High-throughput genetic mapping discovers novel zinc toxicity response loci in Drosophila melanogaster

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Abstract

Heavy metals are a widespread environmental contaminant, and even low levels of some metals can disrupt cellular processes and result in DNA damage. However, the consequences of metal exposure are variable among individuals, with susceptibility to metal toxicity representing a complex trait influenced by genetic and non-genetic factors. To uncover toxicity response genes, and better understand responses to metal toxicity, we sought to dissect resistance to zinc, a metal required for normal cellular function, which can be toxic at high doses. To facilitate efficient, powerful discovery of Quantitative Trait Loci (QTL) we employed extreme, or X-QTL mapping, leveraging a multiparental, recombinant Drosophila melanogaster population. Our approach involved bulk selection of zinc-resistant individuals, sequencing several replicate pools of selected and control animals, and identified QTL as genomic positions showing consistent allele frequency shifts between treatments. We successfully identified seven regions segregating for resistance/susceptibility alleles, and implicated several strong candidate genes. Phenotypic characterization of populations derived from selected or control animals revealed that our selection procedure resulted in greater egg-to-adult emergence, and a reduced developmental delay on zinc media. We subsequently measured emergence and development time for a series of midgut-specific RNAi gene knockdowns and matched genetic controls raised in both zinc-supplemented and normal media. This identified ten genes with significant genotype-by-treatment effects, including pHCl-2 , which encodes a zinc sensor protein. Our work highlights recognized and novel contributors to zinc toxicity resistance in flies, and provides a pathway to a broader understanding of the biological impact of metal toxicity.

ARTICLE SUMMARY

Starting with an outbred Drosophila melanogaster population we repeatedly selected for groups of individuals showing high resistance to toxic levels of zinc during development. Pooled sequencing of these groups, along with matched groups of control individuals, enabled the identification of seven genomic regions – or QTL – contributing to zinc toxicity resistance. Midgut-specific RNAi of genes implicated by these QTL yielded ten genes impacting developmental traits in zinc-supplemented media, including MTF-1 (a metal response transcription factor) and pHCl-2 (a zinc sensor protein).

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