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Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons

Lower muscle strength in midlife predicts disability and mortality in later life. Blood-borne factors, including growth differentiation factor 11 (GDF11), have been linked to muscle regeneration in animal models. We aimed to identify gene transcripts associated with muscle strength in adults. Meta-a...

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Autores principales: Pilling, L. C., Joehanes, R., Kacprowski, T., Peters, M., Jansen, R., Karasik, D., Kiel, D. P., Harries, L. W., Teumer, A., Powell, J., Levy, D., Lin, H., Lunetta, K., Munson, P., Bandinelli, S., Henley, W., Hernandez, D., Singleton, A., Tanaka, T., van Grootheest, G., Hofman, A., Uitterlinden, A. G., Biffar, R., Gläser, S., Homuth, G., Malsch, C., Völker, U., Penninx, B., van Meurs, J. B. J., Ferrucci, L., Kocher, T., Murabito, J., Melzer, D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Physiological Society 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4757025/
https://www.ncbi.nlm.nih.gov/pubmed/26487704
http://dx.doi.org/10.1152/physiolgenomics.00054.2015
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author Pilling, L. C.
Joehanes, R.
Kacprowski, T.
Peters, M.
Jansen, R.
Karasik, D.
Kiel, D. P.
Harries, L. W.
Teumer, A.
Powell, J.
Levy, D.
Lin, H.
Lunetta, K.
Munson, P.
Bandinelli, S.
Henley, W.
Hernandez, D.
Singleton, A.
Tanaka, T.
van Grootheest, G.
Hofman, A.
Uitterlinden, A. G.
Biffar, R.
Gläser, S.
Homuth, G.
Malsch, C.
Völker, U.
Penninx, B.
van Meurs, J. B. J.
Ferrucci, L.
Kocher, T.
Murabito, J.
Melzer, D.
author_facet Pilling, L. C.
Joehanes, R.
Kacprowski, T.
Peters, M.
Jansen, R.
Karasik, D.
Kiel, D. P.
Harries, L. W.
Teumer, A.
Powell, J.
Levy, D.
Lin, H.
Lunetta, K.
Munson, P.
Bandinelli, S.
Henley, W.
Hernandez, D.
Singleton, A.
Tanaka, T.
van Grootheest, G.
Hofman, A.
Uitterlinden, A. G.
Biffar, R.
Gläser, S.
Homuth, G.
Malsch, C.
Völker, U.
Penninx, B.
van Meurs, J. B. J.
Ferrucci, L.
Kocher, T.
Murabito, J.
Melzer, D.
author_sort Pilling, L. C.
collection PubMed
description Lower muscle strength in midlife predicts disability and mortality in later life. Blood-borne factors, including growth differentiation factor 11 (GDF11), have been linked to muscle regeneration in animal models. We aimed to identify gene transcripts associated with muscle strength in adults. Meta-analysis of whole blood gene expression (overall 17,534 unique genes measured by microarray) and hand-grip strength in four independent cohorts (n = 7,781, ages: 20–104 yr, weighted mean = 56), adjusted for age, sex, height, weight, and leukocyte subtypes. Separate analyses were performed in subsets (older/younger than 60, men/women). Expression levels of 221 genes were associated with strength after adjustment for cofactors and for multiple statistical testing, including ALAS2 (rate-limiting enzyme in heme synthesis), PRF1 (perforin, a cytotoxic protein associated with inflammation), IGF1R, and IGF2BP2 (both insulin like growth factor related). We identified statistical enrichment for hemoglobin biosynthesis, innate immune activation, and the stress response. Ten genes were associated only in younger individuals, four in men only and one in women only. For example, PIK3R2 (a negative regulator of PI3K/AKT growth pathway) was negatively associated with muscle strength in younger (<60 yr) individuals but not older (≥60 yr). We also show that 115 genes (52%) have not previously been linked to muscle in NCBI PubMed abstracts. This first large-scale transcriptome study of muscle strength in human adults confirmed associations with known pathways and provides new evidence for over half of the genes identified. There may be age- and sex-specific gene expression signatures in blood for muscle strength.
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spelling pubmed-47570252016-03-10 Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons Pilling, L. C. Joehanes, R. Kacprowski, T. Peters, M. Jansen, R. Karasik, D. Kiel, D. P. Harries, L. W. Teumer, A. Powell, J. Levy, D. Lin, H. Lunetta, K. Munson, P. Bandinelli, S. Henley, W. Hernandez, D. Singleton, A. Tanaka, T. van Grootheest, G. Hofman, A. Uitterlinden, A. G. Biffar, R. Gläser, S. Homuth, G. Malsch, C. Völker, U. Penninx, B. van Meurs, J. B. J. Ferrucci, L. Kocher, T. Murabito, J. Melzer, D. Physiol Genomics Omics Technologies and Applications Lower muscle strength in midlife predicts disability and mortality in later life. Blood-borne factors, including growth differentiation factor 11 (GDF11), have been linked to muscle regeneration in animal models. We aimed to identify gene transcripts associated with muscle strength in adults. Meta-analysis of whole blood gene expression (overall 17,534 unique genes measured by microarray) and hand-grip strength in four independent cohorts (n = 7,781, ages: 20–104 yr, weighted mean = 56), adjusted for age, sex, height, weight, and leukocyte subtypes. Separate analyses were performed in subsets (older/younger than 60, men/women). Expression levels of 221 genes were associated with strength after adjustment for cofactors and for multiple statistical testing, including ALAS2 (rate-limiting enzyme in heme synthesis), PRF1 (perforin, a cytotoxic protein associated with inflammation), IGF1R, and IGF2BP2 (both insulin like growth factor related). We identified statistical enrichment for hemoglobin biosynthesis, innate immune activation, and the stress response. Ten genes were associated only in younger individuals, four in men only and one in women only. For example, PIK3R2 (a negative regulator of PI3K/AKT growth pathway) was negatively associated with muscle strength in younger (<60 yr) individuals but not older (≥60 yr). We also show that 115 genes (52%) have not previously been linked to muscle in NCBI PubMed abstracts. This first large-scale transcriptome study of muscle strength in human adults confirmed associations with known pathways and provides new evidence for over half of the genes identified. There may be age- and sex-specific gene expression signatures in blood for muscle strength. American Physiological Society 2015-10-20 2016-01 /pmc/articles/PMC4757025/ /pubmed/26487704 http://dx.doi.org/10.1152/physiolgenomics.00054.2015 Text en Copyright © 2016 the American Physiological Society http://creativecommons.org/licenses/by/3.0/deed.en_US Licensed under Creative Commons Attribution CC-BY 3.0 (http://creativecommons.org/licenses/by/3.0/deed.en_US) : © the American Physiological Society.
spellingShingle Omics Technologies and Applications
Pilling, L. C.
Joehanes, R.
Kacprowski, T.
Peters, M.
Jansen, R.
Karasik, D.
Kiel, D. P.
Harries, L. W.
Teumer, A.
Powell, J.
Levy, D.
Lin, H.
Lunetta, K.
Munson, P.
Bandinelli, S.
Henley, W.
Hernandez, D.
Singleton, A.
Tanaka, T.
van Grootheest, G.
Hofman, A.
Uitterlinden, A. G.
Biffar, R.
Gläser, S.
Homuth, G.
Malsch, C.
Völker, U.
Penninx, B.
van Meurs, J. B. J.
Ferrucci, L.
Kocher, T.
Murabito, J.
Melzer, D.
Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons
title Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons
title_full Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons
title_fullStr Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons
title_full_unstemmed Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons
title_short Gene transcripts associated with muscle strength: a CHARGE meta-analysis of 7,781 persons
title_sort gene transcripts associated with muscle strength: a charge meta-analysis of 7,781 persons
topic Omics Technologies and Applications
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4757025/
https://www.ncbi.nlm.nih.gov/pubmed/26487704
http://dx.doi.org/10.1152/physiolgenomics.00054.2015
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