Autophagy proteins stabilize pathogen-containing phagosomes for prolonged MHC II antigen processing

Romao, Susana; Gasser, Nathalie; Becker, Andrea C.

doi:10.1083/jcb.201308173

Javascript is disabled or not supported in your browser. JavaScript must be enabled in order for you to use WIKINDX fully. Enable JavaScript through your browser options then try again, otherwise, try using a different browser.

BioAcyl Corp

WIKINDX Resources

Romao, S., Gasser, N., & Becker, A. C. (2013). Autophagy proteins stabilize pathogen-containing phagosomes for prolonged MHC II antigen processing. Journal of Cell Biology, 203(5), 757–766.
Added by: Dr. Enrique Feoli (02/05/2024, 11:38) Last edited by: Dr. Enrique Feoli (29/12/2025, 18:54)

Resource type: Journal Article
DOI: 10.1083/jcb.201308173
ID no. (ISBN etc.): 0021-9525
BibTeX citation key: Romao2013
View all bibliographic details

Categories: ARIA, BioAcyl Corp
Subcategories: Autophagy and mitophagy
Creators: Becker, Gasser, Romao
Collection: Journal of Cell Biology

Views: 5/165

Abstract

{Antigen preservation for presentation is a hallmark of potent antigen-presenting cells. In this paper, we report that in human macrophages and dendritic cells, a subset of phagosomes gets coated with Atg8/LC3, a component of the molecular machinery of macroautophagy, and maintains phagocytosed antigens for prolonged presentation on major histocompatibility complex class II molecules. These Atg8/LC3-positive phagosomes are formed around the antigen with TLR2 agonists and require reactive oxygen species production by NOX2 for their generation. A deficiency in the NOX2-dependent formation of these antigen storage phagosomes could contribute to compromise antifungal immune control in chronic granulomatous disease patients.}