Leishmania allelic selection during experimental sand fly infection correlates with mutational signatures of oxidative DNA damage.
Giovanni BussottiBlaise LiPascale PescherBarbora VojtkovaIsabelle LouradourKaterina PruzinovaJovana SadlovaPetr VolfGerald Frank SpäthPublished in: Proceedings of the National Academy of Sciences of the United States of America (2023)
Trypanosomatid pathogens are transmitted by blood-feeding insects, causing devastating human infections. These parasites show important phenotypic shifts that often impact parasite pathogenicity, tissue tropism, or drug susceptibility. The evolutionary mechanisms that allow for the selection of such adaptive phenotypes remain only poorly investigated. Here, we use Leishmania donovani as a trypanosomatid model pathogen to assess parasite evolutionary adaptation during experimental sand fly infection. Comparing the genome of the parasites before and after sand fly infection revealed a strong population bottleneck effect as judged by allele frequency analysis. Apart from random genetic drift caused by the bottleneck effect, our analyses revealed haplotype and allelic changes during sand fly infection that seem under natural selection given their convergence between independent biological replicates. Our analyses further uncovered signature mutations of oxidative DNA damage in the parasite genomes after sand fly infection, suggesting that Leishmania suffers from oxidative stress inside the insect digestive tract. Our results propose a model of Leishmania genomic adaptation during sand fly infection, with oxidative DNA damage and DNA repair processes likely driving haplotype and allelic selection. The experimental and computational framework presented here provides a useful blueprint to assess evolutionary adaptation of other eukaryotic pathogens inside their insect vectors, such as Plasmodium spp, Trypanosoma brucei , and Trypanosoma cruzi .
Keyphrases
- dna damage
- dna repair
- oxidative stress
- drinking water
- plasmodium falciparum
- trypanosoma cruzi
- genome wide
- emergency department
- staphylococcus aureus
- endothelial cells
- dna methylation
- copy number
- escherichia coli
- gram negative
- high resolution
- multidrug resistant
- mass spectrometry
- dna damage response
- drug induced
- life cycle
- data analysis
- heat shock protein