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James Grogan

Researcher at Boston University

Publications -  21
Citations -  1854

James Grogan is an academic researcher from Boston University. The author has contributed to research in topics: Histatin & Cytochrome P450. The author has an hindex of 17, co-authored 21 publications receiving 1787 citations. Previous affiliations of James Grogan include Boston Medical Center & University of California, Santa Barbara.

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Journal Article

Selective biotransformation of taxol to 6 alpha-hydroxytaxol by human cytochrome P450 2C8.

TL;DR: Analysis of membrane fractions from Hep G2 cells infected with recombinant vaccinia viruses shows that human biotransformation routes of taxol result from catalysis by specific enzymes of two P450 families and that taxol 6 alpha-hydroxylation is a useful indicator of P450 2C8 activity in human hepatic microsomes.
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Saliva and dental pellicle--a review.

TL;DR: Improved pellicle harvesting procedures and analysis by state-of-the-art proteomics with mass spectroscopy approaches promise to make major inroads into the characterization of enamel pellicles.
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Activation of CYP3A4: evidence for the simultaneous binding of two substrates in a cytochrome P450 active site.

TL;DR: Kinetic analyses of these two substrates show that 7,8-benzoflavone increases the Vmax of phenanthrene metabolism without changing the Km and that Phenanthrene decreases the V max of 7, 8-benZ oflavone metabolism without increasing the KM, providing the first evidence that two different molecules can be simultaneously bound to the same P450 active site.
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Compositional analysis of human acquired enamel pellicle by mass spectrometry

TL;DR: An improved method of harvesting pellicle that combines mechanical and chemical removal is described and this approach was used to investigate systematically the desorption of in vitro pellicles components with different solutions.
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Is salivary histatin 5 a metallopeptide

TL;DR: Results indicate that histatin 5 exhibits metallopeptide-like properties and may contribute significantly to salivary metal binding capacity.