CSF-1 receptor-mediated differentiation of a new type of monocytic cell with B cell-stimulating activity: its selective dependence on IL-34

Yamane, Fumihiro; Nishikawa, Yumiko; Matsui, Kazue; Asakura, Miki; Iwasaki, Eriko; Watanabe, Kôji; Tanimoto, Hirokazu; Sano, Hiroki; Fujiwara, Yuki; Stanley, E. Richard; Kanayama, Naoki; Mabbott, Neil A.; Ohmori, Hitoshi

doi:10.1189/jlb.0613311

Cited by 28 publications

(34 citation statements)

References 52 publications

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“…In addition to the already identified functions of IL-34 and M-CSF in exacerbated macrophage activation (bowel diseases, liver fibrosis, chronic skin inflammation, arthritis, etc. ), this new heteromeric cytokine M-CSF/IL-34 which may differentially regulates the activation/localization of M-CSFR strengthens the global therapeutic approaches for blocking all biological functions coming from these molecules [7,8,[45][46][47][48][49][50][51].…”

Section: Discussionmentioning

confidence: 83%

IL-34 and M-CSF form a novel heteromeric cytokine and regulate the M-CSF receptor activation and localization

et al. 2015

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Section: Discussionmentioning

confidence: 83%

IL-34 and M-CSF form a novel heteromeric cytokine and regulate the M-CSF receptor activation and localization

et al. 2015

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“…Although CSF1 and IL-34 are both CSF1R ligands, they have been shown to activate biologically distinct signaling in vitro (31,32). Therefore, to identify the relevant CSF1R ligand(s) in human high-grade gliomas, mRNA expression array data at www.oncomine.org was mined.…”

Section: Resultsmentioning

confidence: 99%

CSF1 Overexpression Promotes High-Grade Glioma Formation without Impacting the Polarization Status of Glioma-Associated Microglia and Macrophages

Steffen

Clark

et al. 2016

Cancer Research

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Current therapies for high-grade gliomas extend survival only modestly. The glioma microenvironment, including glioma-associated microglia/macrophages (GAMs), is a potential therapeutic target. The microglia/macrophage cytokine CSF1 and its receptor CSF1R are overexpressed in human high-grade gliomas. To determine if the other known CSF1R ligand IL-34 is expressed in gliomas, we examined expression array data of human high-grade gliomas and performed RT-PCR on glioblastoma sphere-forming cell lines (GSCs). Expression microarray analyses indicated that CSF1, but not IL-34, is frequently overexpressed in human tumors. We found that while GSCs did express CSF1, most GSC lines did not express detectable levels of IL-34 mRNA. We therefore studied the impact of modulating CSF1 levels on gliomagenesis in the context of the GFAP-V12Ha-ras-IRESLacZ (Ras*) model. Csf1 deficiency deterred glioma formation in the Ras* model while CSF1 transgenic overexpression decreased the survival of Ras* mice and promoted the formation of high-grade gliomas. Conversely, CSF1 overexpression increased GAM density, but did not impact GAM polarization state. Regardless of CSF1 expression status, most GAMs were negative for the M2 polarization markers ARG1 and CD206; when present, ARG1+ and CD206+ cells were found in regions of peripheral immune cell invasion. Therefore, our findings indicate that CSF1 signaling is oncogenic during gliomagenesis through a mechanism distinct from modulating GAM polarization status.

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“…Furthermore, the congenital absence of CSF-1 is not equivalent to inhibition of the CSF-1R. The CSF-1R has a second ligand, IL-34, which has unique roles in the regulation of monocyte/macrophage populations [37]. Thus, in the CSF-1 or CSF-1R knockout strains reported previously, nephritis may have been attenuated because it developed on an altered background, preventing the conclusive determination of the therapeutic efficacy of suppressing CSF-1R in lupus.…”

Section: Discussionmentioning

confidence: 99%

Macrophage depletion ameliorates nephritis induced by pathogenic antibodies

Chalmers

Chiţu

Herlitz

et al. 2015

Journal of Autoimmunity

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Objective Kidney involvement affects 40–60% of patients with lupus and is responsible for significant morbidity and mortality. Using depletion approaches, several studies have suggested that macrophages may play a key role in the pathogenesis of lupus nephritis. However, “off target” effects of macrophage depletion, such as altered hematopoiesis or enhanced autoantibody production, impeded the determination of a conclusive relationship. Methods In this study, we investigated the role of macrophages in mice receiving rabbit anti-glomerular antibodies, or nephrotoxic serum (NTS), an experimental model which closely mimics the immune complex mediated disease seen in murine and human lupus nephritis. GW2580, a selective inhibitor of the colony stimulating factor-1 (CSF-1) receptor kinase, was used for macrophage depletion. Results We found that GW2580-treated, NTS challenged mice did not develop the increased levels of proteinuria, serum creatinine, or serum urea seen in control-treated, NTS challenged mice. NTS challenged mice exhibited significantly increased kidney expression of inflammatory cytokines including RANTES, IP-10, VCAM-1 and iNOS, whereas GW2580-treated mice were protected from the robust expression of these inflammatory cytokines that are associated with LN. Quantification of macrophage related gene expression, flow cytometry analysis of kidney single cell suspensions, and immunofluorescence staining confirmed the depletion of macrophages in GW2580-treated mice, specifically within renal glomeruli. Conclusions Our results strongly implicate a specific and necessary role for macrophages in the development of immune glomerulonephritis mediated by pathogenic antibodies, and support the development of macrophage targeting approaches for the treatment of lupus nephritis.

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CSF-1 receptor-mediated differentiation of a new type of monocytic cell with B cell-stimulating activity: its selective dependence on IL-34

Cited by 28 publications

References 52 publications

IL-34 and M-CSF form a novel heteromeric cytokine and regulate the M-CSF receptor activation and localization

IL-34 and M-CSF form a novel heteromeric cytokine and regulate the M-CSF receptor activation and localization

CSF1 Overexpression Promotes High-Grade Glioma Formation without Impacting the Polarization Status of Glioma-Associated Microglia and Macrophages

Macrophage depletion ameliorates nephritis induced by pathogenic antibodies

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