Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood

Many common chronic diseases of aging are negatively associated with socioeconomic status (SES). This study examines whether inequalities can already be observed in the molecular underpinnings of such diseases in the 30s, before many of them become prevalent. Data come from the National Longitudinal...

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Autores principales: Shanahan, Michael J., Cole, Steven W., Ravi, Sudharshan, Chumbley, Justin, Xu, Wenjia, Potente, Cecilia, Levitt, Brandt, Bodelet, Julien, Aiello, Allison, Gaydosh, Lauren, Harris, Kathleen Mullan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: National Academy of Sciences 2022
Materias:
Social Sciences
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9621370/
https://www.ncbi.nlm.nih.gov/pubmed/36252037
http://dx.doi.org/10.1073/pnas.2103088119
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author Shanahan, Michael J.
Cole, Steven W.
Ravi, Sudharshan
Chumbley, Justin
Xu, Wenjia
Potente, Cecilia
Levitt, Brandt
Bodelet, Julien
Aiello, Allison
Gaydosh, Lauren
Harris, Kathleen Mullan
author_facet Shanahan, Michael J.
Cole, Steven W.
Ravi, Sudharshan
Chumbley, Justin
Xu, Wenjia
Potente, Cecilia
Levitt, Brandt
Bodelet, Julien
Aiello, Allison
Gaydosh, Lauren
Harris, Kathleen Mullan
author_sort Shanahan, Michael J.
collection PubMed
description Many common chronic diseases of aging are negatively associated with socioeconomic status (SES). This study examines whether inequalities can already be observed in the molecular underpinnings of such diseases in the 30s, before many of them become prevalent. Data come from the National Longitudinal Study of Adolescent to Adult Health (Add Health), a large, nationally representative sample of US subjects who were followed for over two decades beginning in adolescence. We now have transcriptomic data (mRNA-seq) from a random subset of 4,543 of these young adults. SES in the household-of-origin and in young adulthood were examined as covariates of a priori-defined mRNA-based disease signatures and of specific gene transcripts identified de novo. An SES composite from young adulthood predicted many disease signatures, as did income and subjective status. Analyses highlighted SES-based inequalities in immune, inflammatory, ribosomal, and metabolic pathways, several of which play central roles in senescence. Many genes are also involved in transcription, translation, and diverse signaling mechanisms. Average causal-mediated effect models suggest that body mass index plays a key role in accounting for these relationships. Overall, the results reveal inequalities in molecular risk factors for chronic diseases often decades before diagnoses and suggest future directions for social signal transduction models that trace how social circumstances regulate the human genome.
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spelling pubmed-96213702022-11-01 Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood Shanahan, Michael J. Cole, Steven W. Ravi, Sudharshan Chumbley, Justin Xu, Wenjia Potente, Cecilia Levitt, Brandt Bodelet, Julien Aiello, Allison Gaydosh, Lauren Harris, Kathleen Mullan Proc Natl Acad Sci U S A Social Sciences Many common chronic diseases of aging are negatively associated with socioeconomic status (SES). This study examines whether inequalities can already be observed in the molecular underpinnings of such diseases in the 30s, before many of them become prevalent. Data come from the National Longitudinal Study of Adolescent to Adult Health (Add Health), a large, nationally representative sample of US subjects who were followed for over two decades beginning in adolescence. We now have transcriptomic data (mRNA-seq) from a random subset of 4,543 of these young adults. SES in the household-of-origin and in young adulthood were examined as covariates of a priori-defined mRNA-based disease signatures and of specific gene transcripts identified de novo. An SES composite from young adulthood predicted many disease signatures, as did income and subjective status. Analyses highlighted SES-based inequalities in immune, inflammatory, ribosomal, and metabolic pathways, several of which play central roles in senescence. Many genes are also involved in transcription, translation, and diverse signaling mechanisms. Average causal-mediated effect models suggest that body mass index plays a key role in accounting for these relationships. Overall, the results reveal inequalities in molecular risk factors for chronic diseases often decades before diagnoses and suggest future directions for social signal transduction models that trace how social circumstances regulate the human genome. National Academy of Sciences 2022-10-17 2022-10-25 /pmc/articles/PMC9621370/ /pubmed/36252037 http://dx.doi.org/10.1073/pnas.2103088119 Text en Copyright © 2022 the Author(s). Published by PNAS. https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under Creative Commons Attribution-NonCommercial-NoDerivatives License 4.0 (CC BY-NC-ND) (https://creativecommons.org/licenses/by-nc-nd/4.0/) .
spellingShingle Social Sciences
Shanahan, Michael J.
Cole, Steven W.
Ravi, Sudharshan
Chumbley, Justin
Xu, Wenjia
Potente, Cecilia
Levitt, Brandt
Bodelet, Julien
Aiello, Allison
Gaydosh, Lauren
Harris, Kathleen Mullan
Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
title Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
title_full Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
title_fullStr Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
title_full_unstemmed Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
title_short Socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
title_sort socioeconomic inequalities in molecular risk for chronic diseases observed in young adulthood
topic Social Sciences
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9621370/
https://www.ncbi.nlm.nih.gov/pubmed/36252037
http://dx.doi.org/10.1073/pnas.2103088119
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