Your search keyword '"Lau, C-HE"' showing total 4 results

1. Associations of four biological age markers with child development: a multi-omic analysis in the European HELIX cohort

Author

Robinson, O, Lau, C-HE, Joo, S, Andrusaityte, S, Borras, E, De Prado-Bert, P, Chatzi, L, Keun, HC, and Grazuleviciene, R

Abstract

Background: While biological age in adults is often understood as representing general health and resilience, the conceptual interpretation of accelerated biological age in children and its relationship to development remains unclear. We aimed to clarify the relationship of accelerated biological age, assessed through two established biological age indicators, telomere length and DNA methylation age, and two novel candidate biological age indicators , to child developmental outcomes, including growth and adiposity, cognition, behaviour, lung function and onset of puberty, among European school-age children participating in the HELIX exposome cohort. Methods: The study population included up to 1,173 children, aged between 5 and 12 years, from study centres in the UK, France, Spain, Norway, Lithuania, and Greece. Telomere length was measured through qPCR, blood DNA methylation and gene expression was measured using microarray, and proteins and metabolites were measured by a range of targeted assays. DNA methylation age was assessed using Horvath's skin and blood clock, while novel blood transcriptome and 'immunometabolic' (based on plasma protein and urinary and serum metabolite data) clocks were derived and tested in a subset of children assessed six months after the main follow-up visit. Associations between biological age indicators with child developmental measures as well as health risk factors were estimated using linear regression, adjusted for chronological age, sex, ethnicity and study centre. The clock derived markers were expressed as Δ age (i.e., predicted minus chronological age). Results: Transcriptome and immunometabolic clocks predicted chronological age well in the test set (r= 0.93 and r= 0.84 respectively). Generally, weak correlations were observed, after adjustment for chronological age, between the biological age indicators. Among associations with health risk factors, higher birthweight was associated with greater immunometabolic Δ age, smoke exposure with greater DNA methylation Δ age and high family affluence with longer telomere length. Among associations with child developmental measures, all biological age markers were associated with greater BMI and fat mass, and all markers except telomere length were associated with greater height, at least at nominal significance (p

Published

2023

2. Systematic integration of molecular profiles identifies miR-22 as a regulator of lipid and folate metabolism in breast cancer cells

Author

Koufaris, C, Valbuena, G N, Pomyen, Y, Tredwell, G D, Nevedomskaya, E, Lau, C-HE, Yang, T, Benito, A, Ellis, J K, and Keun, H C

Published

2016

3. Assessment of metabolic phenotypic variability in children's urine using H-1 NMR spectroscopy

Author

Maitre, L, Lau, C-HE, Vizcaino, E, Robinson, O, Casas, M, Siskos, AP, Want, EJ, Athersuch, T, Slama, R, Vrijheid, M, Keun, HC, Coen, M, and Commission of the European Communities

Subjects

Multidisciplinary Sciences, Science & Technology, STRESS, PLASMA, CARDIOVASCULAR-DISEASE, BIOMARKERS, Science & Technology - Other Topics, POPULATIONS, SPECTRA, CONSUMPTION, PROFILES, ASSOCIATION, RHYTHMS

Abstract

The application of metabolic phenotyping in clinical and epidemiological studies is limited by a poor understanding of inter-individual, intra-individual and temporal variability in metabolic phenotypes. Using 1H NMR spectroscopy we characterised short-term variability in urinary metabolites measured from 20 children aged 8–9 years old. Daily spot morning, night-time and pooled (50:50 morning and night-time) urine samples across six days (18 samples per child) were analysed, and 44 metabolites quantified. Intraclass correlation coefficients (ICC) and mixed effect models were applied to assess the reproducibility and biological variance of metabolic phenotypes. Excellent analytical reproducibility and precision was demonstrated for the 1H NMR spectroscopic platform (median CV 7.2%). Pooled samples captured the best inter-individual variability with an ICC of 0.40 (median). Trimethylamine, N-acetyl neuraminic acid, 3-hydroxyisobutyrate, 3-hydroxybutyrate/3-aminoisobutyrate, tyrosine, valine and 3-hydroxyisovalerate exhibited the highest stability with over 50% of variance specific to the child. The pooled sample was shown to capture the most inter-individual variance in the metabolic phenotype, which is of importance for molecular epidemiology study design. A substantial proportion of the variation in the urinary metabolome of children is specific to the individual, underlining the potential of such data to inform clinical and exposome studies conducted early in life.

Published

2017

4. Systematic integration of molecular profiles identifies miR-22 as a regulator of lipid and folate metabolism in breast cancer cells

Author

Koufaris, C, primary, Valbuena, G N, additional, Pomyen, Y, additional, Tredwell, G D, additional, Nevedomskaya, E, additional, Lau, C-HE, additional, Yang, T, additional, Benito, A, additional, Ellis, J K, additional, and Keun, H C, additional

Published

2015