AI Article Synopsis

  • Anti-bacterial proteins in mosquitoes help modulate the immune response to human pathogens, especially malaria, with this study focusing on AgNimB2 and AgEater from the Anopheles gambiae species.
  • Researchers found that AgNimB2 is misidentified in the genome and actually aids in phagocytosis of Staphylococcus aureus, functioning downstream of a complement-like pathway without directly interacting with the bacteria.
  • AgNimB2 also demonstrates an anti-Plasmodium effect, while AgEater appears to play a less significant role in the phagocytosis of either S. aureus or E. coli, shedding light on the functions of the Nimrod superfamily in malaria transmission.

Article Abstract

Anti-bacterial proteins in mosquitoes are known to play an important modulatory role on immune responses to infections with human pathogens including malaria parasites. In this study we characterized two members of the Anopheles gambiae Nimrod superfamily, namely AgNimB2 and AgEater. We confirm that current annotation of the An. gambiae genome incorrectly identifies AgNimB2 and AgEater as a single gene, AGAP009762. Through in silico and experimental approaches, it has been shown that AgNimB2 is a secreted protein that mediates phagocytosis of Staphylococcus aureus but not of Escherichia coli bacteria. We also reveal that this function does not involve a direct interaction of AgNimB2 with S. aureus. Therefore, AgNimB2 may act downstream of complement-like pathway activation, first requiring bacterial opsonization. In addition, it has been shown that AgNimB2 has an anti-Plasmodium effect. Conversely, AgEater is a membrane-bound protein that either functions redundantly or is dispensable for phagocytosis of E. coli or S. aureus. Our study provides insights into the role of members of the complex Nimrod superfamily in An. gambiae, the most important African vector of human malaria.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4073527PMC
http://dx.doi.org/10.1179/204777213X13867543472674DOI Listing

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