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Greece Project Notice - Phagosomal Lc3s Alternative Role


Project Notice

PNR 65164
Project Name Phagosomal LC3s Alternative Role
Project Detail Dissecting host-fungus interplay Aspergillus fumigatus is an opportunistic pathogen and can cause serious respiratory infections in individuals with compromised immune systems. Understanding the interplay between A. fumigatus and host immune cells is critical for combating such infections. A. fumigatus is typically eliminated by alveolar macrophages through phagocytosis, but the fungus has evolved strategies to evade this process. The EU-funded POLAR project aims to investigate the molecular mechanism of phagosome formation and membrane repair during A. fumigatus infection. Project findings will guide the design of new immunomodulatory strategies against fungal pathogens and deepen our understanding of macrophage biology. The opportunistic fungus Aspergillus fumigatus is an emerging cause of life-threatening respiratory infections in an expanding group of patients with acquired innate immune defects. Dissecting the molecular dynamics of fungal-host interplay mediating sterilizing immunity against A. fumigatus is crucial to gain insight in disease pathogenesis and develop novel immunomodulatory therapies. Physiologically, Aspergillus fumigatus conidia are eliminated inside Alveolar Macrophages (AMs) via activation of the LC3 associated phagocytosis (LAP) pathway. A. fumigatus cell wall melanin blocks LAP to promote pathogenicity. Intracellular germination of A. fumigatus conidia results in exposure of immunostimulatory fungal molecules concomitantly with melanin removal and triggers NADPH oxidase-dependent activation of LAP. The molecular mechanism of LC3 conjugation on A. fumigatus phagosome membrane and the physiological function of LAP on AM biology and antifungal host defense remain elusive. Of interest, pilot studies in the host lab demonstrate that infection of AMs and other types of macrophages with live conidia of A. fumigatus results in a unique pattern of pulsatile LC3 recruitment on the phagosome membrane, which is accompanied by waves of increased phagosome permeability. These findings imply for a novel mechanism of LC3+ phagosome (LAPosome) formation via cytosolic sensing of fungal vita-PAMPs and suggests for an unconventional function of LAPosomes in regulation of membrane repair mechanisms in response to damage induced by Aspergillus infection. This research project aims to understand the precise host and pathogen molecular determinants of LAPosome formation and exploit the intriguing role of LC3 on regulation of phagosomal membrane repair during A. fumigatus infection. Using A. fumigatus as a model pathogen, this project with provide fundamental insights on the role of LAP in macrophage biology paving the way for new host-directed strategies.
Funded By European Union (EU)
Sector BPO
Country Greece , Western Europe
Project Value EUR 153,487

Contact Information

Company Name IDRYMA TECHNOLOGIAS KAI EREVNAS
Web Site https://cordis.europa.eu/project/id/101180628

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