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Featured researches published by Dionne Arthur.


PLOS ONE | 2015

Ascites Bacterial Burden and Immune Cell Profile Are Associated with Poor Clinical Outcomes in the Absence of Overt Infection

Kevin J. Fagan; Geraint B. Rogers; Michelle Melino; Dionne Arthur; Mary-Ellen Costello; Mark Morrison; Elizabeth E. Powell; Katharine M. Irvine

Bacterial infections, most commonly spontaneous bacterial peritonitis in patients with ascites, occur in one third of admitted patients with cirrhosis, and account for a 4-fold increase in mortality. Bacteria are isolated from less than 40% of ascites infections by culture, necessitating empirical antibiotic treatment, but culture-independent studies suggest bacteria are commonly present, even in the absence of overt infection. Widespread detection of low levels of bacteria in ascites, in the absence of peritonitis, suggests immune impairment may contribute to higher susceptibility to infection in cirrhotic patients. However, little is known about the role of ascites leukocyte composition and function in this context. We determined ascites bacterial composition by quantitative PCR and 16S rRNA gene sequencing in 25 patients with culture-negative, non-neutrocytic ascites, and compared microbiological data with ascites and peripheral blood leukocyte composition and phenotype. Bacterial DNA was detected in ascitic fluid from 23 of 25 patients, with significant positive correlations between bacterial DNA levels and poor 6-month clinical outcomes (death, readmission). Ascites leukocyte composition was variable, but dominated by macrophages or T lymphocytes, with lower numbers of B lymphocytes and natural killer cells. Consistent with the hypothesis that impaired innate immunity contributes to susceptibility to infection, high bacterial DNA burden was associated with reduced major histocompatibility complex class II expression on ascites (but not peripheral blood) monocytes/macrophages. These data indicate an association between the presence of ascites bacterial DNA and early death and readmission in patients with decompensated cirrhosis. They further suggest that impairment of innate immunity contributes to increased bacterial translocation, risk of peritonitis, or both.


Chemosphere | 2013

Assessing benzene-induced toxicity on wild type Euglena gracilis Z and its mutant strain SMZ.

Cheng Peng; Dionne Arthur; Homa Teimouri Sichani; Qing Xia; J. C. Ng

Benzene is a representative member of volatile organic compounds and has been widely used as an industrial solvent. Groundwater contamination of benzene may pose risks to human health and ecosystems. Detection of benzene in the groundwater using chemical analysis is expensive and time consuming. In addition, biological responses to environmental exposures are uninformative using such analysis. Therefore, the aim of this study was to employ a microorganism, Euglena gracilis (E. gracilis) as a putative model to monitor the contamination of benzene in groundwater. To this end, we examined the wild type of E. gracilis Z and its mutant form, SMZ in their growth rate, morphology, chlorophyll content, formation of reactive oxygen species (ROS) and DNA damage in response to benzene exposure. The results showed that benzene inhibited cell growth in a dose response manner up to 48 h of exposure. SMZ showed a greater sensitivity compared to Z in response to benzene exposure. The difference was more evident at lower concentrations of benzene (0.005-5 μM) where growth inhibition occurred in SMZ but not in Z cells. We found that benzene induced morphological changes, formation of lipofuscin, and decreased chlorophyll content in Z strain in a dose response manner. No significant differences were found between the two strains in ROS formation and DNA damage by benzene at concentrations affecting cell growth. Based on these results, we conclude that E. gracilis cells were sensitive to benzene-induced toxicities for certain endpoints such as cell growth rate, morphological change, depletion of chlorophyll. Therefore, it is a potentially suitable model for monitoring the contamination of benzene and its effects in the groundwater.


Toxicology and Applied Pharmacology | 2012

Metabolism of bilirubin by human cytochrome P450 2A6

A'edah Abu-Bakar; Dionne Arthur; Anna Wikman; Minna Rahnasto; Risto O. Juvonen; Jouko Vepsäläinen; Hannu Raunio; J. C. Ng; Matti A. Lang


Toxicology and Applied Pharmacology | 2011

Inducible bilirubin oxidase: A novel function for the mouse cytochrome P450 2A5

A'edah Abu-Bakar; Dionne Arthur; Simona Aganovic; J. C. Ng; Matti A. Lang


Cell Biology and Toxicology | 2013

Genotoxicity of hydroquinone in A549 cells

Cheng Peng; Dionne Arthur; F. F. Liu; Jongwha Lee; Qing Xia; Martin F. Lavin; J. C. Ng


Organic and Biomolecular Chemistry | 2016

Synthesis of L-indospicine, [5,5,6-2H3]-L-indospicine and L-norindospicine

Cheng-Shan Lang; Siew Hoon Wong; Sharon Chow; Victoria L. Challinor; Ken W. L. Yong; Mary T. Fletcher; Dionne Arthur; J. C. Ng; James J. De Voss


Journal of Toxicological Sciences | 2012

Urinary excretion of bilirubin oxidative metabolites in arsenite-treated mice

Dionne Arthur; J. C. Ng; Matti A. Lang; A’edah Abu-Bakar


Understanding the Geological and Medical Interface of Arsenic, As 2012 - 4th International Congress: Arsenic in the Environment | 2012

Bilirubin oxidative metabolites: Novel biomarkers for acute arsenite exposure?

A'edah Abu-Bakar; Dionne Arthur; J. C. Ng


Archive | 2010

Bilirubin metabolism during arsenic toxicity of the liver: involvement of murine cytochrome P450 2a5 and its human orthologue CYP2A6

Dionne Arthur


18th International Symposium on Microsomes and Drug Oxidations (MDO) | 2010

Bilirubin degradation by cytochrome P450 2A: caharacterization of metabolites by high performance liquid chromatography/electrospray ionization mass spectrometry

A'edah Abu-Bakar; Dionne Arthur; G. Eaglesham; Matti A. Lang

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J. C. Ng

University of Queensland

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Cheng Peng

University of Queensland

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Qing Xia

University of Queensland

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