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Genetic architecture of heart mitochondrial proteome influencing cardiac hypertrophy
by
Keller, Mark P
, Seldin, Marcus M
, Rosenthal, Nadia A
, Attie, Alan D
, Kaczor-Urbanowicz, Karolina Elżbieta
, James, David E
, Carroll, Luke
, Vegas, Alexis Diaz
, Lee, Chi Fung
, Churchill, Gary A
, Lusis, Aldons J
, Shravah, Varun
, Parker, Benjamin
, Gerdes Gyuricza, Isabela
, Pan, Calvin
, Anum, Diana
, Cao, Yang
, Light, Christine
, Chella Krishnan, Karthickeyan
, Patel, Sanjeet G
, El Hachem, Elie-Julien
, Pellegrini, Matteo
in
Analysis
/ Animals
/ Apoptosis
/ Cardiomegaly - genetics
/ Computational and Systems Biology
/ Congestive heart failure
/ COQ7 gene
/ Development and progression
/ Disease
/ Disease susceptibility
/ DNA, Mitochondrial - metabolism
/ Electron Transport Complex I - metabolism
/ Gene loci
/ Gene mapping
/ Gene regulation
/ Genes
/ Genetic analysis
/ Genetic diversity
/ Genetic research
/ genetic, association studies
/ Genetics
/ Genetics and Genomics
/ Genomes
/ Genotype & phenotype
/ Heart
/ Heart diseases
/ Heart enlargement
/ Heart failure
/ Heart Failure - genetics
/ Heart Failure - metabolism
/ Hypertrophy
/ Inbreeding
/ Mediation
/ Metabolic syndrome
/ Mice
/ Mice, Inbred Strains
/ mitochondria
/ Mitochondria - metabolism
/ Mitochondrial DNA
/ Mitochondrial Proteins - genetics
/ Mitochondrial Proteins - metabolism
/ Pathophysiology
/ Peptide mapping
/ Proteins
/ Proteome - metabolism
/ Proteomes
/ Proteomics
/ Sexes
/ Statistical analysis
2023
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Genetic architecture of heart mitochondrial proteome influencing cardiac hypertrophy
by
Keller, Mark P
, Seldin, Marcus M
, Rosenthal, Nadia A
, Attie, Alan D
, Kaczor-Urbanowicz, Karolina Elżbieta
, James, David E
, Carroll, Luke
, Vegas, Alexis Diaz
, Lee, Chi Fung
, Churchill, Gary A
, Lusis, Aldons J
, Shravah, Varun
, Parker, Benjamin
, Gerdes Gyuricza, Isabela
, Pan, Calvin
, Anum, Diana
, Cao, Yang
, Light, Christine
, Chella Krishnan, Karthickeyan
, Patel, Sanjeet G
, El Hachem, Elie-Julien
, Pellegrini, Matteo
in
Analysis
/ Animals
/ Apoptosis
/ Cardiomegaly - genetics
/ Computational and Systems Biology
/ Congestive heart failure
/ COQ7 gene
/ Development and progression
/ Disease
/ Disease susceptibility
/ DNA, Mitochondrial - metabolism
/ Electron Transport Complex I - metabolism
/ Gene loci
/ Gene mapping
/ Gene regulation
/ Genes
/ Genetic analysis
/ Genetic diversity
/ Genetic research
/ genetic, association studies
/ Genetics
/ Genetics and Genomics
/ Genomes
/ Genotype & phenotype
/ Heart
/ Heart diseases
/ Heart enlargement
/ Heart failure
/ Heart Failure - genetics
/ Heart Failure - metabolism
/ Hypertrophy
/ Inbreeding
/ Mediation
/ Metabolic syndrome
/ Mice
/ Mice, Inbred Strains
/ mitochondria
/ Mitochondria - metabolism
/ Mitochondrial DNA
/ Mitochondrial Proteins - genetics
/ Mitochondrial Proteins - metabolism
/ Pathophysiology
/ Peptide mapping
/ Proteins
/ Proteome - metabolism
/ Proteomes
/ Proteomics
/ Sexes
/ Statistical analysis
2023
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Genetic architecture of heart mitochondrial proteome influencing cardiac hypertrophy
by
Keller, Mark P
, Seldin, Marcus M
, Rosenthal, Nadia A
, Attie, Alan D
, Kaczor-Urbanowicz, Karolina Elżbieta
, James, David E
, Carroll, Luke
, Vegas, Alexis Diaz
, Lee, Chi Fung
, Churchill, Gary A
, Lusis, Aldons J
, Shravah, Varun
, Parker, Benjamin
, Gerdes Gyuricza, Isabela
, Pan, Calvin
, Anum, Diana
, Cao, Yang
, Light, Christine
, Chella Krishnan, Karthickeyan
, Patel, Sanjeet G
, El Hachem, Elie-Julien
, Pellegrini, Matteo
in
Analysis
/ Animals
/ Apoptosis
/ Cardiomegaly - genetics
/ Computational and Systems Biology
/ Congestive heart failure
/ COQ7 gene
/ Development and progression
/ Disease
/ Disease susceptibility
/ DNA, Mitochondrial - metabolism
/ Electron Transport Complex I - metabolism
/ Gene loci
/ Gene mapping
/ Gene regulation
/ Genes
/ Genetic analysis
/ Genetic diversity
/ Genetic research
/ genetic, association studies
/ Genetics
/ Genetics and Genomics
/ Genomes
/ Genotype & phenotype
/ Heart
/ Heart diseases
/ Heart enlargement
/ Heart failure
/ Heart Failure - genetics
/ Heart Failure - metabolism
/ Hypertrophy
/ Inbreeding
/ Mediation
/ Metabolic syndrome
/ Mice
/ Mice, Inbred Strains
/ mitochondria
/ Mitochondria - metabolism
/ Mitochondrial DNA
/ Mitochondrial Proteins - genetics
/ Mitochondrial Proteins - metabolism
/ Pathophysiology
/ Peptide mapping
/ Proteins
/ Proteome - metabolism
/ Proteomes
/ Proteomics
/ Sexes
/ Statistical analysis
2023
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Genetic architecture of heart mitochondrial proteome influencing cardiac hypertrophy
Journal Article
Genetic architecture of heart mitochondrial proteome influencing cardiac hypertrophy
2023
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Overview
Mitochondria play an important role in both normal heart function and disease etiology. We report analysis of common genetic variations contributing to mitochondrial and heart functions using an integrative proteomics approach in a panel of inbred mouse strains called the Hybrid Mouse Diversity Panel (HMDP). We performed a whole heart proteome study in the HMDP (72 strains, n=2-3 mice) and retrieved 848 mitochondrial proteins (quantified in ≥50 strains). High-resolution association mapping on their relative abundance levels revealed three trans -acting genetic loci on chromosomes (chr) 7, 13 and 17 that regulate distinct classes of mitochondrial proteins as well as cardiac hypertrophy. DAVID enrichment analyses of genes regulated by each of the loci revealed that the chr13 locus was highly enriched for complex-I proteins (24 proteins, P =2.2E-61), the chr17 locus for mitochondrial ribonucleoprotein complex (17 proteins, P =3.1E-25) and the chr7 locus for ubiquinone biosynthesis (3 proteins, P =6.9E-05). Follow-up high resolution regional mapping identified NDUFS4, LRPPRC and COQ7 as the candidate genes for chr13, chr17 and chr7 loci, respectively, and both experimental and statistical analyses supported their causal roles. Furthermore, a large cohort of Diversity Outbred mice was used to corroborate Lrpprc gene as a driver of mitochondrial DNA (mtDNA)-encoded gene regulation, and to show that the chr17 locus is specific to heart. Variations in all three loci were associated with heart mass in at least one of two independent heart stress models, namely, isoproterenol-induced heart failure and diet-induced obesity. These findings suggest that common variations in certain mitochondrial proteins can act in trans to influence tissue-specific mitochondrial functions and contribute to heart hypertrophy, elucidating mechanisms that may underlie genetic susceptibility to heart failure in human populations.
Publisher
eLife Science Publications, Ltd,eLife Sciences Publications Ltd,eLife Sciences Publications, Ltd
Subject
/ Animals
/ Computational and Systems Biology
/ Disease
/ DNA, Mitochondrial - metabolism
/ Electron Transport Complex I - metabolism
/ Genes
/ genetic, association studies
/ Genetics
/ Genomes
/ Heart
/ Mice
/ Mitochondrial Proteins - genetics
/ Mitochondrial Proteins - metabolism
/ Proteins
/ Sexes
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