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Nanoscale imaging of CD47 informs how plasma membrane modifications shape apoptotic cell recognition.


ABSTRACT: CD47 recognized by its macrophage receptor SIRPα serves as a "don't eat-me" signal protecting viable cells from phagocytosis. How this is abrogated by apoptosis-induced changes in the plasma membrane, concomitantly with exposure of phosphatidylserine and calreticulin "eat-me" signals, is not well understood. Using STORM imaging and single-particle tracking, we interrogate how the distribution of these molecules on the cell surface correlates with plasma membrane alteration, SIRPα binding, and cell engulfment by macrophages. Apoptosis induces calreticulin clustering into blebs and CD47 mobility. Modulation of integrin affinity impacts CD47 mobility on the plasma membrane but not the SIRPα binding, whereas CD47/SIRPα interaction is suppressed by cholesterol destabilization. SIRPα no longer recognizes CD47 localized on apoptotic blebs. Overall, the data suggest that disorganization of the lipid bilayer at the plasma membrane, by inducing inaccessibility of CD47 possibly due to a conformational change, is central to the phagocytosis process.

SUBMITTER: Dufour S 

PROVIDER: S-EPMC9947010 | biostudies-literature | 2023 Feb

REPOSITORIES: biostudies-literature

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Nanoscale imaging of CD47 informs how plasma membrane modifications shape apoptotic cell recognition.

Dufour Samy S   Tacnet-Delorme Pascale P   Kleman Jean-Philippe JP   Glushonkov Oleksandr O   Thielens Nicole N   Bourgeois Dominique D   Frachet Philippe P  

Communications biology 20230222 1


CD47 recognized by its macrophage receptor SIRPα serves as a "don't eat-me" signal protecting viable cells from phagocytosis. How this is abrogated by apoptosis-induced changes in the plasma membrane, concomitantly with exposure of phosphatidylserine and calreticulin "eat-me" signals, is not well understood. Using STORM imaging and single-particle tracking, we interrogate how the distribution of these molecules on the cell surface correlates with plasma membrane alteration, SIRPα binding, and ce  ...[more]

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