Nitric oxide-mediated tumoricidal activity of murine microglial cells

Emily C. Brantley; Lixia Guo; Chenyu Zhang; Qingtang Lin; Kenji Yokoi; Robert R. Langley; Ewa Kruzel; Marva Maya; Seung Wook Kim; Sun Jin Kim; Dominic Fan; Isaiah J. Fidler

doi:10.1593/tlo.10208

Nitric oxide-mediated tumoricidal activity of murine microglial cells

Emily C. Brantley, Lixia Guo, Chenyu Zhang, Qingtang Lin, Kenji Yokoi, Robert R. Langley, Ewa Kruzel, Marva Maya, Seung Wook Kim, Sun Jin Kim, Dominic Fan, Isaiah J. Fidler

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

65 Scopus citations

Abstract

Experimental metastases in the brain of mice are infiltrated by microglia, and parabiosis experiments of green fluorescent protein (GFP⁺) and GFP^- mice revealed that these microglia are derived from circulating monocytes (GFP⁺, F4/80⁺, and CD68⁺). These findings raised the question as to whether microglia (specialized macrophages) possess tumoricidal activity. C8-B4 murine microglia cells were incubated in vitro in medium (control) or in medium containing both lipopolysaccharide and interferon-γ. Control microgliawere not tumoricidal against a number ofmurine and human tumor cells, whereas lipopolysaccharide/interferon-γ-activated microglia lysed murine and human tumor cells by release of nitric oxide. Parallel experiments with murine peritoneal macrophages produced identical results. Neither activated microglia nor activated macrophages lysed nontumorigenic murine or human cells. Collectively, these data demonstrate that brain metastasis-associated microglia are derived from circulating mononuclear cells and exhibit selective and specific tumoricidal activity.

Original language	English (US)
Pages (from-to)	380-388
Number of pages	9
Journal	Translational Oncology
Volume	3
Issue number	6
DOIs	https://doi.org/10.1593/tlo.10208
State	Published - Dec 2010

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1593/tlo.10208

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title = "Nitric oxide-mediated tumoricidal activity of murine microglial cells",

abstract = "Experimental metastases in the brain of mice are infiltrated by microglia, and parabiosis experiments of green fluorescent protein (GFP+) and GFP- mice revealed that these microglia are derived from circulating monocytes (GFP+, F4/80+, and CD68+). These findings raised the question as to whether microglia (specialized macrophages) possess tumoricidal activity. C8-B4 murine microglia cells were incubated in vitro in medium (control) or in medium containing both lipopolysaccharide and interferon-γ. Control microgliawere not tumoricidal against a number ofmurine and human tumor cells, whereas lipopolysaccharide/interferon-γ-activated microglia lysed murine and human tumor cells by release of nitric oxide. Parallel experiments with murine peritoneal macrophages produced identical results. Neither activated microglia nor activated macrophages lysed nontumorigenic murine or human cells. Collectively, these data demonstrate that brain metastasis-associated microglia are derived from circulating mononuclear cells and exhibit selective and specific tumoricidal activity.",

author = "Brantley, {Emily C.} and Lixia Guo and Chenyu Zhang and Qingtang Lin and Kenji Yokoi and Langley, {Robert R.} and Ewa Kruzel and Marva Maya and Kim, {Seung Wook} and Kim, {Sun Jin} and Dominic Fan and Fidler, {Isaiah J.}",

note = "Funding Information: Address all correspondence to: Isaiah J. Fidler, DVM, PhD, Department of Cancer Biology, Cancer Metastasis Research Center, The University of Texas MD Anderson Cancer Center, Unit 854, 1515 Holcombe Blvd, Houston, TX 77030. E-mail: ifidler@mdanderson.org 1This work was supported in part by Cancer Center Support Core grants CA16672 and 1U54CA143837 from the National Cancer Institute, National Institutes of Health. 2There is no conflict of interest with any author or product used in this translational research study. 3These authors contributed equally to this work. 4Current address: Department of Molecular and Cellular Oncology, The University of Texas MD Anderson Cancer Center, Houston, TX. Received 26 July 2010; Revised 16 August 2010; Accepted 18 August 2010 Copyright {\textcopyright} 2010 Neoplasia Press, Inc. All rights reserved 1944-7124/10/$25.00 DOI 10.1593/tlo.10208",

year = "2010",

month = dec,

doi = "10.1593/tlo.10208",

language = "English (US)",

volume = "3",

pages = "380--388",

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T1 - Nitric oxide-mediated tumoricidal activity of murine microglial cells

AU - Brantley, Emily C.

AU - Guo, Lixia

AU - Zhang, Chenyu

AU - Lin, Qingtang

AU - Yokoi, Kenji

AU - Langley, Robert R.

AU - Kruzel, Ewa

AU - Maya, Marva

AU - Kim, Seung Wook

AU - Kim, Sun Jin

AU - Fan, Dominic

AU - Fidler, Isaiah J.

N1 - Funding Information: Address all correspondence to: Isaiah J. Fidler, DVM, PhD, Department of Cancer Biology, Cancer Metastasis Research Center, The University of Texas MD Anderson Cancer Center, Unit 854, 1515 Holcombe Blvd, Houston, TX 77030. E-mail: ifidler@mdanderson.org 1This work was supported in part by Cancer Center Support Core grants CA16672 and 1U54CA143837 from the National Cancer Institute, National Institutes of Health. 2There is no conflict of interest with any author or product used in this translational research study. 3These authors contributed equally to this work. 4Current address: Department of Molecular and Cellular Oncology, The University of Texas MD Anderson Cancer Center, Houston, TX. Received 26 July 2010; Revised 16 August 2010; Accepted 18 August 2010 Copyright © 2010 Neoplasia Press, Inc. All rights reserved 1944-7124/10/$25.00 DOI 10.1593/tlo.10208

PY - 2010/12

Y1 - 2010/12

N2 - Experimental metastases in the brain of mice are infiltrated by microglia, and parabiosis experiments of green fluorescent protein (GFP+) and GFP- mice revealed that these microglia are derived from circulating monocytes (GFP+, F4/80+, and CD68+). These findings raised the question as to whether microglia (specialized macrophages) possess tumoricidal activity. C8-B4 murine microglia cells were incubated in vitro in medium (control) or in medium containing both lipopolysaccharide and interferon-γ. Control microgliawere not tumoricidal against a number ofmurine and human tumor cells, whereas lipopolysaccharide/interferon-γ-activated microglia lysed murine and human tumor cells by release of nitric oxide. Parallel experiments with murine peritoneal macrophages produced identical results. Neither activated microglia nor activated macrophages lysed nontumorigenic murine or human cells. Collectively, these data demonstrate that brain metastasis-associated microglia are derived from circulating mononuclear cells and exhibit selective and specific tumoricidal activity.

AB - Experimental metastases in the brain of mice are infiltrated by microglia, and parabiosis experiments of green fluorescent protein (GFP+) and GFP- mice revealed that these microglia are derived from circulating monocytes (GFP+, F4/80+, and CD68+). These findings raised the question as to whether microglia (specialized macrophages) possess tumoricidal activity. C8-B4 murine microglia cells were incubated in vitro in medium (control) or in medium containing both lipopolysaccharide and interferon-γ. Control microgliawere not tumoricidal against a number ofmurine and human tumor cells, whereas lipopolysaccharide/interferon-γ-activated microglia lysed murine and human tumor cells by release of nitric oxide. Parallel experiments with murine peritoneal macrophages produced identical results. Neither activated microglia nor activated macrophages lysed nontumorigenic murine or human cells. Collectively, these data demonstrate that brain metastasis-associated microglia are derived from circulating mononuclear cells and exhibit selective and specific tumoricidal activity.

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Nitric oxide-mediated tumoricidal activity of murine microglial cells

Abstract

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