Bone marrow-derived Ly6C− macrophages promote ischemia-induced chronic kidney disease

Yang, Qian; Wang, Yuxi; Pei, Guangchang; Jiang, Hongyang; Wu, Jianzhong; Zhou, Cheng; Guo, Yi; Yao, Ying; Zeng, Rui; Xu, Gang

doi:10.1038/s41419-019-1531-3

Cited by 48 publications

(61 citation statements)

References 51 publications

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“…Our research team sorted out Ly6C-macrophages in mice kidney at 5 days after IR operation and injected them under the renal capsule of mice with immune deficiency, finding that the original normal kidney showed damage and intrarenal fibrosis 5 days later, suggesting that Ly6C-macrophages directly damaged kidney and induced subsequent fibrosis [38]. We further identified that Ly6C− macrophages were the dominant intrarenal macrophages after ischemia-reperfusion injury, especially at the chronic phase, and most were derived from the bone marrow and depended on intrarenal CX3CL1-CX3CR1 interaction [38].…”

Section: Lvs Serve As a Bridge Between Innate And Adaptive Immunitymentioning

confidence: 99%

Lymphatic Vessels Enhancing Adaptive Immunity Deteriorates Renal Inflammation and Renal Fibrosis

Pei

Zeng

et al. 2020

Kidney Dis

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Background: Lymphatic vessels transport lymph away from microvascular beds into the cardiovascular system. The basic function of the lymphatic system include absorption of wa ter and macromolecules in the interstitial fluid, which plays an important role in maintaining osmotic balance of the body. Recent studies have shown that lymphangiogenesis is associated with tumor metabolism, injury repair, and chron ic inflammation, and deteriorates disease progression via immune cell trafficking. Summary: Renal interstitial lymph angiogenesis is found in patients with chronic kidney dis ease and a series of animal models of renal fibrosis. Lymphat ic vessels transfer antigen and antigenpresenting cells from peripheral tissues to lymph nodes, which initiates adaptive immunity and in turn deteriorates renal inflammation and renal fibrosis, even in nonautoimmune renal diseases. Key Messages: This review summarizes the latest findings on how lymphatics participate in the progression of chronic kid ney disease. This discussion will serve to highlight the role of adaptive immunity in noninfectious and nonautoimmune nephropathy, in order to provide new ideas and methods for prevention and treatment of kidney diseases.

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Section: Lvs Serve As a Bridge Between Innate And Adaptive Immunitymentioning

confidence: 99%

Lymphatic Vessels Enhancing Adaptive Immunity Deteriorates Renal Inflammation and Renal Fibrosis

Pei

Zeng

et al. 2020

Kidney Dis

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“…Whereas a number of studies have claimed that both CSF-1 and -2 drive M2 skewing of Mϕ in mice with AKI (Zhang et al, 2012; Huen et al, 2015; Wang et al, 2015), it was controversially found that IL-34, another ligand for CSF-1R, does not polarize Mϕ in murine AKI (Baek et al, 2015) and lupus model (Wada et al, 2019), indicating that CSF-1R signaling is dispensable in M2 Mϕ polarization. Supportive of this data, other studies have shown that: (1) increased CSF-1 expression in the resolution phase of AKI is not sufficient to prevent Mϕ from M1 polarization when Mϕ are exposed to an M1 stimulus or when they are deprived of an M2 stimulus during AKI (Fujiu et al, 2011; Susnik et al, 2014; Chiba et al, 2016); (2) quiescent and M2 Mϕ in the resolution phase of AKI differ in transcriptional profiles and functions (Lever et al, 2019; Yang et al, 2019); and (3) the sustained blockage of CSF-1R or the constitutive deletion of CSF-1 ameliorates AKI (Lenda et al, 2003; Ma et al, 2009; more discussion in Assessing M ϕ functions by depleting M ϕ section). Nevertheless, what is consistent throughout all studies (Zhang et al, 2012; Baek et al, 2015; Huen et al, 2015; Wang et al, 2015; Chiba et al, 2016) is that the deficiency in Mϕ survival factors reduces the number of Mϕ (including that of M2 Mϕ predominating in the resolution phase of AKI).…”

Section: Mϕ In Akimentioning

confidence: 77%

“…The migration of Ly6C high monocytes to the site of inflammation occurs through chemotactic mechanisms (e.g., via CCR2 and CX 3 CR1). Therefore, deletion or blockage of chemotaxis receptors on monocytes is found to be protective against ischemia-induced AKI in mice (Furuichi et al, 2003; Li et al, 2008; Lu et al, 2008; Oh et al, 2008; Yang et al, 2019). Monocyte infiltration occurs in the first 48 h (Lu et al, 2008) and completely ceases before day 3 of AKI.…”

Section: Mϕ In Akimentioning

confidence: 99%

“…Several studies have shown that monocyte-derived Ly6C int and Ly6C low Mϕ populations display transcriptionally and functionally distinct M2 phenotypes, both implicated in immunosuppression and tissue regeneration. In the later stages of AKI, Ly6C low Mϕ predominate over Ly6C int Mϕ and are found to promote interstitial fibrosis (Lin et al, 2009; Clements et al, 2016; Lever et al, 2019; Yang et al, 2019) (Figure 4). More recent studies revealed that quiescent tissue-resident Mϕ remain in the tissue independently of monocyte-derived Ly6C low Mϕ (Lin et al, 2009; Zhang et al, 2012; Lever et al, 2019) and are reprogramed in AKI toward a developmental state resembling perinatal Mϕ (Schulz et al, 2012; Mass et al, 2016), which are implicated in early kidney development (Lever et al, 2019).…”

Section: Mϕ In Akimentioning

confidence: 99%

“…However, it is to note that M2 Mϕ are considered to be instrumental in the development of pathological fibrosis and the progression of CKD (Duffield, 2010; Anders and Ryu, 2011). Especially, several studies have identified monocyte-derived Ly6C low Mϕ, which predominate over Ly6C int Mϕ in the later stages of AKI, as direct or indirect contributors to interstitial fibrosis (Lin et al, 2009; Anders and Ryu, 2011; Clements et al, 2016; Lever et al, 2019; Yang et al, 2019) and as a hallmark of CKD progression post-AKI. In line with this, CX 3 CL1-CX 3 CR1-mediated survival of Ly6C low Mϕ correlates with interstitial fibrosis in obstructed kidneys (Peng et al, 2015).…”

Section: Mϕ In Akimentioning

confidence: 99%

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The Impact of Versatile Macrophage Functions on Acute Kidney Injury and Its Outcomes

Baek

2019

Front. Physiol.

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Acute kidney injury (AKI) is a common and devastating clinical condition with a high morbidity and mortality rate and is associated with a rapid decline of kidney function mostly resulting from the injury of proximal tubules. AKI is typically accompanied by inflammation and immune activation and involves macrophages (Mϕ) from the beginning: The inflamed kidney recruits “classically” activated (M1) Mϕ, which are initially poised to destroy potential pathogens, exacerbating inflammation. Of note, they soon turn into “alternatively” activated (M2) Mϕ and promote immunosuppression and tissue regeneration. Based on their roles in kidney recovery, there is a growing interest to use M2 Mϕ and Mϕ-modulating agents therapeutically against AKI. However, it is pertinent to note that the clinical translation of Mϕ-based therapies needs to be critically reviewed and questioned since Mϕ are functionally plastic with versatile roles in AKI and some Mϕ functions are detrimental to the kidney during AKI. In this review, we discuss the current state of knowledge on the biology of different Mϕ subtypes during AKI and, especially, on their role in AKI and assess the impact of versatile Mϕ functions on AKI based on the findings from translational AKI studies.

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Interleukin‐2/anti‐interleukin‐2 immune complex attenuates cold ischemia‐reperfusion injury after kidney transplantation by increasing renal regulatory T cells

Jang,

Kim,

Yan

et al. 2024

Clinical & Translational Med

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BackgroundCold ischemia‐reperfusion injury (IRI) is an unavoidable complication of kidney transplantation. We investigated the role of regulatory T cells (Treg) in cold IRI and whether the interleukin (IL)‐2/anti‐IL‐2 antibody complex (IL‐2C) can ameliorate cold IRI.MethodsWe developed a cold IRI mouse model using kidney transplantation and analyzed the IL‐2C impact on cold IRI in acute, subacute and chronic phases.ResultsTreg transfer attenuated cold IRI, while Treg depletion aggravated cold IRI. Next, IL‐2C administration prior to IRI mitigated acute renal function decline, renal tissue damage and apoptosis and inhibited infiltration of effector cells into kidneys and pro‐inflammatory cytokine expression on day 1 after IRI. On day 7 after IRI, IL‐2C promoted renal regeneration and reduced subacute renal damage. Furthermore, on day 28 following IRI, IL‐2C inhibited chronic fibrosis. IL‐2C decreased reactive oxygen species‐mediated injury and improved antioxidant function. When IL‐2C was administered following IRI, it also increased renal regeneration with Treg infiltration and suppressed renal fibrosis. In contrast, Treg depletion in the presence of IL‐2C eliminated the positive effects of IL‐2C on IRI.ConclusionTregs protect kidneys from cold IRI and IL‐2C inhibited cold IRI by increasing the renal Tregs, suggesting a potential of IL‐2C in treating cold IRI.Key Points Interleukin (IL)‐2/anti‐IL‐2 antibody complex attenuated acute renal injury, facilitated subacute renal regeneration and suppressed chronic renal fibrosis after cold ischemia‐reperfusion injury (IRI) by increasing the renal Tregs. IL‐2/anti‐IL‐2 antibody complex decreased reactive oxygen species‐mediated injury and improved antioxidant function. This study suggests the therapeutic potential of the IL‐2/anti‐IL‐2 antibody complex in kidney transplantation‐associated cold IR.

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Bone marrow-derived Ly6C− macrophages promote ischemia-induced chronic kidney disease

Cited by 48 publications

References 51 publications

Lymphatic Vessels Enhancing Adaptive Immunity Deteriorates Renal Inflammation and Renal Fibrosis

Lymphatic Vessels Enhancing Adaptive Immunity Deteriorates Renal Inflammation and Renal Fibrosis

The Impact of Versatile Macrophage Functions on Acute Kidney Injury and Its Outcomes

Interleukin‐2/anti‐interleukin‐2 immune complex attenuates cold ischemia‐reperfusion injury after kidney transplantation by increasing renal regulatory T cells

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