The dual NOD1/NOD2 agonism of muropeptides containing a meso-diaminopimelic acid residue

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Abstract

Muropeptides are fragments of peptidoglycan that trigger innate immune responses by activating nucleotide-binding oligomerization domain (NOD) 1 and NOD2. Muropeptides from Gram-negative bacteria contain a meso-diaminopimelic acid (meso-DAP) residue in either a terminal or a non-terminal position. While the former ones are known to be recognized by NOD1, much less is known about recognition of muropeptides with non-terminal meso-DAP, which are most abundant moieties of Gram-negative peptidoglycans. Here, we developed a novel system to assess biological activity of muropeptides, based on CRISPR/Cas9-mediated knockout (KO) of NOD1 and NOD2 genes inmodified HEK293T cells. Using NOD1/NOD2 knockout and overexpression systems, as well as human monocytes and macrophages, we refine the current view ofmuropeptide recognition. We show that NOD2 can recognize different natural muropeptides containing a meso-DAP residue (preferably in a nonterminal position), provided they are present at micromolar concentrations. NOD2 accepts muropeptides with long and branched peptide chains and requires an intact N-acetylmuramyl residue. Muropeptides with non-terminal meso-DAP can activate NOD1 as well, but, in this case, probably require peptidase pre-processing to expose the meso-DAP residue. Depending on NOD1/NOD2 ratio in specific cell types,meso-DAP-containing muropeptides can be recognized either primarily via NOD2 (inmonocytes) or via NOD1 (in monocyte-derivedmacrophages and HEK293T-derived cells). The dual NOD1/NOD2 agonism of meso-DAP-containing muropeptides should be taken into account when assessing cellular responses to muropeptides and designing muropeptide immunostimulants and vaccine adjuvants.

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Dagil, Y. A., Arbatsky, N. P., Alkhazova, B. I., L’vov, V. L., Mazurov, D. V., & Pashenkov, M. V. (2016). The dual NOD1/NOD2 agonism of muropeptides containing a meso-diaminopimelic acid residue. PLoS ONE, 11(8). https://doi.org/10.1371/journal.pone.0160784

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