The Protective Role of CD59 and Pathogenic Role of Complement in Hepatic Ischemia and Reperfusion Injury

Zhang, Jinyan; Hu, Weiguo; Xing, Wei; You, Tao; Xu, Junming; Qin, Xuebin; Peng, Zhihai

doi:10.1016/j.ajpath.2011.08.040

Cited by 28 publications

(20 citation statements)

References 62 publications

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“…Transplantation of kidneys from C3-deficient donors resulted in an increased rejection free survival supporting a role for donor-derived C3 in murine transplant rejection [16]. These models illustrate how complement damages the renal parenchyma directly and indirectly by enhancing the recipient's T cell response in a C3 dependent manner [31,47]. A similar phenomenon is reported in cardiac transplants with activation of the classical and alternative pathways via inhibition of the complement regulator CD55 [70][71][72].…”

Section: Kidney Transplant Rejection 221 Cell-mediated Allograft Rementioning

confidence: 51%

“…This has been found in studies of complement deficient and depleted mice that are protected against reperfusion damage [30,31,33,34]. C5a acts directly on the C5a receptor on parenchymal cells, as well as stimulating chemotaxis and degranulation of neutrophils [35,36].…”

Section: Ischaemia-reperfusion Injurymentioning

confidence: 95%

“…This induces cellular inflammation via toll-like receptors, cytokines, chemokines and complement. Complement activation both initiates and propagates tissue damage not only in kidney transplantation but also in other major transplanted organs such as the heart, lung, liver and pancreas [27][28][29][30][31][32]. The classical pathway is triggered by the C1 complex (C1q, C1r, C1s) binding to antibody or C-reactive protein on the activating surface, leading to the formation of the classical pathway C3 convertase from C4 and C2 (C4bC2a) and to subsequent cleavage of C3.…”

Section: Ischaemia-reperfusion Injurymentioning

confidence: 99%

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Complement—here, there and everywhere, but what about the transplanted organ?

Montero

Sacks

Smith

2016

Seminars in Immunology

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The part of the innate immune system that communicates and effectively primes the adaptive immune system was termed "complement" by Ehrlich to reflect its complementarity to antibodies having previously been described as "alexine" (i.e protective component of serum) by Buchner and Bordet. It has been established that complement is not solely produced systemically but may have origin in different tissues where it can influence organ specific functions that may affect the outcome of transplanted organs. This review looks at the role of complement in particular to kidney transplantation. We look at current literature to determine whether blockade of the peripheral or central compartments of complement production may prevent ischaemic reperfusion injury or rejection in the transplanted organ.We also review new therapeutics that have been developed to inhibit components of the complement cascade with varying degrees of success leading to an increase in our understanding of the multiple triggers of this complex system. In addition, we consider whether biomarkers in this field are effective markers of disease or treatment. Word count 169

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Section: Kidney Transplant Rejection 221 Cell-mediated Allograft Rementioning

confidence: 51%

Section: Ischaemia-reperfusion Injurymentioning

confidence: 95%

Section: Ischaemia-reperfusion Injurymentioning

confidence: 99%

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Complement—here, there and everywhere, but what about the transplanted organ?

Montero

Sacks

Smith

2016

Seminars in Immunology

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“…This indicates that whereas the anaphylatoxins may contribute to IRI, likely via the recruitment and/or activation of leukocytes, other operative mechanisms that are not affected by C3aR/C5aR deficiency, namely C3 opsonins and/or the MAC, play a prominent role in VCA IRI. Indeed, in some solid organs the MAC appears to be the primary mediator of IRI 31–34 . In addition to being directly cytolytic, deposition of the MAC at sublytic concentrations can, as can the anaphylatoxins, result in the activation of endothelial cells, expression of adhesion molecules, and the recruitment and activation of leukocytes 35,36 .…”

Section: Discussionmentioning

confidence: 99%

Targeted Complement Inhibition Protects Vascularized Composite Allografts From Acute Graft Injury and Prolongs Graft Survival When Combined With Subtherapeutic Cyclosporine A Therapy

et al. 2017

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Background Recipients of vascularized composite allografts require aggressive and life-long immunosuppression, and since the surgery is usually performed in nonlife threatening situations, the development of strategies to minimize immunosuppression is especially pertinent for this procedure. We investigated how complement affects acute graft injury, alloimmunity, and immunosuppressive therapy. Methods Vascularized composite allografts were transplanted from Balb/C to C57BL/6 mice that were complement deficient (C3 or double C3a Receptor (R)/C5aR), or treated with a targeted complement inhibitor (CR2-Crry). Allografts were analyzed for acute inflammation and injury, subacute T cell response, and survival in the absence and presence of CsA therapy. Results Allografts in C3-deficient or CR2-Crry treated recipients were protected from skin and muscle ischemia reperfusion injury (IRI). C3aR/C5aR deficient recipients were more modestly protected. IgM and C3d colocalized within allografts from wild type and C3aR/C5aR-deficient recipients indicating IgM-mediated complement activation, and C3d deposition was almost absent in allografts from C3-deficient and CR2-Crry treated recipients. Inflammatory cell infiltration and P-selectin expression was also significantly reduced in C3-deficient and CR2-Crry treated recipients. Acute treatment with CR2-Crry or with 3 mg/kg/day cyclosporine A (CsA) modestly, but significantly increased median allograft survival from 5.8 to 7.4 and 7.2 days, respectively. However, combined acute CR2-Crry treatment and CsA therapy increased mean graft survival to 17.2 days. Protection was associated with significantly reduced T cell infiltration of allografts and Tc1 cells in recipient spleens. Conclusions Complement-mediated IRI augments graft allogenicity, and appropriate complement inhibition ameliorates IRI, decreases alloimmune priming and allows more immune-sparing CsA dosing.

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“…liver transplantation, hepatic tumor resection or trauma repair and can result in liver failure which has a high mortality rate [1][2] . Therefore murine studies of hepatic ischemia have become an important field of research by providing the opportunity to utilize pharmacological and genetic studies [3][4][5][6][7][8][9] . Specifically, conditional mice with tissue specific deletion of a gene (cre, flox system) provide insights into the role of proteins in particular tissues [10][11][12][13] .…”

mentioning

confidence: 99%

Use of a Hanging-weight System for Liver Ischemia in Mice

Zimmerman

Tak

Kaplan

et al. 2012

JoVE

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Acute liver injury due to ischemia can occur during several clinical procedures e.g. liver transplantation, hepatic tumor resection or trauma repair and can result in liver failure which has a high mortality rate [1][2] . Therefore murine studies of hepatic ischemia have become an important field of research by providing the opportunity to utilize pharmacological and genetic studies [3][4][5][6][7][8][9] . Specifically, conditional mice with tissue specific deletion of a gene (cre, flox system) provide insights into the role of proteins in particular tissues [10][11][12][13] . Because of the technical difficulty associated with manually clamping the portal triad in mice, we performed a systematic evaluation using a hanging-weight system for portal triad occlusion which has been previously described 3. By using a hanging-weight system we place a suture around the left branch of the portal triad without causing any damage to the hepatic lobes, since also the finest clamps available can cause hepatic tissue damage because of the close location of liver tissue to the vessels. Furthermore, the right branch of the hepatic triad is still perfused thus no intestinal congestion occurs with this technique as blood flow to the right hepatic lobes is preserved. Furthermore, the portal triad is only manipulated once throughout the entire surgical procedure. As a result, procedures like pre-conditioning, with short times of ischemia and reperfusion, can be easily performed. Systematic evaluation of this model by performing different ischemia and reperfusion times revealed a close correlation of hepatic ischemia time with liver damage as measured by alanine (ALT) and aspartate (AST) aminotransferase serum levels 3,9 . Taken together, these studies confirm highly reproducible liver injury when using the hanging-weight system for hepatic ischemia and intermittent reperfusion. Thus, this technique might be useful for other investigators interested in liver ischemia studies in mice. Therefore the video clip provides a detailed step-by-step description of this technique. Video LinkThe video component of this article can be found at https://www.jove.com/video/2550/ ProtocolGeneral remarks. All operations should be performed under an upright dissecting microscope (Leica) and by using a surgical coagulator. The mice in the experimental and sham groups should be matched in age and weight to ensure comparability of the results. Temperature, blood pressure, anesthesia and fluid administration should be stable and monitored during the entire experiment. Anesthesia and Surgery1. C57BL/6 mice should be within an age range of 10 to 16 weeks and they should be gender-matched in the respective groups. 2. Anesthetize mice with sodium pentobarbital (70 mg/kg body weight i.p.) and maintain anesthesia with approx. 10 mg/kg/h sodium pentobarbital. Overdosing can significantly lower blood pressure and thus can alter the results. 3. Place mice on a temperature-controlled heated table (RT, Effenberg, Munich, Germany) with a rectal thermometer ...

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The Protective Role of CD59 and Pathogenic Role of Complement in Hepatic Ischemia and Reperfusion Injury

Cited by 28 publications

References 62 publications

Complement—here, there and everywhere, but what about the transplanted organ?

Complement—here, there and everywhere, but what about the transplanted organ?

Targeted Complement Inhibition Protects Vascularized Composite Allografts From Acute Graft Injury and Prolongs Graft Survival When Combined With Subtherapeutic Cyclosporine A Therapy

Use of a Hanging-weight System for Liver Ischemia in Mice

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