Your search keyword '"Khuntikeo, Narong"' showing total 2 results

1. Mapping of population disparities in the cholangiocarcinoma urinary metabolome.

Author

Alsaleh, Munirah, Leftley, Zoe, O'Connor, Thomas, Hughes, Thomas, Barbera, Thomas A., Koomson, Larry K., Zabron, Abigail, Reeves, Helen, Cramp, Matthew, Ryder, Stephen D., Greer, Shaun, Prince, Martin, Sithithaworn, Paiboon, Khuntikeo, Narong, Loilome, Watcharin, Yongvanit, Puangrat, Cox, I. Jane, Williams, Roger, Wadsworth, Christopher A., and Holmes, Elaine

Subjects

CHOLANGIOCARCINOMA, BODY composition, MASS spectrometry, BODY weight, MICROBIAL metabolism, ENTEROHEPATIC circulation, BIOMARKERS, TUMOR markers

Abstract

Phenotypic diversity in urinary metabolomes of different geographical populations has been recognized recently. In this study, urinary metabolic signatures from Western (United Kingdom) and South-East Asian (Thai) cholangiocarcinoma patients were characterized to understand spectral variability due to host carcinogenic processes and/or exogenous differences (nutritional, environmental and pharmaceutical). Urinary liquid chromatography mass spectroscopy (LC–MS) spectral profiles from Thai (healthy = 20 and cholangiocarcinoma = 14) and UK cohorts (healthy = 22 and cholangiocarcinoma = 10) were obtained and modelled using chemometric data analysis. Healthy metabolome disparities between the two distinct populations were primarily related to differences in dietary practices and body composition. Metabolites excreted due to drug treatment were dominant in urine specimens from cholangiocarcinoma patients, particularly in Western individuals. Urine from participants with sporadic (UK) cholangiocarcinoma contained greater levels of a nucleotide metabolite (uridine/pseudouridine). Higher relative concentrations of 7-methylguanine were observed in urine specimens from Thai cholangiocarcinoma patients. The urinary excretion of hippurate and methyladenine (gut microbial-host co-metabolites) showed a similar pattern of lower levels in patients with malignant biliary tumours from both countries. Intrinsic (body weight and body composition) and extrinsic (xenobiotic metabolism) factors were the main causes of disparities between the two populations. Regardless of the underlying aetiology, biological perturbations associated with cholangiocarcinoma urine metabolome signatures appeared to be influenced by gut microbial community metabolism. Dysregulation in nucleotide metabolism was associated with sporadic cholangiocarcinoma, possibly indicating differences in mitochondrial energy production pathways between cholangiocarcinoma tumour subtypes. Mapping population-specific metabolic disparities may aid in interpretation of disease processes and identification of candidate biomarkers. [ABSTRACT FROM AUTHOR]

Published

2021

2. Characterisation of the Serum Metabolic Signature of Cholangiocarcinoma in a United Kingdom Cohort.

Author

Alsaleh, Munirah, Leftley, Zoe, Barbera, Thomas A., Koomson, Larry K., Zabron, Abigail, Crossey, Mary M.E., Reeves, Helen L., Cramp, Matthew, Ryder, Stephen, Greer, Shaun, Prince, Martin, Sithithaworn, Paiboon, Shariff, Mohamed, Khuntikeo, Narong, Loilome, Watcharin, Yongvanit, Puangrat, Shen, Yi-Liang, Cox, I. Jane, Williams, Roger, and Wadsworth, Christopher A.

Subjects

*HYDROPHILIC interaction liquid chromatography, *SERUM, BILIARY tract cancer

Abstract

A distinct serum metabonomic pattern has been previously revealed to be associated with various forms of liver disease. Here, we aimed to apply mass spectrometry to obtain serum metabolomic profiles from individuals with cholangiocarcinoma and benign hepatobiliary diseases to gain an insight into pathogenesis and search for potential early-disease biomarkers. Serum samples were profiled using a hydrophilic interaction liquid chromatography platform, coupled to a mass spectrometer. A total of 47 serum specimens from 8 cholangiocarcinoma cases, 20 healthy controls, 8 benign disease controls (bile duct strictures) and 11 patients with hepatocellular carcinoma (as malignant disease controls) were included. Data analysis was performed using univariate and multivariate statistics. The serum metabolome disparities between the metabolite profiles from healthy controls and patients with hepatobiliary disease were predominantly related to changes in lipid and lipid-derived compounds (phospholipids, bile acids and steroids) and amino acid metabolites (phenylalanine). A metabolic pattern indicative of inflammatory response due to cirrhosis and cholestasis was associated with the disease groups. The abundance of phospholipid metabolites was altered in individuals with liver disease, particularly cholangiocarcinoma, but no significant difference was seen between profiles from patients with benign biliary strictures and cholangiocarcinoma. The serum metabolome in cholangiocarcinoma exhibited changes in metabolites related to inflammation, altered energy production and phospholipid metabolism. This study serves to highlight future avenues for biomarker research in large-scale studies. [ABSTRACT FROM AUTHOR]

Published

2020