Your search keyword '"Southam, Andrew D."' showing total 9 results

1. Simultaneously discovering the fate and biochemical effects of pharmaceuticals through untargeted metabolomics.

Author

Bowen, Tara J., Southam, Andrew D., Hall, Andrew R., Weber, Ralf J. M., Lloyd, Gavin R., Macdonald, Ruth, Wilson, Amanda, Pointon, Amy, and Viant, Mark R.

Subjects

BIOTRANSFORMATION (Metabolism), BIOLOGICAL systems, METABOLOMICS, LIQUID chromatography-mass spectrometry, BIOCONVERSION

Abstract

Untargeted metabolomics is an established approach in toxicology for characterising endogenous metabolic responses to xenobiotic exposure. Detecting the xenobiotic and its biotransformation products as part of the metabolomics analysis provides an opportunity to simultaneously gain deep insights into its fate and metabolism, and to associate the internal relative dose directly with endogenous metabolic responses. This integration of untargeted exposure and response measurements into a single assay has yet to be fully demonstrated. Here we assemble a workflow to discover and analyse pharmaceutical-related measurements from routine untargeted UHPLC-MS metabolomics datasets, derived from in vivo (rat plasma and cardiac tissue, and human plasma) and in vitro (human cardiomyocytes) studies that were principally designed to investigate endogenous metabolic responses to drug exposure. Our findings clearly demonstrate how untargeted metabolomics can discover extensive biotransformation maps, temporally-changing relative systemic exposure, and direct associations of endogenous biochemical responses to the internal dose. Untargeted metabolomics enables simultaneous measurement of xenobiotic fate and effects in biological systems. This is demonstrated through discovering extensive biotransformation maps, measuring systemic exposures over time, and directly associating endogenous biochemical responses to internal dose. [ABSTRACT FROM AUTHOR]

Published

2023

2. Valproic acid disables the Nrf2 anti-oxidant response in acute myeloid leukaemia cells enhancing reactive oxygen species-mediated killing.

Author

Jiang, Yao, Southam, Andrew D., Trova, Sandro, Beke, Flavio, Alhazmi, Bader, Francis, Thomas, Radotra, Anshul, di Maio, Alessandro, Drayson, Mark T., Bunce, Chris M., and Khanim, Farhat L.

Subjects

*PROTEIN metabolism, *ANTICONVULSANTS, *ANTILIPEMIC agents, *DRUG dosage, *CLINICAL trials, *MEDROXYPROGESTERONE, *NUCLEAR factor E2 related factor, *ANTIOXIDANTS, *RESEARCH funding, *REACTIVE oxygen species, *CELL lines, *VALPROIC acid, *DRUG toxicity, *PHARMACODYNAMICS

Abstract

Background: We previously demonstrated the in vitro killing of AML cells by the combination of the lipid-lowering agent bezafibrate (BEZ) and the contraceptive hormone medroxyprogesterone acetate (MPA). A phase II trial demonstrated in vivo safety and efficacy of BEZ and MPA (BaP) in elderly, relapsed/refractory AML and high-risk myelodysplastic syndrome (MDS) patients. However, we observed dose-limiting toxicities in a second trial that attempted to improve outcomes via escalation of BaP doses. Thus we sought to identify a third repurposed drug that potentiates activity of low dose BaP (BaP 0.1 mM).Methods and Results: We demonstrate that addition of a commonly used anti-epileptic, valproic acid (VAL) to low dose BaP (BaP 0.1 mM)(VBaP) enhanced killing of AML cell lines/primary AML cells to levels similar to high dose BaP (BaP 0.5 mM). Similarly, addition of VAL to BaP 0.1 mM enhanced reactive oxygen species (ROS), lipid peroxidation and inhibition of de novo fatty acid synthesis. Overexpression of Nrf2 in K562 and KG1a completely inhibited ROS production and rescued cells from VAL/BaP 0.1 mM/VBaP killing.Conclusions: Given the good safety data of low-dose BaP in elderly/relapsed/refractory AML patients, and that VAL alone is well-tolerated, we propose VBaP as a novel therapeutic combination for AML. [ABSTRACT FROM AUTHOR]

Published

2022

3. Cytoglobin protects cancer cells from apoptosis by regulation of mitochondrial cardiolipin.

Author

Thorne, Lorna S., Rochford, Garret, Williams, Timothy D., Southam, Andrew D., Rodriguez-Blanco, Giovanny, Dunn, Warwick B., and Hodges, Nikolas J.

Subjects

SQUAMOUS cell carcinoma, CANCER invasiveness, APOPTOSIS, CARDIOLIPIN, PHENOTYPES, CELL proliferation

Abstract

Cytoglobin is important in the progression of oral squamous cell carcinoma but the molecular and cellular basis remain to be elucidated. In the current study, we develop a new cell model to study the function of cytoglobin in oral squamous carcinoma and response to cisplatin. Transcriptomic profiling showed cytoglobin mediated changes in expression of genes related to stress response, redox metabolism, mitochondrial function, cell adhesion, and fatty acid metabolism. Cellular and biochemical studies show that cytoglobin expression results in changes to phenotype associated with cancer progression including: increased cellular proliferation, motility and cell cycle progression. Cytoglobin also protects cells from cisplatin-induced apoptosis and oxidative stress with levels of the antioxidant glutathione increased and total and mitochondrial reactive oxygen species levels reduced. The mechanism of cisplatin resistance involved inhibition of caspase 9 activation and cytoglobin protected mitochondria from oxidative stress-induced fission. To understand the mechanism behind these phenotypic changes we employed lipidomic analysis and demonstrate that levels of the redox sensitive and apoptosis regulating cardiolipin are significantly up-regulated in cells expressing cytoglobin. In conclusion, our data shows that cytoglobin expression results in important phenotypic changes that could be exploited by cancer cells in vivo to facilitate disease progression. [ABSTRACT FROM AUTHOR]

Published

2021

4. Metabolic characterisation of disturbances in the APOC3/triglyceride-rich lipoprotein pathway through sample-based recall by genotype.

Author

Corbin, Laura J., Hughes, David A., Chetwynd, Andrew J., Taylor, Amy E., Southam, Andrew D., Jankevics, Andris, Weber, Ralf J. M., Groom, Alix, Dunn, Warwick B., and Timpson, Nicholas J.

Subjects

GENOTYPES, TREATMENT effectiveness, METABOLITES, CARDIOVASCULAR diseases

Abstract

Introduction: High plasma triacylglyceride levels are known to be associated with increased risk of atherosclerotic cardiovascular disease. Apolipoprotein C-III (apoC-III) is a key regulator of plasma triacylglyceride levels and is associated with hypertriglyceridemia via a number of pathways. There is consistent evidence for an association of cardiovascular events with blood apoC-III level, with support from human genetic studies of APOC3 variants. As such, apoC-III has been recognised as a potential therapeutic target for patients with severe hypertriglyceridaemia with one of the most promising apoC-III-targeting drugs, volanesorsen, having recently progressed through Phase III trials. Objectives: To exploit a rare loss of function variant in APOC3 (rs138326449) to characterise the potential long-term treatment effects of apoC-III targeting interventions on the metabolome. Methods: In a recall-by-genotype study, 115 plasma samples were analysed by UHPLC-MS to acquire non-targeted metabolomics data. The study included samples from 57 adolescents and 33 adults. Overall, 12 985 metabolic features were tested for an association with APOC3 genotype. Results: 161 uniquely annotated metabolites were found to be associated with rs138326449(APOC3). The highest proportion of associated metabolites belonged to the acyl-acyl glycerophospholipid and triacylglyceride metabolite classes. In addition to the anticipated (on-target) reduction of metabolites in the triacylglyceride and related classes, carriers of the rare variant exhibited previously unreported increases in levels of a number of metabolites from the acyl-alkyl glycerophospholipid class. Conclusion: Overall, our results suggest that therapies targeting apoC-III may potentially achieve a broad shift in lipid profile that favours better metabolic health. [ABSTRACT FROM AUTHOR]

Published

2020

5. Characterisation of the dynamic nature of lipids throughout the lifespan of genetically identical female and male Daphnia magna.

Author

Constantinou, Julia K., Southam, Andrew D., Kvist, Jouni, Jones, Martin R., Viant, Mark R., and Mirbahai, Leda

Subjects

*LIPIDS, *DAPHNIA magna, *TRIGLYCERIDES, *DIGLYCERIDES, *CERAMIDES

Abstract

Lipids play a significant role in regulation of health and disease. To enhance our understanding of the role of lipids in regulation of lifespan and healthspan additional studies are required. Here, UHPLC-MS/MS lipidomics was used to measure dynamic changes in lipid composition as a function of age and gender in genetically identical male and female Daphnia magna with different average lifespans. We demonstrate statistically significant age-related changes in triglycerides (TG), diglycerides (DG), phosphatidylcholine, phosphatidylethanolamine, ceramide and sphingomyelin lipid groups, for example, in males, 17.04% of TG lipid species decline with age whilst 37.86% increase in relative intensity with age. In females, 23.16% decrease and 25.31% increase in relative intensity with age. Most interestingly, the rate and direction of change can differ between genetically identical female and male Daphnia magna, which could be the cause and/or the consequence of the different average lifespans between the two genetically identical genders. This study provides a benchmark dataset to understand how lipids alter as a function of age in genetically identical female and male species with different average lifespan and ageing rate. [ABSTRACT FROM AUTHOR]

Published

2020

6. A complete workflow for high-resolution spectral-stitching nanoelectrospray direct-infusion mass-spectrometry-based metabolomics and lipidomics.

Author

Southam, Andrew D, Weber, Ralf J M, Engel, Jasper, Jones, Martin R, and Viant, Mark R

Published

2017

7. Correction to: Metabolic characterisation of disturbances in the APOC3/triglyceride‑rich lipoprotein pathway through sample‑based recall by genotype.

Author

Corbin, Laura J., Hughes, David A., Chetwynd, Andrew J., Taylor, Amy E., Southam, Andrew D., Jankevics, Andris, Weber, Ralf J. M., Groom, Alix, Dunn, Warwick B., and Timpson, Nicholas J.

Subjects

METABOLIC disorders, GENOTYPES, CHYLOMICRONS, METABOLITES

Abstract

As a result of incorrect processing of two raw datasets presented (LIPIDS-POS and LIPIDS-NEG), some metabolite annotations reported in the original publication were incorrectly labeled. Correction of this error has resulted in the number of metabolite annotations changing from 183 to 213 and this has altered the number of metabolites reported in each lipid class. This presents a necessary technical update to the original paper, however the biological conclusions advanced in the original publication are largely unaltered. The biological interpretation of the ceramide lipid class was altered given the amended metabolite annotations. This error came to the attention of the authors after article publication. [ABSTRACT FROM AUTHOR]

Published

2021

8. Distinguishing between the metabolome and xenobiotic exposome in environmental field samples analysed by direct-infusion mass spectrometry based metabolomics and lipidomics

Author

Southam, Andrew D., Lange, Anke, Al-Salhi, Raghad, Hill, Elizabeth M., Tyler, Charles R., and Viant, Mark R.

Subjects

Exposome, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Xenometabolome, Original Article, Rutilus rutilus, Lipidome, Endometabolome, Biochemistry

Abstract

Environmental metabolomics is increasingly used to investigate organismal responses to complex chemical mixtures, including waste water effluent (WWE). In parallel, increasingly sensitive analytical methods are being used in metabolomics studies, particularly mass spectrometry. This introduces a considerable, yet overlooked, challenge that high analytical sensitivity will not only improve the detection of endogenous metabolites in biological specimens but also exogenous chemicals. If these often unknown xenobiotic features are not removed from the “biological” dataset, they will bias the interpretation and could lead to incorrect conclusions about the biotic response. Here we illustrate and validate a novel workflow classifying the origin of peaks detected in biological samples as: endogenous, xenobiotics, or metabolised xenobiotics. The workflow is demonstrated using direct infusion mass spectrometry-based metabolomic analysis of testes from roach exposed to different concentrations of a complex WWE. We show that xenobiotics and their metabolic products can be detected in roach testes (including triclosan, chloroxylenol and chlorophene), and that these compounds have a disproportionately high level of statistical significance within the total (bio)chemical changes induced by the WWE. Overall we have demonstrated that this workflow extracts more information from an environmental metabolomics study of complex mixture exposures than was possible previously. Electronic supplementary material The online version of this article (doi:10.1007/s11306-014-0693-3) contains supplementary material, which is available to authorized users.

9. Multiple metabolic pathways are predictive of ricin intoxication in a rat model.

Author

D'Elia, Riccardo V., Goodchild, Sarah A., Winder, Catherine L., Southam, Andrew D., Weber, Ralf J. M., Stahl, Fiona M., Docx, Cerys, Patel, Vikesh, Green, A. Christopher, Viant, Mark R., Lukaszewski, Roman A., and Dunn, Warwick B.

Subjects

RICIN, BILE acids, RATS, ETHYLENE glycol, UNIVARIATE analysis

Abstract

Introduction: Exposure to ricin can be lethal and treatments that are under development have short windows of opportunity for administration after exposure. It is therefore essential to achieve early detection of ricin exposure to provide the best prognosis for exposed individuals. Ricin toxin can be detected in clinical samples via several antibody-based techniques, but the efficacy of these can be limited due to the rapid processing and cellular uptake of toxin in the body and subsequent low blood ricin concentrations. Other diagnostic tools that perform, in an orthogonal manner, are therefore desirable. Objectives: To determine time-dependent metabolic changes in Sprague–Dawley rats following intravenous exposure to ricin. Methods: Sprague–Dawley rats were intravenously exposed to ricin and multiple blood samples were collected from each animal for up to 48 h following exposure in two independent studies. Plasma samples were analysed applying HILIC and C18 reversed phase UHPLC–MS assays followed by univariate and multivariate analysis. Results: In Sprague–Dawley rats we have demonstrated that metabolic changes measured in blood can distinguish between rats exposed intravenously to ricin and controls prior to the onset of behavioral signs of intoxication after 24 h. A total of 37 metabolites were significantly altered following exposure to ricin when compared to controls. The arginine/proline, bile acid and triacylglyceride metabolic pathways were highlighted as being important with two triacylglycerides at 8 h post exposure giving an AUROC score of 0.94. At 16 h and 24 h the AUROC score increased to 0.98 and 1.0 with the number of metabolites in the panel increasing to 5 and 7, respectively. Conclusions: These data demonstrate that metabolites may be a useful tool to diagnose and detect ricin exposure, thus increasing the effectiveness of supportive therapy and future ricin-specific medical treatments. [ABSTRACT FROM AUTHOR]

Published

2019