Formylated MHC class Ib binding peptides activate both human and mouse Neutrophils primarily through formyl peptide receptor 1

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Abstract

Two different immune recognition systems have evolved in parallel to recognize peptides starting with an N-formylated methionine, and recognition similarities/differences between these two systems have been investigated. A number of peptides earlier characterized in relation to the H2-M3 complex that presents N-formylated peptides to cytotoxic T cells, have been characterized in relation to the formyl peptide receptors expressed by phagocytic neutrophils in both men (FPRs) and mice (Fprs). FPR1/Fpr1 was identified as the preferred receptor for all fMet-containing peptides examined, but there was no direct correlation between H2-M3 binding and the neutrophil activation potencies. Similarly, there was no direct correlation between the activities induced by the different peptides in human and mouse neutrophils, respectively. The formyl group was important in both H2-M3 binding and FPR activation, but FPR2 was the preferred receptor for the non-formylated peptide. The structural requirements differed between the H2-M3 and FPR/Fpr recognition systems and these data suggest that the two recognition systems have different evolutionary traits.

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Winther, M., Holdfeldt, A., Gabl, M., Wang, J. M., Forsman, H., & Dahlgren, C. (2016). Formylated MHC class Ib binding peptides activate both human and mouse Neutrophils primarily through formyl peptide receptor 1. PLoS ONE, 11(12). https://doi.org/10.1371/journal.pone.0167529

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