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Dive into the research topics where J. J. De Voss is active.

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Featured researches published by J. J. De Voss.


Journal of Clinical Pharmacy and Therapeutics | 2004

Permeability studies of alkylamides and caffeic acid conjugates from echinacea using a Caco-2 cell monolayer model

A. Matthias; Joanne T. Blanchfield; Kerry Penman; Istvan Toth; C. S. Lang; J. J. De Voss; Reg Lehmann

Background:  Echinacea is composed of three major groups of compounds that are thought to be responsible for stimulation of the immune system – the caffeic acid conjugates, alkylamides and polysaccharides. This study has focussed on the former two classes, as these are the constituents found in ethanolic liquid extracts.


Metabolic Engineering | 2011

Facile production of minor metabolites for drug development using a CYP3A shuffled library

Dominic J. B. Hunter; James B. Y. H. Behrendorff; Wayne A. Johnston; Patricia Y. Hayes; Weiliang Huang; B. Bonn; Martin A. Hayes; J. J. De Voss; Elizabeth M. J. Gillam

Metabolic profiling of new drugs is limited by the difficulty in obtaining sufficient quantities of minor metabolites for definitive structural identification. Biocatalytic methods offer the potential to produce metabolites that are difficult to synthesize by traditional medicinal chemistry. We hypothesized that the regioselectivity of the drug metabolizing cytochrome P450s could be altered by directed evolution to produce minor metabolites of drugs in development. A biocatalyst library was constructed by DNA shuffling of four CYP3A forms. The library contained 11 ± 4 (mean ± SD) recombinations and 1 ± 1 spontaneous mutations per mutant. On expression in Escherichia coli, 96% of mutants showed detectable activity to at least one probe substrate. Using testosterone as a model drug-like substrate, mutants were found that preferentially formed metabolites produced in only trace amounts by parental forms. A single 1.6L batch culture of one such mutant enabled the facile isolation of 0.3mg of the minor metabolite 1β-hydroxytestosterone and its ab initio structural determination by 1D- and 2D-NMR spectroscopy.


Chemico-Biological Interactions | 2005

Cytochrome P450 enzyme-mediated degradation of Echinacea alkylamides in human liver microsomes

A. Matthias; Elizabeth M. J. Gillam; Kerry Penman; Nicholas J. Matovic; K. M. Bone; J. J. De Voss; Reg Lehmann


Planta Medica | 2016

Is DNA Barcoding Using Universal Barcodes A Useful Test For Botanical Raw Materials, Extracts And Products?

H Wohlmuth; D Leach; K McGrath; L Gordon; Peter Mouatt; J. J. De Voss


Planta Medica | 2007

NMR studies found that a commercially supplied standard reference purported to be Withanolide D was instead Withanolide A

Kerry Penman; K. M. Bone; P.C. Hayes; J. J. De Voss; A. Agarwal; B Murali; D. Mundkinajeddu; A. Mayachari; R. Shenoy; R. P. Lehmann


Planta Medica | 2016

An assessment of the utility of DNA barcoding in the quality control of herbal raw materials, extracts and finished products

H Wohlmuth; D Leach; K McGrath; L Gordon; Peter Mouatt; J. J. De Voss


Planta Medica | 2016

Establishing compositional guidelines for flavonoids and saponins in Gynostemma pentaphyllum

D Leach; I Ahmed; J. J. De Voss; H Wohlmuth


ICCC2009: 16th International Conference on Cytochrome P450. Biochemistry, Biophysics, Biotechnology | 2009

Cytochrome P450-mediated fatty acid oxidation: Mechanistic investigations

Arti A. Singh; Max J. Cryle; Dominic J. B. Hunter; Jeanette E. Stok; J. J. De Voss


Planta Medica | 2006

Prevalence of three tetraene alkamide isomers in Echinacea angustifolia and Echinacea purpurea roots

R. P. Lehmann; A. Matthias; Nicholas J. Matovic; Kerry Penman; K. M. Bone; J. J. De Voss


14th European Symposium in Organic Chemistry | 2005

Synthesis of polyunsaturated alkyl amide constituents from Echinacea

Nicholas J. Matovic; J. J. De Voss

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Kerry Penman

University of Queensland

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A. Matthias

University of Queensland

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D Leach

University of Sydney

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H Wohlmuth

University of Queensland

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L. Notley

University of Queensland

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