Genetic variation in the Yolk protein expression network of Drosophila melanogaster: sex-biased negative correlations with longevity. Academic Article

abstract

• One of the persistent problems in biology is understanding how genetic variation contributes to phenotypic variation. Associations at many levels have been reported, and yet causal inference has remained elusive. We propose to rely on the knowledge of causal relationships established by molecular biology approaches. The existing molecular knowledge forms a firm backbone upon which hypotheses connecting genetic variation, transcriptional variation and phenotypic variation can be built. The sex determination pathway is a well-established molecular network, with the Yolk protein 1-3 (Yp) genes as the most downstream target. Our analyses reveal that genetic variation in expression for genes known to be upstream in the pathway explains variation in downstream targets. Relationships differ between the two sexes, and each Yp has a distinct transcriptional pattern. Yp expression is significantly negatively correlated with longevity, an important life history trait, for both males and females.

authors

• Tarone, Aaron

published proceedings

• Heredity (Edinb)

author list (cited authors)

• Tarone, A. M., McIntyre, L. M., Harshman, L. G., & Nuzhdin, S. V.

citation count

• 24

complete list of authors

• Tarone, AM||McIntyre, LM||Harshman, LG||Nuzhdin, SV

publication date

• October 2012

publisher

• Springer Nature  Publisher

published in

• Heredity  Journal

keywords

• Animals
• Cluster Analysis
• Dosage Compensation, Genetic
• Drosophila Melanogaster
• Drosophila Proteins
• Egg Proteins
• Female
• Gene Regulatory Networks
• Genetic Variation
• Longevity
• Male
• Models, Molecular
• Sex Determination Processes
• Systems Biology
• Transcriptome
• Vitellogenins

Digital Object Identifier (DOI)

• 10.1038/hdy.2012.34

start page

• 226

end page

• 234

volume

• 109

issue

• 4

URL

• http://dx.doi.org/10.1038/hdy.2012.34