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Zooming in on common immune evasion mechanisms of pathogens in phagolysosomes: potential broad-spectrum therapeutic targets against infectious diseases. | LitMetric

AI Article Synopsis

  • Intracellular pathogens like viruses, bacteria, and parasites develop strategies to evade the host's immune system, allowing them to spread and cause severe diseases.
  • They interfere with various stages of the immune response, such as cell entry, phagosome formation, and the breakdown of pathogens in phagolysosomes.
  • Understanding the common mechanisms used by these pathogens could help identify new targets for drug development, aiding in the fight against infections.

Article Abstract

The intracellular viral, bacterial, or parasitic pathogens evade the host immune challenges to propagate and cause fatal diseases. The microbes overpower host immunity at various levels including during entry into host cells, phagosome formation, phagosome maturation, phagosome-lysosome fusion forming phagolysosomes, acidification of phagolysosomes, and at times after escape into the cytosol. Phagolysosome is the final organelle in the phagocyte with sophisticated mechanisms to degrade the pathogens. The immune evasion strategies by the pathogens include the arrest of host cell apoptosis, decrease in reactive oxygen species, the elevation of Th2 anti-inflammatory response, avoidance of autophagy and antigen cross-presentation pathways, and escape from phagolysosomal killing. Since the phagolysosome organelle in relation to infection/cure is seldom discussed in the literature, we summarize here the common host as well as pathogen targets manipulated or utilized by the pathogens established in phagosomes and phagolysosomes, to hijack the host immune system for their benefit. These common molecules or pathways can be broad-spectrum therapeutic targets for drug development for intervention against infectious diseases caused by different intracellular pathogens.

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Source
http://dx.doi.org/10.1093/femsre/fuac041DOI Listing

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