Blockade of CCR2 Ameliorates Progressive Fibrosis in Kidney

Kitagawa, Kiyoki; Wada, Takashi; Furuichi, Kengo; Hashimoto, Hiroyuki; Ishiwata, Yoichi; Asano, Masahide; Takeya, Motohiro; Kuziel, William A.; Matsushima, Kouji; Mukaida, Naofumi; Yokoyama, Hitoshi

doi:10.1016/s0002-9440(10)63292-0

Cited by 296 publications

(259 citation statements)

References 37 publications

(41 reference statements)

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“…1) because it has been previously reported that renal macrophages but not DCs mediate fibrosis in this model (16,18,66). However, Cx 3 cr1 GFP/GFP mice possessed similar or lower numbers of GFP + renal phagocytes under homeostatic conditions, in experimental glomerulonephritis and in kidney infection compared with CX 3 CR1-competent controls (3, 58), consistent with our present findings in UUO ( Fig.…”

Section: Cx3cr1 Deficiency Enhances Renal Fibrosissupporting

confidence: 91%

“…In contrast, inappropriate macrophage functions promoted fibrosis in various organs (13,14). In the kidney, macrophages but not DCs mediated fibrosis in unilateral ureter ligation (UUO) and after ischemia/reperfusion (15)(16)(17)(18). Several mechanisms contribute to renal fibrosis, including the production of the main profibrotic molecule TGF-b (14,19).…”

mentioning

confidence: 99%

“…Inflammatory Gr1 + macrophages possess profibrotic properties (42), and their depletion or genetic CCR2 deficiency attenuated tissue damage and fibrosis in UUO (16), lupus nephritis (43), and ischemia/ reperfusion (44). Also, CX 3 CR1 has been implicated in monocyte recruitment into inflamed tissues, like arteriosclerotic vessels (45), the listeria-infected spleen (46), the eye (47), in colitis models (28), or the skin (48).…”

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confidence: 99%

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CX3CR1 Reduces Kidney Fibrosis by Inhibiting Local Proliferation of Profibrotic Macrophages

Engel

Krause

Snelgrove

et al. 2015

The Journal of Immunology

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A dense network of macrophages and dendritic cells (DC) expressing the chemokine receptor CX3CR1 populates most tissues. We recently reported that CX3CR1 regulates the abundance of CD11c+ DC in the kidney and thereby promotes renal inflammation in glomerulonephritis. Given that chronic inflammation usually causes fibrosis, we hypothesized that CX3CR1 deficiency should attenuate renal fibrosis. However, when we tested this hypothesis using the DC-independent murine fibrosis model of unilateral ureteral obstruction, kidney fibrosis was unexpectedly more severe, despite less intrarenal inflammation. Two-photon imaging and flow cytometry revealed in kidneys of CX3CR1-deficient mice more motile Ly6C/Gr-1+ macrophages. Flow cytometry verified that renal macrophages were more abundant in the absence of CX3CR1 and produced more of the key profibrotic mediator, TGF-β. Macrophages accumulated because of higher intrarenal proliferation, despite reduced monocyte recruitment and higher signs of apoptosis within the kidney. These findings support the theory that tissue macrophage numbers are regulated through local proliferation and identify CX3CR1 as a regulator of such proliferation. Thus, CX3CR1 inhibition should be avoided in DC-independent inflammatory diseases because it may promote fibrosis.

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Section: Cx3cr1 Deficiency Enhances Renal Fibrosissupporting

confidence: 91%

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confidence: 99%

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confidence: 99%

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CX3CR1 Reduces Kidney Fibrosis by Inhibiting Local Proliferation of Profibrotic Macrophages

Engel

Krause

Snelgrove

et al. 2015

The Journal of Immunology

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“…Especially, the severity of interstitial fibrosis has been reported to determine the prognosis of kidney function [2]. To date, resident fibroblasts, epithelial-mesenchymal transition (EMT)-derived fibroblasts/myofibroblasts, and monocytes/macrophages have been suggested to be involved in the progression of kidney diseases [3,4]. However, the precise pathogenic mechanisms of tubulointerstitial lesions, especially related to interstitial fibrosis, in patients with CKD remain to be determined.…”

Section: Introductionmentioning

confidence: 99%

Fibrocytes are involved in the pathogenesis of human chronic kidney disease

et al. 2010

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“…Likewise, cross-linking of myeloid IgA Fc receptors (Fc␣RI or CD89) aggravates IgA nephropathy and anti-GBM nephritis in an FcR␥-dependent manner (10). Macrophages and T cells are important in the inflammation associated with ureteral obstruction, another common cause of ESRD (11)(12)(13)(14)(15)(16). Conventional antiinflammatory therapy for ESRD, based on steroids, immunosuppressants, and angiotensin-converting enzyme inhibitors have limited efficacy on disease progression (17).…”

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confidence: 99%

Inhibitory ITAM Signaling by FcαRI-FcRγ Chain Controls Multiple Activating Responses and Prevents Renal Inflammation

Kanamaru

Pfirsch

Aloulou

et al. 2008

The Journal of Immunology

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Inhibitory signaling is an emerging function of ITAM-bearing immunoreceptors in the maintenance of homeostasis. Monovalent targeting of the IgA Fc receptor (FcαRI or CD89) by anti-FcαRI Fab triggers potent inhibitory ITAM (ITAMi) signaling through the associated FcRγ chain (FcαRI-FcRγ ITAMi) that prevents IgG phagocytosis and IgE-mediated asthma. It is not known whether FcαRI-FcRγ ITAMi signaling controls receptors that do not function through an ITAM and whether this inhibition requires Src homology protein 1 phosphatase. We show in this study that FcαRI-Fcγ ITAMi signals depend on Src homology protein 1 phosphatase to target multiple non-ITAM-bearing receptors such as chemotactic receptors, cytokine receptors, and TLRs. We found that anti-FcαRI Fab treatment in vivo reduced kidney inflammation in models of immune-mediated glomerulonephritis and nonimmune obstructive nephropathy by a mechanism that involved decreased inflammatory cell infiltration and fibrosis development. This treatment also prevented ex vivo LPS activation of monocytes from patients with lupus nephritis or vasculitis, as well as receptor activation through serum IgA complexes from IgA nephropathy patients. These findings point to a crucial role of FcαRI-FcRγ ITAMi signaling in the control of multiple heterologous or autologous inflammatory responses. They also identify anti-FcαRI Fab as a new potential therapeutic tool for preventing progression of renal inflammatory diseases.

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Blockade of CCR2 Ameliorates Progressive Fibrosis in Kidney

Cited by 296 publications

References 37 publications

CX3CR1 Reduces Kidney Fibrosis by Inhibiting Local Proliferation of Profibrotic Macrophages

CX3CR1 Reduces Kidney Fibrosis by Inhibiting Local Proliferation of Profibrotic Macrophages

Fibrocytes are involved in the pathogenesis of human chronic kidney disease

Inhibitory ITAM Signaling by FcαRI-FcRγ Chain Controls Multiple Activating Responses and Prevents Renal Inflammation

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