4.8 Article

Genetic architecture of natural variation of cardiac performance from flies to humans

期刊

ELIFE
卷 11, 期 -, 页码 -

出版社

eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.82459

关键词

heart function; GWAS; gene regulatory networks; Drosophila; human; conserved genetic architecture; D; melanogaster

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资金

  1. Fondation de France [00071034]
  2. Aix-Marseille Universite
  3. National Institutes of Health [R01 HL148827-03, R01 HL149992-02, R01 AG071464-01, R01 HL132241, R21 AG061598]
  4. U.S. Department of Defense [R01 AG071464-01]

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Studying the cardiac performance variations in Drosophila reveals genetic networks associated with natural variation of cardiac traits and identifies genes related to cardiac function variations. The findings in fruit flies can potentially accelerate the discovery of heart diseases in humans.
Deciphering the genetic architecture of human cardiac disorders is of fundamental importance but their underlying complexity is a major hurdle. We investigated the natural variation of cardiac performance in the sequenced inbred lines of the Drosophila Genetic Reference Panel (DGRP). Genome-wide associations studies (GWAS) identified genetic networks associated with natural variation of cardiac traits which were used to gain insights as to the molecular and cellular processes affected. Non-coding variants that we identified were used to map potential regulatory non-coding regions, which in turn were employed to predict transcription factors (TFs) binding sites. Cognate TFs, many of which themselves bear polymorphisms associated with variations of cardiac performance, were also validated by heart-specific knockdown. Additionally, we showed that the natural variations associated with variability in cardiac performance affect a set of genes overlapping those associated with average traits but through different variants in the same genes. Furthermore, we showed that phenotypic variability was also associated with natural variation of gene regulatory networks. More importantly, we documented correlations between genes associated with cardiac phenotypes in both flies and humans, which supports a conserved genetic architecture regulating adult cardiac function from arthropods to mammals. Specifically, roles for PAX9 and EGR2 in the regulation of the cardiac rhythm were established in both models, illustrating that the characteristics of natural variations in cardiac function identified in Drosophila can accelerate discovery in humans.

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