Login / Signup

Transposon mutagenesis of Rickettsia felis sca1 confers a distinct phenotype during flea infection.

Hanna J LaukaitisTriston T CooperChanakan SuwanbongkotVictoria I VerhoeveTimothy J KurttiUlrike G MunderlohKevin R Macaluso
Published in: PLoS pathogens (2022)
Since its recognition in 1994 as the causative agent of human flea-borne spotted fever, Rickettsia felis, has been detected worldwide in over 40 different arthropod species. The cat flea, Ctenocephalides felis, is a well-described biological vector of R. felis. Unique to insect-borne rickettsiae, R. felis can employ multiple routes of infection including inoculation via salivary secretions and potentially infectious flea feces into the skin of vertebrate hosts. Yet, little is known of the molecular interactions governing flea infection and subsequent transmission of R. felis. While the obligate intracellular nature of rickettsiae has hampered the function of large-scale mutagenesis strategies, studies have shown the efficiency of mariner-based transposon systems in Rickettsiales. Thus, this study aimed to assess R. felis genetic mutants in a flea transmission model to elucidate genes involved in vector infection. A Himar1 transposase was used to generate R. felis transformants, in which subsequent genome sequencing revealed a transposon insertion near the 3' end of sca1. Alterations in sca1 expression resulted in unique infection phenotypes. While the R. felis sca1::tn mutant portrayed enhanced growth kinetics compared to R. felis wild-type during in vitro culture, rickettsial loads were significantly reduced during flea infection. As a consequence of decreased rickettsial loads within infected donor fleas, R. felis sca1::tn exhibited limited transmission potential. Thus, the use of a biologically relevant model provides evidence of a defective phenotype associated with R. felis sca1::tn during flea infection.
Keyphrases
  • wild type
  • endothelial cells
  • crispr cas
  • gene expression
  • poor prognosis
  • zika virus
  • climate change
  • single molecule
  • soft tissue
  • aedes aegypti
  • copy number
  • human health
  • induced pluripotent stem cells