Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line

Unlike single-gene mutations leading to Mendelian conditions, common human diseases are likely to be emergent phenomena arising from multilayer, multiscale, and highly interconnected interactions. Atrial and ventricular septal defects are the most common forms of cardiac congenital anomalies in huma...

Descripción completa

Detalles Bibliográficos
Autores principales: Moradi Marjaneh, Mahdi, Kirk, Edwin P, Patrick, Ralph, Alankarage, Dimuthu, Humphreys, David T, Del Monte-Nieto, Gonzalo, Cornejo-Paramo, Paola, Janbandhu, Vaibhao, Doan, Tram B, Dunwoodie, Sally L, Wong, Emily S, Moran, Chris, Martin, Ian CA, Thomson, Peter C, Harvey, Richard P
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2023
Materias:
Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10284603/
https://www.ncbi.nlm.nih.gov/pubmed/37272612
http://dx.doi.org/10.7554/eLife.83606
_version_ 1785061438426972160
author Moradi Marjaneh, Mahdi
Kirk, Edwin P
Patrick, Ralph
Alankarage, Dimuthu
Humphreys, David T
Del Monte-Nieto, Gonzalo
Cornejo-Paramo, Paola
Janbandhu, Vaibhao
Doan, Tram B
Dunwoodie, Sally L
Wong, Emily S
Moran, Chris
Martin, Ian CA
Thomson, Peter C
Harvey, Richard P
author_facet Moradi Marjaneh, Mahdi
Kirk, Edwin P
Patrick, Ralph
Alankarage, Dimuthu
Humphreys, David T
Del Monte-Nieto, Gonzalo
Cornejo-Paramo, Paola
Janbandhu, Vaibhao
Doan, Tram B
Dunwoodie, Sally L
Wong, Emily S
Moran, Chris
Martin, Ian CA
Thomson, Peter C
Harvey, Richard P
author_sort Moradi Marjaneh, Mahdi
collection PubMed
description Unlike single-gene mutations leading to Mendelian conditions, common human diseases are likely to be emergent phenomena arising from multilayer, multiscale, and highly interconnected interactions. Atrial and ventricular septal defects are the most common forms of cardiac congenital anomalies in humans. Atrial septal defects (ASD) show an open communication between the left and right atria postnatally, potentially resulting in serious hemodynamic consequences if untreated. A milder form of atrial septal defect, patent foramen ovale (PFO), exists in about one-quarter of the human population, strongly associated with ischaemic stroke and migraine. The anatomic liabilities and genetic and molecular basis of atrial septal defects remain unclear. Here, we advance our previous analysis of atrial septal variation through quantitative trait locus (QTL) mapping of an advanced intercross line (AIL) established between the inbred QSi5 and 129T2/SvEms mouse strains, that show extremes of septal phenotypes. Analysis resolved 37 unique septal QTL with high overlap between QTL for distinct septal traits and PFO as a binary trait. Whole genome sequencing of parental strains and filtering identified predicted functional variants, including in known human congenital heart disease genes. Transcriptome analysis of developing septa revealed downregulation of networks involving ribosome, nucleosome, mitochondrial, and extracellular matrix biosynthesis in the 129T2/SvEms strain, potentially reflecting an essential role for growth and cellular maturation in septal development. Analysis of variant architecture across different gene features, including enhancers and promoters, provided evidence for the involvement of non-coding as well as protein-coding variants. Our study provides the first high-resolution picture of genetic complexity and network liability underlying common congenital heart disease, with relevance to human ASD and PFO.
format Online
Article
Text
id pubmed-10284603
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher eLife Sciences Publications, Ltd
record_format MEDLINE/PubMed
spelling pubmed-102846032023-06-22 Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line Moradi Marjaneh, Mahdi Kirk, Edwin P Patrick, Ralph Alankarage, Dimuthu Humphreys, David T Del Monte-Nieto, Gonzalo Cornejo-Paramo, Paola Janbandhu, Vaibhao Doan, Tram B Dunwoodie, Sally L Wong, Emily S Moran, Chris Martin, Ian CA Thomson, Peter C Harvey, Richard P eLife Developmental Biology Unlike single-gene mutations leading to Mendelian conditions, common human diseases are likely to be emergent phenomena arising from multilayer, multiscale, and highly interconnected interactions. Atrial and ventricular septal defects are the most common forms of cardiac congenital anomalies in humans. Atrial septal defects (ASD) show an open communication between the left and right atria postnatally, potentially resulting in serious hemodynamic consequences if untreated. A milder form of atrial septal defect, patent foramen ovale (PFO), exists in about one-quarter of the human population, strongly associated with ischaemic stroke and migraine. The anatomic liabilities and genetic and molecular basis of atrial septal defects remain unclear. Here, we advance our previous analysis of atrial septal variation through quantitative trait locus (QTL) mapping of an advanced intercross line (AIL) established between the inbred QSi5 and 129T2/SvEms mouse strains, that show extremes of septal phenotypes. Analysis resolved 37 unique septal QTL with high overlap between QTL for distinct septal traits and PFO as a binary trait. Whole genome sequencing of parental strains and filtering identified predicted functional variants, including in known human congenital heart disease genes. Transcriptome analysis of developing septa revealed downregulation of networks involving ribosome, nucleosome, mitochondrial, and extracellular matrix biosynthesis in the 129T2/SvEms strain, potentially reflecting an essential role for growth and cellular maturation in septal development. Analysis of variant architecture across different gene features, including enhancers and promoters, provided evidence for the involvement of non-coding as well as protein-coding variants. Our study provides the first high-resolution picture of genetic complexity and network liability underlying common congenital heart disease, with relevance to human ASD and PFO. eLife Sciences Publications, Ltd 2023-06-05 /pmc/articles/PMC10284603/ /pubmed/37272612 http://dx.doi.org/10.7554/eLife.83606 Text en © 2023, Moradi Marjaneh, Kirk, Patrick et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Developmental Biology
Moradi Marjaneh, Mahdi
Kirk, Edwin P
Patrick, Ralph
Alankarage, Dimuthu
Humphreys, David T
Del Monte-Nieto, Gonzalo
Cornejo-Paramo, Paola
Janbandhu, Vaibhao
Doan, Tram B
Dunwoodie, Sally L
Wong, Emily S
Moran, Chris
Martin, Ian CA
Thomson, Peter C
Harvey, Richard P
Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
title Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
title_full Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
title_fullStr Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
title_full_unstemmed Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
title_short Quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
title_sort quantitative trait and transcriptome analysis of genetic complexity underpinning cardiac interatrial septation in mice using an advanced intercross line
topic Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10284603/
https://www.ncbi.nlm.nih.gov/pubmed/37272612
http://dx.doi.org/10.7554/eLife.83606
work_keys_str_mv AT moradimarjanehmahdi quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT kirkedwinp quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT patrickralph quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT alankaragedimuthu quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT humphreysdavidt quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT delmontenietogonzalo quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT cornejoparamopaola quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT janbandhuvaibhao quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT doantramb quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT dunwoodiesallyl quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT wongemilys quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT moranchris quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT martinianca quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT thomsonpeterc quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline
AT harveyrichardp quantitativetraitandtranscriptomeanalysisofgeneticcomplexityunderpinningcardiacinteratrialseptationinmiceusinganadvancedintercrossline

Ejemplares similares