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Dive into the research topics where Geoffrey P. McDermott is active.

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Featured researches published by Geoffrey P. McDermott.


Analytical Chemistry | 2011

Direct Detection of Biologically Significant Thiols and Disulfides with Manganese(IV) Chemiluminescence

Geoffrey P. McDermott; Jessica M. Terry; Xavier A. Conlan; Neil W. Barnett; Paul S. Francis

The quantification of low-molecular mass thiols and disulfides involved in cellular redox processes is hindered by oxidation or degradation of analytes during conventional sample preparation steps (including deproteinization and derivatization). Researchers therefore seek techniques that minimize sample handling and permit direct detection of thiols and disulfides within a single chromatographic separation. We demonstrate a new HPLC procedure for these biologically important analytes that incorporates direct chemiluminescence detection with a manganese(IV) reagent. A mixture of seven thiols and disulfides (cysteine, N-acetylcysteine, homocysteine, glutathione (GSH), glutathione disulfide (GSSG), cystine, and homocystine) in their native forms were separated using a C18 column within 20 min. Detection limits for these analytes ranged from 5 × 10(-8) to 1 × 10(-7) M, and the precision for retention times and peak areas was excellent, with relative standard deviations of less than 0.3% and 2%, respectively. This approach was employed to determine two key biomarkers of oxidative stress, GSH and GSSG, in whole blood taken from 12 healthy volunteers. Samples were deproteinized, centrifuged, and diluted prior to analysis using a simple procedure that was shown to avoid significant artificial oxidation of GSH.


Analytica Chimica Acta | 2009

Comparison of homoleptic and heteroleptic 2,2′-bipyridine and 1,10-phenanthroline ruthenium complexes as chemiluminescence and electrochemiluminescence reagents in aqueous solution

Michaela M. Cooke; Egan H. Doeven; Conor F. Hogan; Jacqui L. Adcock; Geoffrey P. McDermott; Xavier A. Conlan; Neil W. Barnett; Frederick M. Pfeffer; Paul S. Francis

We have conducted a comprehensive comparative study of Ru(bipy)(3)(2+), Ru(bipy)(2)(phen)(2+), Ru(bipy)(phen)(2)(2+), and Ru(phen)(3)(2+) as chemiluminescence and electrochemiluminescence (ECL) reagents, to address several previous conflicting observations and gain a greater insight into their potential for chemical analysis. Clear trends were observed in many of their spectroscopic and electrochemical properties, but the relative chemiluminescence or ECL intensity with a range of analytes/co-reactants is complicated by the contribution of numerous (sometimes opposing) factors. Significantly, the reversibility of cyclic voltammetric responses for the complexes decreased as the number of phenanthroline ligands was increased, due to the lower stability of their ruthenium(III) form in the aqueous solvent. This trend was also evident over a longer timescale when the ruthenium(III) form was spectrophotometrically monitored after chemical oxidation of the ruthenium(II) complexes. In general, the greater stability of Ru(bipy)(3)(3+) resulted in lower blank signals, although this effect was less pronounced with ECL, where the reagent is oxidised in the presence of the co-reactants. Nevertheless, this shows the need to compare signal-to-blank ratios or detection limits, rather than the more common comparisons of overall signal intensity for different ruthenium complexes. Furthermore, our results support previous observations that, compared to Ru(bipy)(3)(2+), Ru(phen)(3)(2+) provides greater ECL and chemiluminescence intensities with oxalate, which in some circumstances translates to superior detection limits, but they do not support the subsequent generalised notion that Ru(phen)(3)(2+) is a more sensitive reagent than Ru(bipy)(3)(2+) for all analytes.


Analytical Chemistry | 2011

Stable Tris(2,2′-bipyridine)ruthenium(III) for Chemiluminescence Detection

Geoffrey P. McDermott; Philip Jones; Neil W. Barnett; David N. Donaldson; Paul S. Francis

Two exceedingly stable [Ru(bipy)(3)](3+) reagents were prepared by dissolving either [Ru(bipy)(3)](ClO(4))(2) in acetonitrile (containing 0.05 M HClO(4)) or [Ru(bipy)(3)]Cl(2)·6H(2)O in 95:5 glacial acetic acid-acetic anhydride (containing 0.05 M H(2)SO(4)) followed by oxidation with PbO(2). These conveniently prepared solutions provide highly reproducible chemiluminescence detection over long periods of analysis, avoiding the need for recalibration or preparation of fresh reagent solutions and without the complications associated with online chemical or electrochemical oxidations. The reagent prepared in acetonitrile produced much greater signal intensities with a range of analytes and was deemed most suitable for high-performance liquid chromatography (HPLC) with postcolumn chemiluminescence detection.


Analytical Methods | 2010

Correlation between acidic potassium permanganate chemiluminescence and in vitro cell culture assay: Physiologically meaningful antioxidant activity

Xavier A. Conlan; Nicole Stupka; Geoffrey P. McDermott; Neil W. Barnett; Paul S. Francis

There is great interest in the activity of antioxidant molecules, including polyphenols, from food and plant sources. Acidic potassium permanganate chemiluminescence signal intensity was shown to predict the ability of polyphenols to positively act on cellular redox state and attenuate oxidative stress in cultured skeletal muscle cells.


Biomedical Chromatography | 2009

Determination of intracellular glutathione and cysteine using HPLC with a monolithic column after derivatization with monobromobimane

Xavier A. Conlan; Nicole Stupka; Geoffrey P. McDermott; Paul S. Francis; Neil W. Barnett

An optimized high-performance liquid chromatography (HPLC) method is used to show that, as myoblasts differentiate into multinucleated muscle fibers, there is a shift to a more oxidized cell redox state. The HPLC method incorporated derivatization with monobromobimane for the determination of the reduced (GSH) and oxidized (GSSG) forms of glutathione and the reduced (Cys) and oxidized (CysSS) forms of cysteine. The derivatization was optimized to improve the sensitivity of the approach; the limits of detection for glutathione and cysteine were 3 x 10(-8) and 5 x 10(-8) M, respectively.


Analytical Chemistry | 2013

Multiplexed target detection using DNA-binding dye chemistry in droplet digital PCR.

Geoffrey P. McDermott; Duc Do; Claudia Litterst; Dianna Maar; Christopher M. Hindson; Erin Steenblock; Tina C. Legler; Yann Jouvenot; Samuel H. Marrs; Adam Bemis; Pallavi Shah; Josephine Wong; Shenglong Wang; David Sally; Leanne Javier; Theresa Dinio; Chunxiao Han; Timothy P. Brackbill; Shawn Hodges; Yunfeng Ling; Niels Klitgord; George Carman; Jennifer R. Berman; Ryan Koehler; Amy L. Hiddessen; Pramod Walse; Luc J. Bousse; Svilen Tzonev; Eli Hefner; Benjamin J. Hindson


Analyst | 2011

Determination of intracellular glutathione and glutathione disulfide using high performance liquid chromatography with acidic potassium permanganate chemiluminescence detection

Geoffrey P. McDermott; Paul S. Francis; Kayla J. Holt; Kristen L. Scott; Sheree D. Martin; Nicole Stupka; Neil W. Barnett; Xavier A. Conlan


Talanta | 2010

High performance liquid chromatography with two simultaneous on-line antioxidant assays : evaluation and comparison of espresso coffees

Mariam Mnatsakanyan; Tiffany A. Goodie; Xavier A. Conlan; Paul S. Francis; Geoffrey P. McDermott; Neil W. Barnett; David Shock; Fabrice Gritti; Georges Guiochon; R. Andrew Shalliker


Analytica Chimica Acta | 2011

Screening for antioxidants in complex matrices using high performance liquid chromatography with acidic potassium permanganate chemiluminescence detection

Geoffrey P. McDermott; Xavier A. Conlan; Laura K. Noonan; Jason W. Costin; Mariam Mnatsakanyan; R. Andrew Shalliker; Neil W. Barnett; Paul S. Francis


Analytica Chimica Acta | 2010

High-performance liquid chromatography with post-column 2,2′-diphenyl-1-picrylhydrazyl radical scavenging assay: Methodological considerations and application to complex samples

Geoffrey P. McDermott; Laura K. Noonan; Mariam Mnatsakanyan; R. Andrew Shalliker; Xavier A. Conlan; Neil W. Barnett; Paul S. Francis

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Mariam Mnatsakanyan

University of Western Sydney

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