The roles of complement receptor 3 and Fcγ receptors during Leishmania phagosome maturation

Rachel Polando; Upasna Gaur Dixit; Cristina R. Carter; Blake Jones; James P. Whitcom; Wibke Ballhorn; Melissa Harintho; Christopher L. Jerde; Mary E. Wilson; Mary Ann McDowell

doi:10.1189/jlb.0212086

The roles of complement receptor 3 and Fcγ receptors during Leishmania phagosome maturation

Rachel Polando, Upasna Gaur Dixit, Cristina R. Carter, Blake Jones, James P. Whitcom, Wibke Ballhorn, Melissa Harintho, Christopher L. Jerde, Mary E. Wilson, Mary Ann McDowell

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

18 Scopus citations

Abstract

Leishmania are intracellular parasites adapted to surviving in macrophages, whose primary function is elimination of invading pathogens. Leishmania entry into host cells is receptor-mediated. These parasites are able to engage multiple host cell-surface receptors, including MR, TLRs, CR3, and FcγRs. Here, we investigated the role of CR3 and FcγR engagement on the maturation of Leishmania-containing phagosomes using CD11b-/- and FcγR-/- macrophages, and assessing EEA1 and lysosome-associated proteins is necessary for the phagosome maturation delay, characteristic of Leishmania infection. Leishmania-containing phagosomes do not fuse with lyosomes until 5 h postinfection in WT mice. Phagolysosome fusion occurs by 1 h in CD11b and FcγR common chain KO macrophages, although receptor deficiency does not influence Leishmania entry or viability. We also investigated the influence of serum components and their effects on phagosome maturation progression. Opsonization with normal mouse serum, complement-deficient serum, or serum from Leishmania-infected mice all influenced phagosome maturation progression. Our results indicate that opsonophagocytosis influences phagosomal trafficking of Leishmania without altering the intracellular fate.

Original language	English (US)
Pages (from-to)	921-932
Number of pages	12
Journal	Journal of Leukocyte Biology
Volume	93
Issue number	6
DOIs	https://doi.org/10.1189/jlb.0212086
State	Published - Jun 1 2013
Externally published	Yes

Keywords

CD11b
Deficient
EEA1
LAMP1
Mannose receptor

ASJC Scopus subject areas

Immunology and Allergy
Immunology
Cell Biology

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10.1189/jlb.0212086

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title = "The roles of complement receptor 3 and Fcγ receptors during Leishmania phagosome maturation",

abstract = "Leishmania are intracellular parasites adapted to surviving in macrophages, whose primary function is elimination of invading pathogens. Leishmania entry into host cells is receptor-mediated. These parasites are able to engage multiple host cell-surface receptors, including MR, TLRs, CR3, and FcγRs. Here, we investigated the role of CR3 and FcγR engagement on the maturation of Leishmania-containing phagosomes using CD11b-/- and FcγR-/- macrophages, and assessing EEA1 and lysosome-associated proteins is necessary for the phagosome maturation delay, characteristic of Leishmania infection. Leishmania-containing phagosomes do not fuse with lyosomes until 5 h postinfection in WT mice. Phagolysosome fusion occurs by 1 h in CD11b and FcγR common chain KO macrophages, although receptor deficiency does not influence Leishmania entry or viability. We also investigated the influence of serum components and their effects on phagosome maturation progression. Opsonization with normal mouse serum, complement-deficient serum, or serum from Leishmania-infected mice all influenced phagosome maturation progression. Our results indicate that opsonophagocytosis influences phagosomal trafficking of Leishmania without altering the intracellular fate.",

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author = "Rachel Polando and Dixit, {Upasna Gaur} and Carter, {Cristina R.} and Blake Jones and Whitcom, {James P.} and Wibke Ballhorn and Melissa Harintho and Jerde, {Christopher L.} and Wilson, {Mary E.} and McDowell, {Mary Ann}",

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AU - Dixit, Upasna Gaur

AU - Carter, Cristina R.

AU - Jones, Blake

AU - Whitcom, James P.

AU - Ballhorn, Wibke

AU - Harintho, Melissa

AU - Jerde, Christopher L.

AU - Wilson, Mary E.

AU - McDowell, Mary Ann

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N2 - Leishmania are intracellular parasites adapted to surviving in macrophages, whose primary function is elimination of invading pathogens. Leishmania entry into host cells is receptor-mediated. These parasites are able to engage multiple host cell-surface receptors, including MR, TLRs, CR3, and FcγRs. Here, we investigated the role of CR3 and FcγR engagement on the maturation of Leishmania-containing phagosomes using CD11b-/- and FcγR-/- macrophages, and assessing EEA1 and lysosome-associated proteins is necessary for the phagosome maturation delay, characteristic of Leishmania infection. Leishmania-containing phagosomes do not fuse with lyosomes until 5 h postinfection in WT mice. Phagolysosome fusion occurs by 1 h in CD11b and FcγR common chain KO macrophages, although receptor deficiency does not influence Leishmania entry or viability. We also investigated the influence of serum components and their effects on phagosome maturation progression. Opsonization with normal mouse serum, complement-deficient serum, or serum from Leishmania-infected mice all influenced phagosome maturation progression. Our results indicate that opsonophagocytosis influences phagosomal trafficking of Leishmania without altering the intracellular fate.

AB - Leishmania are intracellular parasites adapted to surviving in macrophages, whose primary function is elimination of invading pathogens. Leishmania entry into host cells is receptor-mediated. These parasites are able to engage multiple host cell-surface receptors, including MR, TLRs, CR3, and FcγRs. Here, we investigated the role of CR3 and FcγR engagement on the maturation of Leishmania-containing phagosomes using CD11b-/- and FcγR-/- macrophages, and assessing EEA1 and lysosome-associated proteins is necessary for the phagosome maturation delay, characteristic of Leishmania infection. Leishmania-containing phagosomes do not fuse with lyosomes until 5 h postinfection in WT mice. Phagolysosome fusion occurs by 1 h in CD11b and FcγR common chain KO macrophages, although receptor deficiency does not influence Leishmania entry or viability. We also investigated the influence of serum components and their effects on phagosome maturation progression. Opsonization with normal mouse serum, complement-deficient serum, or serum from Leishmania-infected mice all influenced phagosome maturation progression. Our results indicate that opsonophagocytosis influences phagosomal trafficking of Leishmania without altering the intracellular fate.

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The roles of complement receptor 3 and Fcγ receptors during Leishmania phagosome maturation

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