The receptor DNGR-1 signals for phagosomal rupture to promote cross-presentation of dead-cell-associated antigens

Canton, Johnathan; Blees, Hanna; Henry, Conor M.; Buck, Michael D.; Schulz, Oliver; Rogers, Neil C.; Childs, Eleanor; Zelenay, Santiago; Rhys, Hefin; Domart, Marie Charlotte; Collinson, Lucy; Alloatti, Andrés; Ellison, Cara J.; Amigorena, Sebastian; Papayannopoulos, Venizelos; Thomas, David C.; Randow, Felix; Reis e Sousa, Caetano

doi:10.1038/s41590-020-00824-x

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dc.contributor.author

Canton, Johnathan

dc.contributor.author

Blees, Hanna

dc.contributor.author

Henry, Conor M.

dc.contributor.author

Buck, Michael D.

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Schulz, Oliver

dc.contributor.author

Rogers, Neil C.

dc.contributor.author

Childs, Eleanor

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Zelenay, Santiago

dc.contributor.author

Rhys, Hefin

dc.contributor.author

Domart, Marie Charlotte

dc.contributor.author

Collinson, Lucy

dc.contributor.author

Alloatti, Andrés Se ha confirmado la validez de este valor de autoridad por un usuario

dc.contributor.author

Ellison, Cara J.

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Amigorena, Sebastian

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Papayannopoulos, Venizelos

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Thomas, David C.

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Randow, Felix

dc.contributor.author

Reis e Sousa, Caetano

dc.date.available

2023-01-26T13:45:56Z

dc.date.issued

2021-02

dc.identifier.citation

Canton, Johnathan; Blees, Hanna; Henry, Conor M.; Buck, Michael D.; Schulz, Oliver; et al.; The receptor DNGR-1 signals for phagosomal rupture to promote cross-presentation of dead-cell-associated antigens; Nature Publishing Group; Nature Immunology (print); 22; 2; 2-2021; 140-153

dc.identifier.issn

1529-2908

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http://hdl.handle.net/11336/185763

dc.description.abstract

Type 1 conventional dendritic (cDC1) cells are necessary for cross-presentation of many viral and tumor antigens to CD8+ T cells. cDC1 cells can be identified in mice and humans by high expression of DNGR-1 (also known as CLEC9A), a receptor that binds dead-cell debris and facilitates XP of corpse-associated antigens. Here, we show that DNGR-1 is a dedicated XP receptor that signals upon ligand engagement to promote phagosomal rupture. This allows escape of phagosomal contents into the cytosol, where they access the endogenous major histocompatibility complex class I antigen processing pathway. The activity of DNGR-1 maps to its signaling domain, which activates SYK and NADPH oxidase to cause phagosomal damage even when spliced into a heterologous receptor and expressed in heterologous cells. Our data reveal the existence of innate immune receptors that couple ligand binding to endocytic vesicle damage to permit MHC class I antigen presentation of exogenous antigens and to regulate adaptive immunity.

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application/pdf

dc.language.iso

eng

dc.publisher

Nature Publishing Group Se ha confirmado la validez de este valor de autoridad por un usuario

dc.rights

info:eu-repo/semantics/restrictedAccess

dc.rights.uri

https://creativecommons.org/licenses/by-nc-sa/2.5/ar/

dc.subject

DNRG-1

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dendritic cells

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cross-presentation

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phagosome rupture

dc.subject.classification

Inmunología Se ha confirmado la validez de este valor de autoridad por un usuario

dc.subject.classification

Medicina Básica Se ha confirmado la validez de este valor de autoridad por un usuario

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CIENCIAS MÉDICAS Y DE LA SALUD Se ha confirmado la validez de este valor de autoridad por un usuario

dc.title

The receptor DNGR-1 signals for phagosomal rupture to promote cross-presentation of dead-cell-associated antigens

dc.type

info:eu-repo/semantics/article

dc.type

info:ar-repo/semantics/artículo

dc.type

info:eu-repo/semantics/publishedVersion

dc.date.updated

2022-10-06T10:42:49Z

dc.journal.volume

22

dc.journal.number

2

dc.journal.pagination

140-153

dc.journal.pais

Reino Unido Se ha confirmado la validez de este valor de autoridad por un usuario

dc.journal.ciudad

Londres

dc.description.fil

Fil: Canton, Johnathan. No especifíca;

dc.description.fil

Fil: Blees, Hanna. No especifíca;

dc.description.fil

Fil: Henry, Conor M.. No especifíca;

dc.description.fil

Fil: Buck, Michael D.. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Schulz, Oliver. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Rogers, Neil C.. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Childs, Eleanor. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Zelenay, Santiago. University of Manchester; Reino Unido

dc.description.fil

Fil: Rhys, Hefin. No especifíca;

dc.description.fil

Fil: Domart, Marie Charlotte. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Collinson, Lucy. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Alloatti, Andrés. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Rosario. Instituto de Inmunología Clinica y Experimental de Rosario. Universidad Nacional de Rosario. Facultad de Ciencias Médicas. Instituto de Inmunología Clinica y Experimental de Rosario; Argentina

dc.description.fil

Fil: Ellison, Cara J.. Imperial College London; Reino Unido

dc.description.fil

Fil: Amigorena, Sebastian. Inserm; Francia

dc.description.fil

Fil: Papayannopoulos, Venizelos. The Francis Crick Institute; Reino Unido

dc.description.fil

Fil: Thomas, David C.. University of Cambridge; Estados Unidos

dc.description.fil

Fil: Randow, Felix. Imperial College London; Reino Unido

dc.description.fil

Fil: Reis e Sousa, Caetano. The Francis Crick Institute; Reino Unido

dc.journal.title

Nature Immunology (print) Se ha confirmado la validez de este valor de autoridad por un usuario

dc.relation.alternativeid

info:eu-repo/semantics/altIdentifier/doi/http://dx.doi.org/10.1038/s41590-020-00824-x

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