F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells.

Susan Ahrens; Santiago Zelenay; David Sancho; Pavel Hanč; Svend Kjær; Christoph Feest; Georgina Fletcher; Charlotte Durkin; Antonio Postigo; Mark Skehel; Facundo Batista; Barry Thompson; Michael Way; Caetano Reis e Sousa; Oliver Schulz

doi:10.1016/j.immuni.2012.03.008

F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells.

Susan Ahrens, Santiago Zelenay, David Sancho, Pavel Hanč, Svend Kjær, Christoph Feest, Georgina Fletcher, Charlotte Durkin, Antonio Postigo, Mark Skehel, Facundo Batista, Barry Thompson, Michael Way, Caetano Reis e Sousa, Oliver Schulz

The University of Manchester

Research output: Contribution to journal › Article › peer-review

Abstract

Sterile inflammation can be initiated by innate immune recognition of markers of tissue injury termed damage-associated molecular patterns (DAMPs). DAMP recognition by dendritic cells (DCs) has also been postulated to lead to T cell responses to foreign antigens in tumors or allografts. Many DAMPs represent intracellular contents that are released upon cell damage, notably after necrosis. In this regard, we have previously described DNGR-1 (CLEC9A) as a DC-restricted receptor specific for an unidentified DAMP that is exposed by necrotic cells and is necessary for efficient priming of cytotoxic T cells against dead cell-associated antigens. Here, we have shown that the DNGR-1 ligand is preserved from yeast to man and corresponds to the F-actin component of the cellular cytoskeleton. The identification of F-actin as a DNGR-1 ligand suggests that cytoskeletal exposure is a universal sign of cell damage that can be targeted by the innate immune system to initiate immunity.

Original language	English
Journal	Immunity
Volume	36
Issue number	4
DOIs	https://doi.org/10.1016/j.immuni.2012.03.008
Publication status	Published - 20 Apr 2012

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Ahrens, S., Zelenay, S., Sancho, D., Hanč, P., Kjær, S., Feest, C., Fletcher, G., Durkin, C., Postigo, A., Skehel, M., Batista, F., Thompson, B., Way, M., Reis e Sousa, C., & Schulz, O. (2012). F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells. Immunity, 36(4). https://doi.org/10.1016/j.immuni.2012.03.008

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title = "F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells.",

abstract = "Sterile inflammation can be initiated by innate immune recognition of markers of tissue injury termed damage-associated molecular patterns (DAMPs). DAMP recognition by dendritic cells (DCs) has also been postulated to lead to T cell responses to foreign antigens in tumors or allografts. Many DAMPs represent intracellular contents that are released upon cell damage, notably after necrosis. In this regard, we have previously described DNGR-1 (CLEC9A) as a DC-restricted receptor specific for an unidentified DAMP that is exposed by necrotic cells and is necessary for efficient priming of cytotoxic T cells against dead cell-associated antigens. Here, we have shown that the DNGR-1 ligand is preserved from yeast to man and corresponds to the F-actin component of the cellular cytoskeleton. The identification of F-actin as a DNGR-1 ligand suggests that cytoskeletal exposure is a universal sign of cell damage that can be targeted by the innate immune system to initiate immunity.",

author = "Susan Ahrens and Santiago Zelenay and David Sancho and Pavel Han{\v c} and Svend Kj{\ae}r and Christoph Feest and Georgina Fletcher and Charlotte Durkin and Antonio Postigo and Mark Skehel and Facundo Batista and Barry Thompson and Michael Way and \{Reis e Sousa\}, Caetano and Oliver Schulz",

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Ahrens, S, Zelenay, S, Sancho, D, Hanč, P, Kjær, S, Feest, C, Fletcher, G, Durkin, C, Postigo, A, Skehel, M, Batista, F, Thompson, B, Way, M, Reis e Sousa, C & Schulz, O 2012, 'F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells.', Immunity, vol. 36, no. 4. https://doi.org/10.1016/j.immuni.2012.03.008

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T1 - F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells.

AU - Ahrens, Susan

AU - Zelenay, Santiago

AU - Sancho, David

AU - Hanč, Pavel

AU - Kjær, Svend

AU - Feest, Christoph

AU - Fletcher, Georgina

AU - Durkin, Charlotte

AU - Postigo, Antonio

AU - Skehel, Mark

AU - Batista, Facundo

AU - Thompson, Barry

AU - Way, Michael

AU - Reis e Sousa, Caetano

AU - Schulz, Oliver

N1 - , Cancer Research UK, United Kingdom

PY - 2012/4/20

Y1 - 2012/4/20

N2 - Sterile inflammation can be initiated by innate immune recognition of markers of tissue injury termed damage-associated molecular patterns (DAMPs). DAMP recognition by dendritic cells (DCs) has also been postulated to lead to T cell responses to foreign antigens in tumors or allografts. Many DAMPs represent intracellular contents that are released upon cell damage, notably after necrosis. In this regard, we have previously described DNGR-1 (CLEC9A) as a DC-restricted receptor specific for an unidentified DAMP that is exposed by necrotic cells and is necessary for efficient priming of cytotoxic T cells against dead cell-associated antigens. Here, we have shown that the DNGR-1 ligand is preserved from yeast to man and corresponds to the F-actin component of the cellular cytoskeleton. The identification of F-actin as a DNGR-1 ligand suggests that cytoskeletal exposure is a universal sign of cell damage that can be targeted by the innate immune system to initiate immunity.

AB - Sterile inflammation can be initiated by innate immune recognition of markers of tissue injury termed damage-associated molecular patterns (DAMPs). DAMP recognition by dendritic cells (DCs) has also been postulated to lead to T cell responses to foreign antigens in tumors or allografts. Many DAMPs represent intracellular contents that are released upon cell damage, notably after necrosis. In this regard, we have previously described DNGR-1 (CLEC9A) as a DC-restricted receptor specific for an unidentified DAMP that is exposed by necrotic cells and is necessary for efficient priming of cytotoxic T cells against dead cell-associated antigens. Here, we have shown that the DNGR-1 ligand is preserved from yeast to man and corresponds to the F-actin component of the cellular cytoskeleton. The identification of F-actin as a DNGR-1 ligand suggests that cytoskeletal exposure is a universal sign of cell damage that can be targeted by the innate immune system to initiate immunity.

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DO - 10.1016/j.immuni.2012.03.008

M3 - Article

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SN - 1097-4180

VL - 36

JO - Immunity

JF - Immunity

IS - 4

ER -

F-actin is an evolutionarily conserved damage-associated molecular pattern recognized by DNGR-1, a receptor for dead cells.

Abstract

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