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Dive into the research topics where Sharvil Patel is active.

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Featured researches published by Sharvil Patel.


Journal of Chromatography B | 2003

Determination of the enantiomers of ketamine and norketamine in human plasma by enantioselective liquid chromatography–mass spectrometry

Maria Esther Rodriguez Rosas; Sharvil Patel; Irving W. Wainer

A sensitive enantioselective liquid chromatographic assay with mass spectrometric detection has been developed and validated for the simultaneous determination of plasma concentrations of (R)- and (S)-ketamine, and (R)- and (S)-norketamine. The compounds were extracted from human plasma using solid-phase extraction and then directly injected into the LC-MS system for detection and quantification. Enantioselective separations were achieved on a liquid chromatographic chiral stationary phase based upon immobilized alpha(1)-acid glycoprotein (the Chiral AGP column). The separations were achieved using a mobile phase composed of 2-propanol-ammonium acetate buffer (10 mM, pH 7.6) (6:94, v/v), a flow-rate of 0.5 ml/min and a temperature of 25 degrees C. Under these conditions, the analysis time was 20 min. Detection of the ketamine, norketamine and bromoketamine (internal standard) enantiomers was achieved using selected ion monitoring at m/z 238.1, 224.1 and 284.0, respectively. Extracted calibration curves were linear from 1 to 125 ng/ml per enantiomer for each analyte with correlation coefficients better than 0.9993 and intra- and inter-day RSDs of less than 8.0%. The method was applied to samples from a clinical study of ketamine in pain management.


Journal of Chromatography B | 2008

Exploring enantiospecific ligand-protein interactions using cellular membrane affinity chromatography: chiral recognition as a dynamic process.

Krzysztof Jozwiak; Ruin Moaddel; Sarangan Ravichandran; Anita Plazinska; Joanna Kozak; Sharvil Patel; Rika Yamaguchi; Irving W. Wainer

The chiral recognition mechanisms responsible for the enantioselective binding on the alpha3beta4 nicotinic acetylcholine receptor (alpha3 beta4 nAChR) and human organic cation transporter 1 (hOCT1) have been reviewed. The results indicate that chiral recognition on the alpha3beta4 nAChR is a process involving initial tethering of dextromethorphan and levomethorphan at hydrophobic pockets within the central lumen followed by hydrogen bonding interactions favoring dextromethorphan. The second step is the defining enantioselective step. Studies with the hOCT1 indentified four binding sites within the transporter that participated in chiral recognition. Each of the enantiomers of the compounds used in the study interacted with three of these sites, while (R)-verapamil interacted with all four. Chiral recognition arose from the conformational adjustments required to produce optimum interactions. With respect to the prevailing interaction-based models, the data suggest that chiral recognition is a dynamic process and that the static point-based models should be amended to reflect this.


Analytical Biochemistry | 2010

Stereoselective binding of chiral ligands to single nucleotide polymorphisms of the human organic cation transporter-1 determined using cellular membrane affinity chromatography

Ruin Moaddel; F. Bighi; Rika Yamaguchi; Sharvil Patel; Sarangan Ravichandran; Irving W. Wainer

Membranes from stably transfected cell lines that express two point mutations of the human organic cation transporter-1 (hOCT1), R488M and G465R, have been immobilized on the immobilized artificial membrane (IAM) liquid chromatographic stationary phase to form two cellular membrane affinity chromatography (CMAC) columns, CMAC(hOCT1(G465R)) and CMAC(hOCT1(R488M)). Columns were created using both stationary phases, and frontal displacement chromatography experiments were conducted using [(3)H] MMP(+) (1-methyl-4-phenylpyridinium) as the marker ligand and various displacers, including the single enantiomers of verapamil, fenoterol, and isoproterenol. The chromatographic data obtained were used to refine a previously developed pharmacophore for hOCT1.


Journal of Chromatography B | 2005

Development and characterization of an immobilized human organic cation transporter based liquid chromatographic stationary phase.

Ruin Moaddel; Rika Yamaguchi; P.C. Ho; Sharvil Patel; C.-P. Hsu; V. Subrahmanyam; Irving W. Wainer


Analytica Chimica Acta | 2006

Identification of P-glycoprotein substrates using open tubular chromatography on an immobilized P-glycoprotein column: Comparison of chromatographic results with Caco-2 permeability.

Ruin Moaddel; Rachid Hamid; Sharvil Patel; Peter L. Bullock; Irving W. Wainer


Chirality | 2005

Enantioselective binding to the human organic cation transporter-1 (hOCT1) determined using an immobilized hOCT1 liquid chromatographic stationary phase

Ruin Moaddel; Sharvil Patel; Krzysztof Jozwiak; Rika Yamaguchi; P.C. Ho; Irving W. Wainer


Archive | 2005

Chromatographic Studies of Molecular Recognition and Solute Binding to Enzymes and Plasma Proteins

W. John Lough; Irving W. Wainer; Sharvil Patel


Archive | 2005

Affinity-Based Chiral Stationary Phases

W. John Lough; Irving W. Wainer; Sharvil Patel


The FASEB Journal | 2006

Development of an immobilized mutant organic cation transporter column for on-line screening using chromatographic techniques

Ruin Moaddel; Federica Bighi; Rika Yamaguchi; Sharvil Patel; Irving W. Wainer


Journal of Chromatography B: Biomedical Sciences and Applications | 2002

Multidimensional on-line screening for ligands to the α3β4 neuronal nicotinic acetylcholine receptor using an immobilized nicotinic receptor liquid chromatographic stationary phase

Michael T. Baynham; Sharvil Patel; Ruin Moaddel; Irving W. Wainer

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Irving W. Wainer

National Institutes of Health

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Ruin Moaddel

National Institutes of Health

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Rika Yamaguchi

National Institutes of Health

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Krzysztof Jozwiak

Medical University of Lublin

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P.C. Ho

National Institutes of Health

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Sarangan Ravichandran

Science Applications International Corporation

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Anita Plazinska

Medical University of Lublin

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Joanna Kozak

Medical University of Lublin

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F. Bighi

National Institutes of Health

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