| Literature DB >> 33503439 |
Charles Maisonneuve1, Derek K L Tsang1, Elisabeth G Foerster1, Lukian Maxence Robert1, Tapas Mukherjee1, Dave Prescott1, Ivan Tattoli2, Paul Lemire3, Daniel A Winer4, Shawn Winer5, Catherine J Streutker5, Kaoru Geddes1, Ken Cadwell6, Richard L Ferrero7, Alberto Martin1, Stephen E Girardin2, Dana J Philpott8.
Abstract
Pioneering studies from the early 1980s suggested that bacterial peptidoglycan-derived muramyl peptides (MPs) could exert either stimulatory or immunosuppressive functions depending, in part, on chronicity of exposure. However, this Janus-faced property of MPs remains largely unexplored. Here, we demonstrate the immunosuppressive potential of Nod1, the bacterial sensor of diaminopimelic acid (DAP)-containing MPs. Using a model of self-limiting peritonitis, we show that systemic Nod1 activation promotes an autophagy-dependent reprogramming of macrophages toward an alternative phenotype. Moreover, Nod1 stimulation induces the expansion of myeloid-derived suppressor cells (MDSCs) and maintains their immunosuppressive potential via arginase-1 activity. Supporting the role of MDSCs and tumor-associated macrophages in cancer, we demonstrate that myeloid-intrinsic Nod1 expression sustains intra-tumoral arginase-1 levels to foster an immunosuppressive and tumor-permissive microenvironment during colorectal cancer (CRC) development. Our findings support the notion that bacterial products, via Nod1 detection, modulate the immunosuppressive activity of myeloid cells and fuel tumor progression in CRC.Entities:
Keywords: Atg16L1; MDSC; Nod1 receptor; TAM; TME; arginase-1; autophagy; colon cancer; immunosuppression; microbiota
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Year: 2021 PMID: 33503439 DOI: 10.1016/j.celrep.2020.108677
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423