and methods of using the same

Todd M. Heidelbaugh; Ken Chow; Phong X. Nguyen; Daniel W. Gil; John E. Donello


Archive | 2006

Alpha-2 adrenergic agonists for the treatment of pain

Ken Chow; Todd M. Heidelbaugh; Phong X. Nguyen; Santosh C. Sinha


Archive | 2010

Compounds as receptor modulators with therapeutic utility

Todd M. Heidelbaugh; Phong X. Nguyen


Archive | 2008

Quinolynylmethylimidizoles as therapeutic agents

Todd M. Heidelbaugh; Phong X. Nguyen; Ken Chow; Michael E. Garst


Archive | 2005

4-(heteroaryl-methyl and substituted heteroaryl-methyl)-imidazole-2-thiones acting as alpha2 adrenergic agonists

Todd M. Heidelbaugh; Ken Chow; Phong X. Nguyen; Daniel W. Gil; John E. Donello; Michael E. Garst; Larry A. Wheeler


Archive | 2005

4-(phenylmethyl and substituted phenylmethyl)-imidazole-2-thiones acting as specific alpha2 adrenergic agonists

Todd M. Heidelbaugh; Ken Chow; Phong X. Nguyen; Daniel W. Gil; John E. Donello; Michael E. Garst; Larry A. Wheeler

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