Mji Paine
University of Dundee
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Publication
Featured researches published by Mji Paine.
Biochemical Society Transactions | 2008
Aldo Gutierrez; Alex Grunau; Mji Paine; Andrew W. Munro; Wolf Cr; G. C. K. Roberts; Nigel S. Scrutton
Cytochrome P450 reductase (CPR) is a diflavin enzyme responsible for electron donation to mammalian cytochrome P450 enzymes in the endoplasmic reticulum. Dissection of the enzyme into functional domains and studies by site-directed mutagenesis have enabled detailed characterization of the mechanism of electron transfer using stopped-flow and equilibrium-perturbation methods, and redox potentiometry. These studies and the mechanism of electron transfer in CPR are reported herein.
Scopus | 2006
Jinglei Yu; Clive J. Ward; Simon Brown; Elaine M. Rankin; Mji Paine; C. R. Wolf; J-D Maréchal; Michael J. Sutcliffe; Carol A. Kemp; G. C. K. Roberts
Patients with cancer often take many different classes of drugs to treat the effects of their malignancy and the side effects of treatment, as well as their comorbidities. The potential for drug-drug interactions that may affect the efficacy of anticancer treatment is high, and a major source of such interactions is competition for the drug-metabolizing enzymes, cytochromes P450 (P450s). We have examined a series of 20 drugs commonly prescribed to cancer patients to look for potential interactions via CYP2D6. We used a homology model of CYP2D6, together with molecular docking techniques, to perform an in silico screen for binding to CYP2D6. Experimental IC50 values were determined for these compounds and compared with the model predictions to reveal a correlation with a regression coefficient of r2 = 0.61. Importantly, the docked conformation of the commonly prescribed antiemetic metoclopramide predicted a new site of metabolism that was further investigated through in vitro analysis with recombinant CYP2D6. An aromatic N-hydroxy metabolite of metoclopramide, consistent with predictions from our modeling studies, was identified by high-performance liquid chromatography/mass spectrometry. This metabolite was found to represent a major product of metabolism in human liver microsomes, and CYP2D6 was identified as the main P450 isoform responsible for catalyzing its formation. In view of the prevalence of interindividual variation in the CYP2D6 genotype and phenotype, we suggest that those experiencing adverse reactions with metoclopramide, e.g., extrapyramidal syndrome, are likely to have a particular CYP2D6 genotype/phenotype. This warrants further investigation.
web science | 1996
Sandeep Modi; Mji Paine; Michael J. Sutcliffe; L.-Y. Lian; William U. Primrose; C. R. Wolf; G. C. K. Roberts
Biochemistry | 2000
Aldo Gutierrez; O. Doehr; Mji Paine; Wolf Cr; Nigel S. Scrutton; G. C. K. Roberts
Biochemistry | 2001
Mji Paine; S. Ayivor; Andrew W. Munro; Pascale Tsan; Lu-Yun Lian; G. C. K. Roberts; C. R. Wolf
In: Ortiz de Montellano P, editor(s). Cytochrome P450. Kluwer Academic/Plenum; 2004. p. 115-148. | 2004
Mji Paine; Nigel S. Scrutton; Andrew W. Munro; Roberts Gck; C. R. Wolf
In: Anzenbacher P, Hudecek J, editor(s). Cytochromes P450 biochemistry, biophysics and drug metabolism. Monduzzi Editore; 2003. p. 81-85. | 2003
Andrew W. Munro; Olivier Roitel; Kirsty J. McLean; Aldo Gutierrez; J Basran; Rajasekhar Neeli; Mji Paine; Robert Finn; C. R. Wolf; G. C. K. Roberts; Nigel S. Scrutton; P Anzenbacher; J Hudecek
Drug Metabolism Reviews | 2003
Aj van Eldik; J-D Maréchal; Carol A. Kemp; Jack U. Flanagan; Michael J. Sutcliffe; Mji Paine; Gck Roberts; Rc Wolf
Archive | 2002
Aldo Gutierrez; Mji Paine; C. R. Wolf; Nigel S. Scrutton; G. C. K. Roberts
Biochemical Society Transactions | 1999
G. C. K. Roberts; Q. Zhao; Sandeep Modi; Mji Paine; L.-Y. Lian; Hpc Driessen; C. R. Wolf
