TRPV2 has a pivotal role in macrophage particle binding and phagocytosis

Tiffany M. Link; Una Park; Becky M. Vonakis; Daniel M. Raben; Mark J. Soloski; Michael J. Caterina

doi:10.1038/ni.1842

TRPV2 has a pivotal role in macrophage particle binding and phagocytosis

Tiffany M. Link, Una Park, Becky M. Vonakis, Daniel M. Raben, Mark J. Soloski, Michael J. Caterina

School of Medicine

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

171 Scopus citations

Abstract

Macrophage phagocytosis is critical for defense against pathogens. Whereas many steps of phagocytosis involve ionic flux, the underlying ion channels remain ill defined. Here we show that zymosan-, immunoglobulin G (IgG)-and complement-mediated particle binding and phagocytosis were impaired in macrophages lacking the cation channel TRPV2. TRPV2 was recruited to the nascent phagosome and depolarized the plasma membrane. Depolarization increased the synthesis of phosphatidylinositol-4,5-bisphosphate (PtdIns(4,5)P 2), which triggered the partial actin depolymerization necessary for occupancy-elicited phagocytic receptor clustering. TRPV2-deficient macrophages were also defective in chemoattractant-elicited motility. Consequently, TRPV2-deficient mice showed accelerated mortality and greater organ bacterial load when challenged with Listeria monocytogenes. Our data demonstrate the participation of TRPV2 in early phagocytosis and its fundamental importance in innate immunity.

Original language	English (US)
Pages (from-to)	232-239
Number of pages	8
Journal	Nature Immunology
Volume	11
Issue number	3
DOIs	https://doi.org/10.1038/ni.1842
State	Published - Mar 2010

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.1038/ni.1842

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title = "TRPV2 has a pivotal role in macrophage particle binding and phagocytosis",

abstract = "Macrophage phagocytosis is critical for defense against pathogens. Whereas many steps of phagocytosis involve ionic flux, the underlying ion channels remain ill defined. Here we show that zymosan-, immunoglobulin G (IgG)-and complement-mediated particle binding and phagocytosis were impaired in macrophages lacking the cation channel TRPV2. TRPV2 was recruited to the nascent phagosome and depolarized the plasma membrane. Depolarization increased the synthesis of phosphatidylinositol-4,5-bisphosphate (PtdIns(4,5)P 2), which triggered the partial actin depolymerization necessary for occupancy-elicited phagocytic receptor clustering. TRPV2-deficient macrophages were also defective in chemoattractant-elicited motility. Consequently, TRPV2-deficient mice showed accelerated mortality and greater organ bacterial load when challenged with Listeria monocytogenes. Our data demonstrate the participation of TRPV2 in early phagocytosis and its fundamental importance in innate immunity.",

author = "Link, {Tiffany M.} and Una Park and Vonakis, {Becky M.} and Raben, {Daniel M.} and Soloski, {Mark J.} and Caterina, {Michael J.}",

note = "Funding Information: We thank J. Brederson, M.-K. Chung, S. Huang, M. Meffert, C. Munns and V. Vega for suggestions; J. Wang and S. Li for technical assistance; S. Hudson for help with flow cytometry; P. Devreotes (Johns Hopkins School of Medicine) for suggestions and latrunculin A; and W. Bishai and S. Huang for critically reading the manuscript. Supported by the National Institutes of Health (R01NS051551 to MJC, RO1AI42287-05 to M.J.S.; AI059298 and AI071117 to B.M.V.; GM059251 to D.M.R.; and a Medical Scientist Training Program Award to T.M.L.).",

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AU - Caterina, Michael J.

N1 - Funding Information: We thank J. Brederson, M.-K. Chung, S. Huang, M. Meffert, C. Munns and V. Vega for suggestions; J. Wang and S. Li for technical assistance; S. Hudson for help with flow cytometry; P. Devreotes (Johns Hopkins School of Medicine) for suggestions and latrunculin A; and W. Bishai and S. Huang for critically reading the manuscript. Supported by the National Institutes of Health (R01NS051551 to MJC, RO1AI42287-05 to M.J.S.; AI059298 and AI071117 to B.M.V.; GM059251 to D.M.R.; and a Medical Scientist Training Program Award to T.M.L.).

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N2 - Macrophage phagocytosis is critical for defense against pathogens. Whereas many steps of phagocytosis involve ionic flux, the underlying ion channels remain ill defined. Here we show that zymosan-, immunoglobulin G (IgG)-and complement-mediated particle binding and phagocytosis were impaired in macrophages lacking the cation channel TRPV2. TRPV2 was recruited to the nascent phagosome and depolarized the plasma membrane. Depolarization increased the synthesis of phosphatidylinositol-4,5-bisphosphate (PtdIns(4,5)P 2), which triggered the partial actin depolymerization necessary for occupancy-elicited phagocytic receptor clustering. TRPV2-deficient macrophages were also defective in chemoattractant-elicited motility. Consequently, TRPV2-deficient mice showed accelerated mortality and greater organ bacterial load when challenged with Listeria monocytogenes. Our data demonstrate the participation of TRPV2 in early phagocytosis and its fundamental importance in innate immunity.

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TRPV2 has a pivotal role in macrophage particle binding and phagocytosis

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