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119 results on '"Tilford, Charles"'

1. Colocalization of GWAS and eQTL signals at loci with multiple signals identifies additional candidate genes for body fat distribution.

Author

Wu, Ying, Broadaway, K, Raulerson, Chelsea, Scott, Laura, Pan, Calvin, Ko, Arthur, He, Aiqing, Tilford, Charles, Fuchsberger, Christian, Locke, Adam, Stringham, Heather, Jackson, Anne, Narisu, Narisu, Kuusisto, Johanna, Pajukanta, Päivi, Collins, Francis, Boehnke, Michael, Laakso, Markku, Lusis, Aldons, Civelek, Mete, and Mohlke, Karen

Subjects
Adipose Tissue, Adult, Bayes Theorem, Body Fat Distribution, Body Mass Index, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Linkage Disequilibrium, Male, Metabolic Syndrome, Phenotype, Polymorphism, Single Nucleotide, Quantitative Trait Loci, Subcutaneous Fat, Waist-Hip Ratio
Abstract

Integration of genome-wide association study (GWAS) signals with expression quantitative trait loci (eQTL) studies enables identification of candidate genes. However, evaluating whether nearby signals may share causal variants, termed colocalization, is affected by the presence of allelic heterogeneity, different variants at the same locus impacting the same phenotype. We previously identified eQTL in subcutaneous adipose tissue from 770 participants in the Metabolic Syndrome in Men (METSIM) study and detected 15 eQTL signals that colocalized with GWAS signals for waist-hip ratio adjusted for body mass index (WHRadjBMI) from the Genetic Investigation of Anthropometric Traits consortium. Here, we reevaluated evidence of colocalization using two approaches, conditional analysis and the Bayesian test COLOC, and show that providing COLOC with approximate conditional summary statistics at multi-signal GWAS loci can reconcile disagreements in colocalization classification between the two tests. Next, we performed conditional analysis on the METSIM subcutaneous adipose tissue data to identify conditionally distinct or secondary eQTL signals. We used the two approaches to test for colocalization with WHRadjBMI GWAS signals and evaluated the differences in colocalization classification between the two tests. Through these analyses, we identified four GWAS signals colocalized with secondary eQTL signals for FAM13A, SSR3, GRB14 and FMO1. Thus, at loci with multiple eQTL and/or GWAS signals, analyzing each signal independently enabled additional candidate genes to be identified.

Published
2019

2. Genetic Regulation of Adipose Gene Expression and Cardio-Metabolic Traits

Author

Civelek, Mete, Wu, Ying, Pan, Calvin, Raulerson, Chelsea K, Ko, Arthur, He, Aiqing, Tilford, Charles, Saleem, Niyas K, Stančáková, Alena, Scott, Laura J, Fuchsberger, Christian, Stringham, Heather M, Jackson, Anne U, Narisu, Narisu, Chines, Peter S, Small, Kerrin S, Kuusisto, Johanna, Parks, Brian W, Pajukanta, Päivi, Kirchgessner, Todd, Collins, Francis S, Gargalovic, Peter S, Boehnke, Michael, Laakso, Markku, Mohlke, Karen L, and Lusis, Aldons J

Subjects
Prevention, Genetics, Human Genome, Biotechnology, Aetiology, 2.1 Biological and endogenous factors, Aged, Animals, Cardiovascular Diseases, Databases, Genetic, Gene Expression Profiling, Gene Expression Regulation, Genome-Wide Association Study, Genotyping Techniques, Humans, Male, Metabolic Syndrome, Mice, Middle Aged, Nuclear Proteins, Phenotype, Quantitative Trait Loci, Reproducibility of Results, Subcutaneous Fat, Trans-Activators, Biological Sciences, Medical and Health Sciences, Genetics & Heredity
Abstract

Subcutaneous adipose tissue stores excess lipids and maintains energy balance. We performed expression quantitative trait locus (eQTL) analyses by using abdominal subcutaneous adipose tissue of 770 extensively phenotyped participants of the METSIM study. We identified cis-eQTLs for 12,400 genes at a 1% false-discovery rate. Among an approximately 680 known genome-wide association study (GWAS) loci for cardio-metabolic traits, we identified 140 coincident cis-eQTLs at 109 GWAS loci, including 93 eQTLs not previously described. At 49 of these 140 eQTLs, gene expression was nominally associated (p < 0.05) with levels of the GWAS trait. The size of our dataset enabled identification of five loci associated (p < 5 × 10-8) with at least five genes located >5 Mb away. These trans-eQTL signals confirmed and extended the previously reported KLF14-mediated network to 55 target genes, validated the CIITA regulation of class II MHC genes, and identified ZNF800 as a candidate master regulator. Finally, we observed similar expression-clinical trait correlations of genes associated with GWAS loci in both humans and a panel of genetically diverse mice. These results provide candidate genes for further investigation of their potential roles in adipose biology and in regulating cardio-metabolic traits.

Published
2017

3. Comparative analysis of proteome and transcriptome variation in mouse.

Author

Ghazalpour, Anatole, Bennett, Brian, Petyuk, Vladislav A, Orozco, Luz, Hagopian, Raffi, Mungrue, Imran N, Farber, Charles R, Sinsheimer, Janet, Kang, Hyun M, Furlotte, Nicholas, Park, Christopher C, Wen, Ping-Zi, Brewer, Heather, Weitz, Karl, Camp, David G, Pan, Calvin, Yordanova, Roumyana, Neuhaus, Isaac, Tilford, Charles, Siemers, Nathan, Gargalovic, Peter, Eskin, Eleazar, Kirchgessner, Todd, Smith, Desmond J, Smith, Richard D, and Lusis, Aldons J

Subjects
Animals, Mice, Proteome, RNA, Messenger, Gene Expression Profiling, Proteomics, Alternative Splicing, Genetic Variation, Genome-Wide Association Study, Biotechnology, Genetics, Human Genome, Generic health relevance, Developmental Biology
Abstract

The relationships between the levels of transcripts and the levels of the proteins they encode have not been examined comprehensively in mammals, although previous work in plants and yeast suggest a surprisingly modest correlation. We have examined this issue using a genetic approach in which natural variations were used to perturb both transcript levels and protein levels among inbred strains of mice. We quantified over 5,000 peptides and over 22,000 transcripts in livers of 97 inbred and recombinant inbred strains and focused on the 7,185 most heritable transcripts and 486 most reliable proteins. The transcript levels were quantified by microarray analysis in three replicates and the proteins were quantified by Liquid Chromatography-Mass Spectrometry using O(18)-reference-based isotope labeling approach. We show that the levels of transcripts and proteins correlate significantly for only about half of the genes tested, with an average correlation of 0.27, and the correlations of transcripts and proteins varied depending on the cellular location and biological function of the gene. We examined technical and biological factors that could contribute to the modest correlation. For example, differential splicing clearly affects the analyses for certain genes; but, based on deep sequencing, this does not substantially contribute to the overall estimate of the correlation. We also employed genome-wide association analyses to map loci controlling both transcript and protein levels. Surprisingly, little overlap was observed between the protein- and transcript-mapped loci. We have typed numerous clinically relevant traits among the strains, including adiposity, lipoprotein levels, and tissue parameters. Using correlation analysis, we found that a low number of clinical trait relationships are preserved between the protein and mRNA gene products and that the majority of such relationships are specific to either the protein levels or transcript levels. Surprisingly, transcript levels were more strongly correlated with clinical traits than protein levels. In light of the widespread use of high-throughput technologies in both clinical and basic research, the results presented have practical as well as basic implications.

Published
2011

4. Supplementary Table S3 from Identification of a nonkinase target mediating cytotoxicity of novel kinase inhibitors

Author

Ross-Macdonald, Petra, primary, de Silva, Heshani, primary, Guo, Qi, primary, Xiao, Hong, primary, Hung, Chen-Yi, primary, Penhallow, Becky, primary, Markwalder, Jay, primary, He, Liqi, primary, Attar, Ricardo M., primary, Lin, Tai-an, primary, Seitz, Steven, primary, Tilford, Charles, primary, Wardwell-Swanson, Judith, primary, and Jackson, Donald, primary

Published
2023
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5. Supplementary Methods from Identification of a nonkinase target mediating cytotoxicity of novel kinase inhibitors

Author

Ross-Macdonald, Petra, primary, de Silva, Heshani, primary, Guo, Qi, primary, Xiao, Hong, primary, Hung, Chen-Yi, primary, Penhallow, Becky, primary, Markwalder, Jay, primary, He, Liqi, primary, Attar, Ricardo M., primary, Lin, Tai-an, primary, Seitz, Steven, primary, Tilford, Charles, primary, Wardwell-Swanson, Judith, primary, and Jackson, Donald, primary

Published
2023
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6. Biochemical and transcriptional profiling to triage additional activities in a series of IGF-1R/IR inhibitors

Author

Ross-Macdonald, Petra, de Silva, Heshani, Patel, Vishal, Truong, Amy, He, Aiqing, Neuhaus, Isaac, Tilford, Charles, Ji, RuiRu, Siemers, Nathan, Greer, Ann, Carboni, Joan, Gottardis, Marco, Menard, Krista, Lee, Frank, Dodier, Marco, Frennesson, David, Sampognaro, Anthony, Saulnier, Mark, Trainor, George, Vyas, Dolatrai, Zimmermann, Kurt, and Wittman, Mark

Published
2012
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10. A physical map of the human Y chromosome

Author

Tilford, Charles A., Kuroda-Kawaguchi, Tomoko, Skaletsky, Helen, Rozen, Steve, Brown, Laura G., Rosenberg, Michael, McPherson, John D., Wylie, Kristine, Sekhon, Mandeep, Kucaba, Tamara A., Waterston, Robert H., and Page, David C.

Published
2001
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11. Partial pressure analysis in space testing

Author

Tilford, Charles R

Subjects
Instrumentation And Photography
Abstract

For vacuum-system or test-article analysis it is often desirable to know the species and partial pressures of the vacuum gases. Residual gas or Partial Pressure Analyzers (PPA's) are commonly used for this purpose. These are mass spectrometer-type instruments, most commonly employing quadrupole filters. These instruments can be extremely useful, but they should be used with caution. Depending on the instrument design, calibration procedures, and conditions of use, measurements made with these instruments can be accurate to within a few percent, or in error by two or more orders of magnitude. Significant sources of error can include relative gas sensitivities that differ from handbook values by an order of magnitude, changes in sensitivity with pressure by as much as two orders of magnitude, changes in sensitivity with time after exposure to chemically active gases, and the dependence of the sensitivity for one gas on the pressures of other gases. However, for most instruments, these errors can be greatly reduced with proper operating procedures and conditions of use. In this paper, data are presented illustrating performance characteristics for different instruments and gases, operating parameters are recommended to minimize some errors, and calibrations procedures are described that can detect and/or correct other errors.

Published
1994

17. Identification of a nonkinase target mediating cytotoxicity of novel kinase inhibitors

Author

Ross-Macdonald, Petra, primary, de Silva, Heshani, additional, Guo, Qi, additional, Xiao, Hong, additional, Hung, Chen-Yi, additional, Penhallow, Becky, additional, Markwalder, Jay, additional, He, Liqi, additional, Attar, Ricardo M., additional, Lin, Tai-an, additional, Seitz, Steven, additional, Tilford, Charles, additional, Wardwell-Swanson, Judith, additional, and Jackson, Donald, additional

Published
2008
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24. Expression Profile of Drug and Nutrient Absorption Related Genes in Madin-Darby Canine Kidney (MDCK) Cells Grown under Differentiation Conditions.

Author

Yong Quan, Yisheng Jin, Faria, Teresa N., Tilford, Charles A., Aiqing He, Wall, Doris A., Smith, Ronald L., and Vig, Balvinder S.

Subjects
GENE expression, GENETIC regulation, HEREDITY, CATALYSTS, GENES, KIDNEY cell culture, ENZYMOLOGY
Abstract

The expression levels of genes involved in drug and nutrient absorption were evaluated in the Madin-Darby Canine Kidney (MDCK) in vitro drug absorption model. MDCK cells were grown on plastic surfaces (for 3 days) or on Transwell® membranes (for 3, 5, 7, and 9 days). The expression profile of genes including ABC transporters, SLC transporters, and cytochrome P450 (CYP) enzymes was determined using the Affymetrix® Canine GeneChip®. Expression of genes whose probe sets passed a stringent confirmation process was examined. Expression of a few transporter (MDR1, PEPT1 and PEPT2) genes in MDCK cells was confirmed by RT-PCR. The overall gene expression profile was strongly influenced by the type of support the cells were grown on. After 3 days of growth, expression of 28% of the genes was statistically different (1.5-fold cutoff, p < 0.05) between the cells grown on plastic and Transwell® membranes. When cells were differentiated on Transwell® membranes, large changes in gene expression profile were observed during the early stages, which then stabilized after 5--7 days. Only a small number of genes encoding drug absorption related SLC, ABC, and CYP were detected in MDCK cells, and most of them exhibited low hybridization signals. Results from this study provide valuable reference information on endogenous gene expression in MDCK cells that could assist in design of drug-transporter and/or drug-enzyme interaction studies, and help interpret the contributions of various transporters and metabolic enzymes in studies with MDCK cells. [ABSTRACT FROM AUTHOR]

Published
2012
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35. Analytical procedure for determining lengths from fractional fringes

Author

Tilford, Charles R.

Abstract

The development of stabilized multifrequency lasers makes fractional fringes an increasingly attractive technique for length measurement. Determination of an unknown length from the measured fractional fringes is aided by the development of analytical equations for the length and its uncertainty, and criteria are given for selecting the wavelengths.

Published
1977

36. CRISPR-DAV: CRISPR NGS data analysis and visualization pipeline.

Author

Xuning Wang, Tilford, Charles, Neuhaus, Isaac, Mintier, Gabe, Qi Guo, Feder, John N., and Kirov, Stefan

Subjects
*CRISPRS, *NUCLEOTIDE sequencing, *DNA repair, *OLIGONUCLEOTIDES, *GENE targeting
Abstract

The simplicity and precision of CRISPR/Cas9 system has brought in a new era of gene editing. Screening for desired clones with CRISPR-mediated genomic edits in a large number of samples is made possible by next generation sequencing (NGS) due to its multiplexing. Here we present CRISPR-DAV (CRISPR Data Analysis and Visualization) pipeline to analyze the CRISPR NGS data in a high throughput manner. In the pipeline, Burrows-Wheeler Aligner and Assembly Based ReAlignment are used for small and large indel detection, and results are presented in a comprehensive set of charts and interactive alignment view. [ABSTRACT FROM AUTHOR]

Published
2017
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