Complement component 3 deficiency prolongs MHC-II disparate skin allograft survival by increasing the CD4+ CD25+ regulatory T cells population

Zheng, Quan‐you; Liang, Shen-Ju; Li, Guiqing; Lv, Yanbo; You, Li; Tang, Ming; Zhang, Kun; Xu, Guiping; Zhang, Ke‐Qin

doi:10.1038/srep33489

Cited by 5 publications

(3 citation statements)

References 48 publications

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“…34 The results of several studies have suggested that complement components (such as C3) are crucial mediators of T cell responses and promote Th1/Th17 differentiation. 35,36 However, the role of C3aR in inflammation has not been investigated. Our current results showed that C3aR knockdown significantly promoted CD4 + cell expression, neutrophil infiltration, and IL-17A-producing γδ-T cells, suggesting that C3aR also…”

Section: Discussionmentioning

confidence: 99%

Activation of the C3a anaphylatoxin receptor inhibits keratinocyte proliferation by regulating keratin 6, keratin 16, and keratin 17 in psoriasis

et al. 2022

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Emerging evidence suggests that signaling through the C3a anaphylatoxin receptor (C3aR) protects against various inflammation‐related diseases. However, the role of C3aR in psoriasis remains unknown. The purpose of this study was to investigate the possible protective role of C3aR in psoriasis and to explore the underlying molecular mechanisms. We initially found that the psoriatic epidermis exhibited significantly decreased C3aR expression. C3aR showed protective roles in mouse models of imiquimod (IMQ)‐ and interleukin‐23‐induced psoriasis. Furthermore, increased epidermal thickness and keratin 6 (K6), K16, and K17 expression occurred in the ears and backs of C3aR−/− mice. Pharmacological treatment with a C3aR agonist ameliorated IMQ‐induced psoriasiform lesions in mice and decreased the expression of K6, K16, and K17. Additionally, the signal transducer and activator of transcription 3 (STAT3) pathway participated in the protective function of C3aR. More importantly, the expression levels of K6, K16, and K17 in keratinocytes were all restored in HaCaT cells transfected with a C3aR‐overexpression plasmid after treating them with colivelin (a STAT3 activator). Our findings demonstrate that C3aR protects against the development of psoriasis and suggest that C3aR confers protection by negatively regulating K6, K16, and K17 expression in a STAT3‐dependent manner, thus inhibiting keratinocyte proliferation and helping reverse the pathogenesis of psoriasis.

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Section: Discussionmentioning

confidence: 99%

Activation of the C3a anaphylatoxin receptor inhibits keratinocyte proliferation by regulating keratin 6, keratin 16, and keratin 17 in psoriasis

et al. 2022

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“…Moreover, the absence of C3aR and C5aR signaling in CD4 + T cells resulted in upregulation of IL‐10, TGF‐β1, and Tregs with immunosuppressive activity, while signaling through C3aR and C5aR on mouse CD4 + FOXP3 + Tregs resulted in suppression of FOXP3 Tregs . Additional studies of Th1/Th17 and Treg response in a mouse model of skin transplantation demonstrated that graft rejection was attenuated by the suppression of Th1/Th17 proinflammatory activity while upregulating the Treg activity, and further deficiency of C3 can delay MHC‐class II‐mismatched skin allograft survival, which is associated with increased Treg and diminished Th1/Th17 balance . These observations concluded that deficiency and inhibition of complement lead to significantly improved tissue oxygenation, subdue pathological airway tissue remodeling, and augment microvascular repair .…”

Section: Complement Factor and T‐regulatory Cell Interactionsmentioning

confidence: 97%

Complement factor and T-cell interactions during alloimmune inflammation in transplantation

Khan

Shamma

2018

Journal of Leukocyte Biology

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Complement factor and T‐cell signaling during an effective alloimmune response plays a key role in transplant‐associated injury, which leads to the progression of chronic rejection (CR). During an alloimmune response, activated complement factors (C3a and C5a) bind to their corresponding receptors (C3aR and C5aR) on a number of lymphocytes, including T‐regulatory cells (Tregs), and these cell‐molecular interactions have been vital to modulate an effective immune response to/from Th1‐effector cell and Treg activities, which result in massive inflammation, microvascular impairments, and fibrotic remodeling. Involvement of the complement‐mediated cell signaling during transplantation signifies a crucial role of complement components as a key therapeutic switch to regulate ongoing inflammatory state, and further to avoid the progression of CR of the transplanted organ. This review highlights the role of complement‐T cell interactions, and how these interactions shunt the effector immune response during alloimmune inflammation in transplantation, which could be a novel therapeutic tool to protect a transplanted organ and avoid progression of CR.

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“…As mentioned above, the complement can also influence the creation of regulatory T-cells ( 11 ). Recent study showed that in C3-deficient mice, the T-cell-mediated rejection of skin grafts was attenuated by the reduction of Th1/Th17 (i.e., pro-inflammatory) T-lymphocyte activity while upregulating the regulatory T-cell expression ( 103 ). Another study reported correlation of regulatory T-cell count and serum C4 levels in patients with systemic lupus erythematosus; according to the results of following in vitro experiment, the C4 component is able to influence the T-cell differentiation in favor of regulatory T-cells in the presence of dendritic cells ( 104 ).…”

Section: Complement and T-cell-mediated Rejectionmentioning

confidence: 99%

Complement in Kidney Transplantation

Cernoch

Viklický

2017

Front. Med.

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The complement system is considered to be an important part of innate immune system with a significant role in inflammation processes. The activation can occur through classical, alternative, or lectin pathway, resulting in the creation of anaphylatoxins C3a and C5a, possessing a vast spectrum of immune functions, and the assembly of terminal complement cascade, capable of direct cell lysis. The activation processes are tightly regulated; inappropriate activation of the complement cascade plays a significant role in many renal diseases including organ transplantation. Moreover, complement cascade is activated during ischemia/reperfusion injury processes and influences delayed graft function of kidney allografts. Interestingly, complement system has been found to play a role in both acute cellular and antibody-mediated rejections and thrombotic microangiopathy. Therefore, complement system may represent an interesting therapeutical target in kidney transplant pathologies.

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Complement component 3 deficiency prolongs MHC-II disparate skin allograft survival by increasing the CD4+ CD25+ regulatory T cells population

Cited by 5 publications

References 48 publications

Activation of the C3a anaphylatoxin receptor inhibits keratinocyte proliferation by regulating keratin 6, keratin 16, and keratin 17 in psoriasis

Activation of the C3a anaphylatoxin receptor inhibits keratinocyte proliferation by regulating keratin 6, keratin 16, and keratin 17 in psoriasis

Complement factor and T-cell interactions during alloimmune inflammation in transplantation

Complement in Kidney Transplantation

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