AI Article Synopsis
- Understanding how T. cruzi interacts with host immunity is essential for managing infections and reducing symptoms of Chagas' disease.
- Recent findings highlight the role of innate immune receptors like TLRs and NLRs, particularly NLRP3, in this interaction across various immune cells.
- The modulation of macrophage activation and the metabolism of amino acids like L-arginine and tryptophan by enzymes such as iNOS, arginase, and IDO, as well as signaling pathways like AhR, mTOR, and Wnt, are key factors that help T. cruzi survive and replicate within the host.
Article Abstract
Current understanding of key cellular pathways, which are activated by the interaction between T. cruzi and host immunity, is crucial for controlling T. cruzi infection and also for limiting the development of the immunopathological symptoms of Chagas´ disease. Here, we focus on recent advances in the knowledge of modulation of innate receptors such as TLRs and NLRs, especially NLRP3, by T. cruzi in different cells of the immune system. On the other hand, the modulation of macrophage activation may be instrumental in allowing parasite persistence and long-term host survival. In this sense, we discuss the importance of the metabolism of two amino acids: L-arginine and tryptophan, and evaluate the role of iNOS, arginase and IDO enzymes in the regulation of innate and adaptive immune response during this infection; and, finally, we also discuss how T. cruzi exploits the AhR, mTOR and Wnt signaling pathways to promote their intracellular replication in macrophages, thus evading the host's immune response.
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| http://dx.doi.org/10.1016/j.bbadis.2020.165707 | DOI Listing |
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