Your search keyword '"Mosley, Thomas"' showing total 3 results

1. METRO: Multi-ancestry transcriptome-wide association studies for powerful gene-trait association detection.

Author

Li, Zheng, Zhao, Wei, Shang, Lulu, Mosley, Thomas H., Kardia, Sharon L.R., Smith, Jennifer A., and Zhou, Xiang

Subjects

*GENETIC epidemiology, *GENOME-wide association studies, *MICROTUBULES, *MICROTUBULE-associated proteins, *TAU proteins, *GENE expression

Abstract

Integrative analysis of genome-wide association studies (GWASs) and gene expression studies in the form of a transcriptome-wide association study (TWAS) has the potential to better elucidate the molecular mechanisms underlying disease etiology. Here we present a method, METRO, that can leverage gene expression data collected from multiple genetic ancestries to enhance TWASs. METRO incorporates expression prediction models constructed in different genetic ancestries through a likelihood-based inference framework, producing calibrated p values with substantially improved TWAS power. We illustrate the benefits of METRO in both simulations and applications to seven complex traits and diseases obtained from four GWASs. These GWASs include two of primarily European ancestry (n = 188,577 and 339,226) and two of primarily African ancestry (n = 42,752 and 23,827). In the real data applications, we leverage gene expression data measured on 1,032 African Americans and 801 European Americans from the Genetic Epidemiology Network of Arteriopathy (GENOA) study to identify a substantially larger number of gene-trait associations as compared to existing TWAS approaches. The benefits of METRO are most prominent in applications to GWASs of African ancestry where the sample size is much smaller than GWASs of European ancestry and where a more powerful TWAS method is crucial. Among the identified associations are high-density lipoprotein-associated genes including PLTP and PPARG that are critical for maintaining lipid homeostasis and the type II diabetes-associated gene MAPT that supports microtubule-associated protein tau as a key component underlying impaired insulin secretion. [ABSTRACT FROM AUTHOR]

Published

2022

2. Genetic Architecture of Gene Expression in European and African Americans: An eQTL Mapping Study in GENOA.

Author

Shang, Lulu, Smith, Jennifer A., Zhao, Wei, Kho, Minjung, Turner, Stephen T., Mosley, Thomas H., Kardia, Sharon L.R., and Zhou, Xiang

Subjects

*AFRICAN Americans, *GENE expression, *LYMPHOBLASTOID cell lines, *GENETIC regulation, *BIRTH size

Abstract

Most existing expression quantitative trait locus (eQTL) mapping studies have been focused on individuals of European ancestry and are underrepresented in other populations including populations with African ancestry. Lack of large-scale well-powered eQTL mapping studies in populations with African ancestry can both impede the dissemination of eQTL mapping results that would otherwise benefit individuals with African ancestry and hinder the comparable analysis for understanding how gene regulation is shaped through evolution. We fill this critical knowledge gap by performing a large-scale in-depth eQTL mapping study on 1,032 African Americans (AA) and 801 European Americans (EA) in the GENOA cohort. We identified a total of 354,931 eSNPs in AA and 371,309 eSNPs in EA, with 112,316 eSNPs overlapped between the two. We found that eQTL harboring genes (eGenes) are enriched in metabolic pathways and tend to have higher SNP heritability compared to non-eGenes. We found that eGenes that are common in the two populations tend to be less conserved than eGenes that are unique to one population, which are less conserved than non-eGenes. Through conditional analysis, we found that eGenes in AA tend to harbor more independent eQTLs than eGenes in EA, suggesting potentially diverse genetic architecture underlying expression variation in the two populations. Finally, the large sample sizes in GENOA allow us to construct accurate expression prediction models in both AA and EA, facilitating powerful transcriptome-wide association studies. Overall, our results represent an important step toward revealing the genetic architecture underlying expression variation in African Americans. [ABSTRACT FROM AUTHOR]

Published

2020

3. Effects of Subclinical Disease on Cognitive Function across Age in African Americans.

Author

Bridges, John M., Griswold, Michael E., Simpson, Brittany N., Peyser, Patricia A., Bielak, Lawrence F., Turner, Stephen T., Lirette, Seth T., Mosley, Thomas H., and Windham, B. Gwen

Subjects

*COGNITIVE ability, *AFRICAN Americans, *INCIDENTAL learning, *MINI-Mental State Examination, *TRAIL Making Test, *CALCIFICATION, *CORONARY arteries

Abstract

Objectives: Determine relationships between calcification and cognitive function. Background: Dementia affects over 5.4 million Americans; prevalence will quadruple in the next 50 years. Coronary artery calcification (CAC), a measure of subclinical atherosclerosis, may affect cognitive function through microvascular brain effects. Abdominal aortoiliac calcification (AAC) generally precedes CAC and may provide earlier risk determination. Effects of calcification on cognition have not been studied in African Americans (AA). Methods: The 2008-2011 GENOA CAC cohort consists of AA sibships (n=657, mean age 69 [range 40-98], 74% women, 82% hypertensive) enriched with hypertension from Jackson, MS with computed tomography (CT) Agatston calcification measures. Cognition was assessed in 4 domains: global cognitive function (Mini-Mental State Examination); processing speed (Digit Symbol Substitution and Trail Making A); memory (RAVLT and WAIS-III Incidental Learning); and executive function (Trail Making B). Relationships of cognition (standardized) and calcification (log base 2 scale accounting for skewness) were examined using linear regressions with GEE to account for sibship clustering, adjusting parsimoniously for age, sex, and education. Results: Doublings of CAC were significantly associated with poorer processing speed (β=-0.049 [-0.072, -0.025] p=0.000) and executive function (β=-0.037 [-0.070, -0.003] p=0.031) in younger subjects and with poorer global function (β=-0.0648 [-0.096, -0.020] p=0.000), memory (β=-0.034 [-0.060, -0.007] p=0.013), and processing speed (β=-0.051 [-0.076, -0.025] p=0.000) in older subjects. Doublings of AAC were significantly associated with poorer processing speed (β=-0.0381 [-0.056, -0.020] p=0.000) and executive function (β=-0.045 [-0.070, -0.020] p=0.000) in younger subjects and poorer processing speed (β=-0.050 [-0.075, -0.025] p=0.000) in older subjects. Conclusions: Calcification is associated with processing speed in young and old AA with prevalent cardiovascular risk factors and may be differentially associated with other cognitive domains by age. Processing speed in particular may be a domain affected early in the calcification process, warranting further study. This supports existing literature addressing the relationship between calcification and cognitive function in ethnically diverse cohorts. Further studies can focus on the temporal and causal relationships between calcification and cognition across age in AA samples enriched for hypertension to identify predictive factors associated with future cognitive decline. [ABSTRACT FROM AUTHOR]

Published

2014