Abstract
AbstractDrosophila Insulin-Producing Cells (IPCs) are the main production site of the Drosophila Insulin-like peptides or Dilps which have key roles in regulating growth, development, reproduction, lifespan and metabolism. To better understand the signalling pathways and transcriptional networks that are active in the IPCs we queried publicly available transcriptome data of over 180 highly inbred fly lines for dilp expression and used this as the input for a Genome-wide association study (GWAS). This resulted in the identification of variants in 125 genes that were associated with variation in dilp expression. The function of 57 of these genes in the IPCs was tested using an RNAi-based approach. We found that IPC-specific depletion of most genes resulted in differences in expression of one or more of the dilps. We then elaborated further on homothorax, one of the candidate genes with the strongest effect on dilp expression. We found that Homothorax and its binding partner Extradenticle are involved in regulating dilp2, -3 and -5 expression and that genetic depletion of both transcription factors leads to phenotypes associated with reduced insulin signalling. Furthermore, we provide evidence that other transcription factors involved in eye development are also functional in the IPCs. In conclusion, we showed that this GWAS approach using gene expression levels as input identified genetic regulators implicated in IPC function and dilp expression.
Publisher
Cold Spring Harbor Laboratory