Your search keyword '"Marc A. Seelen"' showing total 146 results

1. A non-muscle myosin heavy chain 9 genetic variant is associated with graft failure following kidney transplantation

Author

Felix Poppelaars, Siawosh K. Eskandari, Jeffrey Damman, Marc A. Seelen, Bernardo Faria, and Mariana Gaya da Costa

Subjects

genetics, kidney transplantation, molecular motor proteins, nephrology, Internal medicine, RC31-1245, Specialties of internal medicine, RC581-951

Abstract

Background Despite current matching efforts to identify optimal donor-recipient pairs for kidney transplantation, alloimmunity remains a major source of late transplant failure. Additional genetic parameters in donor-recipient matching could help improve long-term outcomes. Here, we studied the impact of a non-muscle myosin heavy chain 9 gene (MYH9) polymorphism on allograft failure. Methods We conducted an observational cohort study, analyzing the DNA of 1,271 kidney donor-recipient transplant pairs from a single academic hospital for the MYH9 rs11089788 C>A polymorphism. The associations of the MYH9 genotype with risk of graft failure, biopsy-proven acute rejection (BPAR), and delayed graft function (DGF) were estimated. Results A trend was seen in the association between the MYH9 polymorphism in the recipient and graft failure (recessive model, p = 0.056), but not for the MYH9 polymorphism in the donor. The AA-genotype MYH9 polymorphism in recipients was associated with higher risk of DGF (p = 0.03) and BPAR (p = 0.021), although significance was lost after adjusting for covariates (p = 0.15 and p = 0.10, respectively). The combined presence of the MYH9 polymorphism in donor-recipient pairs was associated with poor long-term kidney allograft survival (p = 0.04), in which recipients with an AA genotype receiving a graft with an AA genotype had the worst outcomes. After adjustment, this combined genotype remained significantly associated with 15-year death-censored kidney graft survival (hazard ratio, 1.68; 95% confidence interval, 1.05–2.70; p = 0.03). Conclusion Our results reveal that recipients with an AA-genotype MYH9 polymorphism receiving a donor kidney with an AA genotype have significantly elevated risk of graft failure after kidney transplantation.

Published

2023

2. Donor genetic variants in interleukin-6 and interleukin-6 receptor associate with biopsy-proven rejection following kidney transplantation

Author

Felix Poppelaars, Mariana Gaya da Costa, Siawosh K. Eskandari, Jeffrey Damman, and Marc A. Seelen

Subjects

Medicine, Science

Abstract

Abstract Rejection after kidney transplantation remains an important cause of allograft failure that markedly impacts morbidity. Cytokines are a major player in rejection, and we, therefore, explored the impact of interleukin-6 (IL6) and IL-6 receptor (IL6R) gene polymorphisms on the occurrence of rejection after renal transplantation. We performed an observational cohort study analyzing both donor and recipient DNA in 1271 renal transplant‐pairs from the University Medical Center Groningen in The Netherlands and associated single nucleotide polymorphisms (SNPs) with biopsy-proven rejection after kidney transplantation. The C-allele of the IL6R SNP (Asp358Ala; rs2228145 A > C, formerly rs8192284) in donor kidneys conferred a reduced risk of rejection following renal transplantation (HR 0.78 per C-allele; 95%-CI 0.67–0.90; P = 0.001). On the other hand, the C-allele of the IL6 SNP (at position-174 in the promoter; rs1800795 G > C) in donor kidneys was associated with an increased risk of rejection for male organ donors (HR per C-allele 1.31; 95%-CI 1.08–1.58; P = 0.0006), but not female organ donors (P = 0.33). In contrast, neither the IL6 nor IL6R SNP in the recipient showed an association with renal transplant rejection. In conclusion, donor IL6 and IL6R genotypes but not recipient genotypes represent an independent prognostic marker for biopsy-proven renal allograft rejection.

Published

2021

3. MASP-2 Is a Heparin-Binding Protease; Identification of Blocking Oligosaccharides

Author

Ditmer T. Talsma, Felix Poppelaars, Wendy Dam, Anita H. Meter-Arkema, Romain R. Vivès, Peter Gál, Geert-Jan Boons, Pradeep Chopra, Annamaria Naggi, Marc A. Seelen, Stephan P. Berger, Mohamed R. Daha, Coen A. Stegeman, Jacob van den Born, and the COMBAT Consortium

Subjects

lectin pathway, MASP-2, tetrasaccharide, heparin, complement, glycosaminoglycans, Immunologic diseases. Allergy, RC581-607

Abstract

It is well-known that heparin and other glycosaminoglycans (GAGs) inhibit complement activation. It is however not known whether fractionation and/or modification of GAGs might deliver pathway-specific inhibition of the complement system. Therefore, we evaluated a library of GAGs and their derivatives for their functional pathway specific complement inhibition, including the MASP-specific C4 deposition assay. Interaction of human MASP-2 with heparan sulfate/heparin was evaluated by surface plasmon resonance, ELISA and in renal tissue. In vitro pathway-specific complement assays showed that highly sulfated GAGs inhibited all three pathways of complement. Small heparin- and heparan sulfate-derived oligosaccharides were selective inhibitors of the lectin pathway (LP). These small oligosaccharides showed identical inhibition of the ficolin-3 mediated LP activation, failed to inhibit the binding of MBL to mannan, but inhibited C4 cleavage by MASPs. Hexa- and pentasulfated tetrasaccharides represent the smallest MASP inhibitors both in the functional LP assay as well in the MASP-mediated C4 assay. Surface plasmon resonance showed MASP-2 binding with heparin and heparan sulfate, revealing high Kon and Koff rates resulted in a Kd of ~2 μM and confirmed inhibition by heparin-derived tetrasaccharide. In renal tissue, MASP-2 partially colocalized with agrin and heparan sulfate, but not with activated C3, suggesting docking, storage, and potential inactivation of MASP-2 by heparan sulfate in basement membranes. Our data show that highly sulfated GAGs mediated inhibition of all three complement pathways, whereas short heparin- and heparan sulfate-derived oligosaccharides selectively blocked the lectin pathway via MASP-2 inhibition. Binding of MASP-2 to immobilized heparan sulfate/heparin and partial co-localization of agrin/heparan sulfate with MASP, but not C3b, might suggest that in vivo heparan sulfate proteoglycans act as a docking platform for MASP-2 and possibly prevent the lectin pathway from activation.

Published

2020

4. Blocking Complement Factor B Activation Reduces Renal Injury and Inflammation in a Rat Brain Death Model

Author

Neeltina M. Jager, Judith E. van Zanden, Marta Subías, Henri G. D. Leuvenink, Mohamed R. Daha, Santiago Rodríguez de Córdoba, Felix Poppelaars, and Marc A. Seelen

Subjects

factor B, complement, renal transplantation, brain death, donation, Immunologic diseases. Allergy, RC581-607

Abstract

Introduction: The majority of kidneys used for transplantation are retrieved from brain-dead organ donors. In brain death, the irreversible loss of brain functions results in hemodynamic instability, hormonal changes and immunological activation. Recently, brain death has been shown to cause activation of the complement system, which is adversely associated with renal allograft outcome in recipients. Modulation of the complement system in the brain-dead donor might be a promising strategy to improve organ quality before transplantation. This study investigated the effect of an inhibitory antibody against complement factor B on brain death-induced renal inflammation and injury.Method: Brain death was induced in male Fischer rats by inflating a balloon catheter in the epidural space. Anti-factor B (anti-FB) or saline was administered intravenously 20 min before the induction of brain death (n = 8/group). Sham-operated rats served as controls (n = 4). After 4 h of brain death, renal function, renal injury, and inflammation were assessed.Results: Pretreatment with anti-FB resulted in significantly less systemic and local complement activation than in saline-treated rats after brain death. Moreover, anti-FB treatment preserved renal function, reflected by significantly reduced serum creatinine levels compared to saline-treated rats after 4 h of brain death. Furthermore, anti-FB significantly attenuated histological injury, as seen by reduced tubular injury scores, lower renal gene expression levels (>75%) and renal deposition of kidney injury marker-1. In addition, anti-FB treatment significantly prevented renal macrophage influx and reduced systemic IL-6 levels compared to saline-treated rats after brain death. Lastly, renal gene expression of IL-6, MCP-1, and VCAM-1 were significantly reduced in rats treated with anti-FB.Conclusion: This study shows that donor pretreatment with anti-FB preserved renal function, reduced renal damage and inflammation prior to transplantation. Therefore, inhibition of factor B in organ donors might be a promising strategy to reduce brain death-induced renal injury and inflammation.

Published

2019

5. Urinary Properdin and sC5b-9 Are Independently Associated With Increased Risk for Graft Failure in Renal Transplant Recipients

Author

Rosa G. M. Lammerts, Michele F. Eisenga, Mohammed Alyami, Mohamed R. Daha, Marc A. Seelen, Robert A. Pol, Jacob van den Born, Jan-Stephan Sanders, Stephan J. L. Bakker, and Stefan P. Berger

Subjects

transplantation, chronic renal failure, properdin, C5b-9, complement activation, Immunologic diseases. Allergy, RC581-607

Abstract

The pathophysiology of late kidney-allograft failure remains complex and poorly understood. Activation of filtered or locally produced complement may contribute to the progression of renal failure through tubular C5b-9 formation. This study aimed to determine urinary properdin and sC5b-9 excretion and assess their association with long-term outcome in renal transplant recipients (RTR).Methods: We measured urinary properdin and soluble C5b-9 in a well-defined cross-sectional cohort of RTR. Urinary specimens were taken from a morning urine portion, and properdin and sC5b-9 were measured using an enzyme-linked-immunosorbent assay (ELISA). Cox proportional hazard regression analyses were used to investigate prospective associations with death-censored graft failure.Results: We included 639 stable RTR at a median [interquartile range] 5.3 (1.8–12.2) years after transplantation. Urinary properdin and sC5b-9 excretion were detectable in 161 (27%) and 102 (17%) RTR, respectively, with a median properdin level of 27.6 (8.6–68.1) ng/mL and a median sC5b-9 level of 5.1 (2.8–12.8) ng/mL. In multivariable-adjusted Cox regression analyses, including adjustment for proteinuria, urinary properdin (HR, 1.12; 95% CI 1.02–1.28; P = 0.008) and sC5b-9 excretion (HR, 1.34; 95% CI 1.10–1.63; P = 0.003) were associated with an increased risk of graft failure. If both urinary properdin and sC5b-9 were detectable, the risk of graft failure was further increased (HR, 3.12; 95% CI 1.69–5.77; P < 0.001).Conclusions: Our findings point toward a potential role for urinary complement activation in the pathogenesis of chronic allograft failure. Urinary properdin and sC5b-9 might be useful biomarkers for complement activation and chronic kidney allograft deterioration, suggesting a potential role for an alternative pathway blockade in RTR.

Published

2019

6. Administration of Intravenous Iron Formulations Induces Complement Activation in-vivo

Author

Bernardo Faria, Mariana Gaya da Costa, Felix Poppelaars, Casper F. M. Franssen, Manuel Pestana, Stefan P. Berger, Mohamed R. Daha, Carlo A. J. M. Gaillard, and Marc A. Seelen

Subjects

kidney, complement, hemodialysis, iron, anemia and kidney disease, Immunologic diseases. Allergy, RC581-607

Abstract

Background: Intravenous (IV) iron is widely used to treat anemia in chronic kidney disease patients. Previously, iron formulations were shown to induce immune activation in-vitro. The current study aimed to investigate the effect of IV iron on complement activation in-vivo, and whether this subsequently induces inflammation and/or oxidative stress.Methods: Two distinct patient groups were included: 51 non-dialysis and 32 dialysis patients. The non-dialysis group received iron sucrose or ferric carboxymaltose, based on physicians' choice. Plasma samples were collected prior to and 1 h after completion of IV iron infusion. The dialysis group received iron sucrose exclusively. Plasma samples were collected at the start and end of two consecutive hemodialysis sessions, one with and one without IV iron. Finally, plasma levels of MBL, C1q, properdin, factor D, sC5b-9, MPO, PTX3 were assessed by ELISA.Results: In the non-dialysis group, sC5b-9 levels significantly increased after IV iron by 32%, while levels of factor D and MBL significantly dropped. Subgroup analysis demonstrated that iron sucrose induced complement activation whereas ferric carboxymaltose did not. In the dialysis group, levels of sC5b-9 significantly increased by 46% during the dialysis session with IV iron, while factor D levels significantly fell. Furthermore, the relative decrease in factor D by IV iron correlated significantly with the relative increase in sC5b-9 by IV iron. MPO levels rose significantly during the dialysis session with IV iron, but not in the session without iron. Moreover, the relative increase in MPO and sC5b-9 by IV iron correlated significantly. PTX3 levels were not affected by IV iron.Conclusions: Iron sucrose but not ferric carboxymaltose, results in complement activation possibly via the lectin and alternative pathway partially mediating oxidative stress but not inflammation.

Published

2019

7. Complement Therapeutics in the Multi-Organ Donor: Do or Don't?

Author

Judith E. van Zanden, Neeltina M. Jager, Mohamed R. Daha, Michiel E. Erasmus, Henri G. D. Leuvenink, and Marc A. Seelen

Subjects

complement system, complement therapeutics, donor management, organ donor, deceased after brain death, deceased after circulatory death, Immunologic diseases. Allergy, RC581-607

Abstract

Over the last decade, striking progress has been made in the field of organ transplantation, such as better surgical expertise and preservation techniques. Therefore, organ transplantation is nowadays considered a successful treatment in end-stage diseases of various organs, e.g. the kidney, liver, intestine, heart, and lungs. However, there are still barriers which prevent a lifelong survival of the donor graft in the recipient. Activation of the immune system is an important limiting factor in the transplantation process. As part of this pro-inflammatory environment, the complement system is triggered. Complement activation plays a key role in the transplantation process, as highlighted by the amount of studies in ischemia-reperfusion injury (IRI) and rejection. However, new insight have shown that complement is not only activated in the later stages of transplantation, but already commences in the donor. In deceased donors, complement activation is associated with deteriorated quality of deceased donor organs. Of importance, since most donor organs are derived from either brain-dead donors or deceased after circulatory death donors. The exact mechanisms and the role of the complement system in the pathophysiology of the deceased donor have been underexposed. This review provides an overview of the current knowledge on complement activation in the (multi-)organ donor. Targeting the complement system might be a promising therapeutic strategy to improve the quality of various donor organs. Therefore, we will discuss the complement therapeutics that already have been tested in the donor. Finally, we question whether complement therapeutics should be translated to the clinics and if all organs share the same potential complement targets, considering the physiological differences of each organ.

Published

2019

8. Functional Studies on Primary Tubular Epithelial Cells Indicate a Tumor Suppressor Role of SETD2 in Clear Cell Renal Cell Carcinoma

Author

Jun Li, Joost Kluiver, Jan Osinga, Helga Westers, Maaike B van Werkhoven, Marc A. Seelen, Rolf H. Sijmons, Anke van den Berg, and Klaas Kok

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

SET domain-containing 2 (SETD2) is responsible for the trimethylation of histone H3 lysine36 (H3K36me3) and is one of the genes most frequently mutated in clear cell renal cell carcinoma (ccRCC). It is located at 3p21, one copy of which is lost in the majority of ccRCC tumors, suggesting that SETD2 might function as a tumor suppressor gene. However, the manner in which loss of SETD2 contributes to ccRCC development has not been studied in renal primary tubular epithelial cells (PTECs). Therefore, we studied the consequences of SETD2 knockdown through lentiviral shRNA in human PTECs. Consistent with its known function, SETD2 knockdown (SETD-KD) led to loss of H3K36me3 in PTECs. In contrast to SETD2 wild-type PTECs, which have a limited proliferation capacity; the SETD2-KD PTECs continued to proliferate. The expression profiles of SETD2-KD PTECs showed a large overlap with the expression profile of early-passage, proliferating PTECs, whereas nonproliferating PTECs showed a significantly different expression profile. Gene set enrichment analysis revealed a significant enrichment of E2F targets in SETD2-KD and proliferating PTECs as compared with nonproliferating PTECs and in proliferating PTEC compared with SETD2-KD. The SETD2-KD PTECs maintained low expression of CDKN2A and high expression of E2F1, whereas their levels changed with continuing passages in untreated PTECs. In contrast to the nonproliferating PTECs, SETD2-KD PTECs showed no β-galactosidase staining, confirming the protection against senescence. Our results indicate that SETD2 inactivation enables PTECs to bypass the senescence barrier, facilitating a malignant transformation toward ccRCC.

Published

2016

9. Age and Sex-Associated Changes of Complement Activity and Complement Levels in a Healthy Caucasian Population

Author

Mariana Gaya da Costa, Felix Poppelaars, Cees van Kooten, Tom E. Mollnes, Francesco Tedesco, Reinhard Würzner, Leendert A. Trouw, Lennart Truedsson, Mohamed R. Daha, Anja Roos, and Marc A. Seelen

Subjects

complement, health, sex and age, innate imunity, gender, Immunologic diseases. Allergy, RC581-607

Abstract

Introduction: The complement system is essential for an adequate immune response. Much attention has been given to the role of complement in disease. However, to better understand complement in pathology, it is crucial to first analyze this system under different physiological conditions. The aim of the present study was therefore to investigate the inter-individual variation in complement activity and the influences of age and sex.Methods: Complement levels and functional activity were determined in 120 healthy volunteers, 60 women, 60 men, age range 20–69 year. Serum functional activity of the classical pathway (CP), lectin pathway activated by mannan (MBL-LP) and alternative pathway (AP) was measured in sera, using deposition of C5b-9 as readout. In addition, levels of C1q, MBL, MASP-1, MASP-2, ficolin-2, ficolin-3, C2, C4, C3, C5, C6, C7, C8, C9, factor B, factor D, properdin, C1-inhibitor and C4b-binding protein, were determined. Age- and sex-related differences were evaluated.Results: Significantly lower AP activity was found in females compared to males. Further analysis of the AP revealed lower C3 and properdin levels in females, while factor D concentrations were higher. MBL-LP activity was not influenced by sex, but MBL and ficolin-3 levels were significantly lower in females compared to males. There were no significant differences in CP activity or CP components between females and males, nevertheless females had significantly lower levels of the terminal components. The CP and AP activity was significantly higher in the elderly, in contrast to MBL-LP activity. Moreover, C1-inhibitor, C5, C8, and C9 increased with age in contrast to a decrease of factor D and C3 levels. In-depth analysis of the functional activity assays revealed that MBL-LP activity was predominantly dependent on MBL and MASP-2 concentration, whereas CP activity relied on C2, C1-inhibitor and C5 levels. AP activity was strongly and directly associated with levels of C3, factor B and C5.Conclusion: This study demonstrated significant sex and age-related differences in complement levels and functionality in the healthy population. Therefore, age and sex analysis should be taken into consideration when discussing complement-related pathologies and subsequent complement-targeted therapies.

Published

2018

10. Intradialytic Complement Activation Precedes the Development of Cardiovascular Events in Hemodialysis Patients

Author

Felix Poppelaars, Mariana Gaya da Costa, Bernardo Faria, Stefan P. Berger, Solmaz Assa, Mohamed R. Daha, José Osmar Medina Pestana, Willem J. van Son, Casper F. M. Franssen, and Marc A. Seelen

Subjects

complement, kidney, cardiovascular risk, hemodialysis, biocompatibility, innate immunity, Immunologic diseases. Allergy, RC581-607

Abstract

Background: Hemodialysis (HD) is a life-saving treatment for patients with end stage renal disease. However, HD patients have markedly increased rates of cardiovascular morbidity and mortality. Previously, a link between the complement system and cardiovascular events (CV-events) has been reported. In HD, systemic complement activation occurs due to blood-to-membrane interaction. We hypothesize that HD-induced complement activation together with inflammation and thrombosis are involved in the development of CV-events in these patients.Methods: HD patients were followed for the occurrence of CV-events during a maximum follow-up of 45 months. Plasma samples were collected from 55 patients at different time points during one HD session prior to follow-up. Plasma levels of mannose-binding lectin, properdin and C3d/C3 ratios were assessed by ELISA. In addition, levels of von Willebrand factor, TNF-α and IL-6/IL-10 ratios were determined. An ex-vivo model of HD was used to assess the effect of complement inhibition.Results: During median follow-up of 32 months, 17 participants developed CV-events. In the CV-event group, the C3d/C3-ratio sharply increased 30 min after the start of the HD session, while in the event-free group the ratio did not increase. In accordance, HD patients that developed a CV-event also had a sustained higher IL-6/IL-10-ratio during the first 60 min of the HD session, followed by a greater rise in TNF-α levels and von Willebrand factor at the end of the session. In the ex-vivo HD model, we found that complement activation contributed to the induction of TNF-α levels, IL-6/IL-10-ratio and levels of von Willebrand factor.Conclusions: In conclusion, these findings suggest that early intradialytic complement activation predominantly occurred in HD patients who develop a CV-event during follow-up. In addition, in these patients complement activation was accompanied by a pro-inflammatory and pro-thrombotic response. Experimental complement inhibition revealed that this reaction is secondary to complement activation. Therefore, our data suggests that HD-induced complement, inflammation and coagulation are involved in the increased CV risk of HD patients.

Published

2018

11. The Complement System in Dialysis: A Forgotten Story?

Author

Felix Poppelaars, Bernardo Faria, Mariana Gaya da Costa, Casper F. M. Franssen, Willem J. van Son, Stefan P. Berger, Mohamed R. Daha, and Marc A. Seelen

Subjects

complement, kidney, dialysis, hemodialysis, peritoneal dialysis, Immunologic diseases. Allergy, RC581-607

Abstract

Significant advances have lead to a greater understanding of the role of the complement system within nephrology. The success of the first clinically approved complement inhibitor has created renewed appreciation of complement-targeting therapeutics. Several clinical trials are currently underway to evaluate the therapeutic potential of complement inhibition in renal diseases and kidney transplantation. Although, complement has been known to be activated during dialysis for over four decades, this area of research has been neglected in recent years. Despite significant progress in biocompatibility of hemodialysis (HD) membranes and peritoneal dialysis (PD) fluids, complement activation remains an undesired effect and relevant issue. Short-term effects of complement activation include promoting inflammation and coagulation. In addition, long-term complications of dialysis, such as infection, fibrosis and cardiovascular events, are linked to the complement system. These results suggest that interventions targeting the complement system in dialysis could improve biocompatibility, dialysis efficacy, and long-term outcome. Combined with the clinical availability to safely target complement in patients, the question is not if we should inhibit complement in dialysis, but when and how. The purpose of this review is to summarize previous findings and provide a comprehensive overview of the role of the complement system in both HD and PD.

Published

2018

12. Murine Precision-Cut Kidney Slices as an ex vivo Model to Evaluate the Role of Transforming Growth Factor-β1 Signaling in the Onset of Renal Fibrosis

Author

Elisabeth G. D. Stribos, Marc A. Seelen, Harry van Goor, Peter Olinga, and Henricus A. M. Mutsaers

Subjects

precision-cut kidney slices, ex vivo model, renal fibrosis, transforming-growth factor β, antifibrotic therapies, chronic kidney diseases, Physiology, QP1-981

Abstract

Renal fibrosis is characterized by progressive accumulation of extracellular matrix (ECM) proteins, resulting in loss of organ function and eventually requiring renal replacement therapy. Unfortunately, no efficacious treatment options are available to halt renal fibrosis and translational models to test pharmacological agents are not always representative. Here, we evaluated murine precision-cut kidney slices (mPCKS) as a promising ex vivo model of renal fibrosis in which pathophysiology as well as therapeutics can be studied. Unique to this model is the use of rodent as well as human renal tissue, further closing the gap between animal models and clinical trials. Kidneys from C57BL/6 mice were used to prepare mPCKS and slices were incubated up to 96h. Viability, morphology, gene expression of fibrosis markers (Col1a1, Acta2, Serpinh1, Fn1, and Pai-1), inflammatory markers (Il1b, Il6, Cxcl1), and protein expression (collagen type 1, α-smooth muscle actin, HSP47) were determined. Furthermore, to understand the role of the transforming-growth factor β (TGF-β) pathway in mPCKS, slices were incubated with a TGF-β receptor inhibitor (LY2109761) for 48 h. Firstly, viability and morphology revealed an optimal incubation period of 48 h. Secondly, we demonstrated an early inflammatory response in mPCKS, which was accompanied by subsequent spontaneous fibrogenesis. Finally, LY2109761 showed great antifibrotic capacity in mPCKS by decreasing fibrosis markers on mRNA level as well as by reducing HSP47 protein expression. To conclude, we here present an ex vivo model of renal fibrosis, which can be used to further unravel the mechanisms of renal fibrogenesis and to screen antifibrotic therapy efficacy.

Published

2017

13. An interleukin 6-based genetic risk score strengthened with interleukin 10 polymorphisms associated with long-term kidney allograft outcomes

Author

Siawosh K. Eskandari, Mariana Gaya da Costa, Bernardo Faria, Vojtech Petr, Jamil R. Azzi, Stefan P. Berger, Marc A.J. Seelen, Jeffrey Damman, Felix Poppelaars, Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), and Pathology

Subjects

Transplantation, Interleukin-6, long-term graft survival, kidney transplantation, Kidney, Allografts, Interleukin-10, interleukins, Risk Factors, Humans, Immunology and Allergy, Pharmacology (medical), Prospective Studies, polymorphisms

Abstract

Of all kidney transplants, half are still lost in the first decade after transplantation. Here, using genetics, we probed whether interleukin 6 (IL-6) could be a target in kidney transplantation to improve graft survival. Additionally, we investigated if a genetic risk score (GRS) based on IL6 and IL10 variants could improve prognostication of graft loss. In a prospective cohort study, DNA of 1271 donor-recipient kidney transplant pairs was analyzed for the presence of IL6, IL6R, IL10, IL10RA, and IL10RB variants. These polymorphisms and their GRS were then associated with 15-year death-censored allograft survival. The C|C-genotype of the IL6 polymorphism in donor kidneys and the combined C|C-genotype in donor-recipient pairs were both associated with a reduced risk of graft loss (p =.043 and p =.042, respectively). Additionally, the GRS based on IL6, IL6R, IL10, IL10RA, and IL10RB variants was independently associated with the risk of graft loss (HR 1.53, 95%-CI [1.32–1.84]; p

Published

2022

14. Carboxypeptidase B2 gene polymorphisms in the donor associate with kidney allograft loss

Author

Felix Poppelaars, Siawosh K. Eskandari, Jeffrey Damman, Ashley Frazer-Abel, V. Michael Holers, Bradley P. Dixon, Mohamed R. Daha, Jan-Stephan F. Sanders, Marc A. Seelen, Bernardo Faria, Mariana Gaya da Costa, and Joshua M. Thurman

Abstract

IntroductionPlasma carboxypeptidase B2 (CPB2) is an enzyme that cleaves C-terminal amino acids from proteins, thereby regulating their activities. CPB2 has anti-inflammatory and anti-fibrinolytic properties and can therefore be protective or harmful in disease. We explored the impact of functional carboxypeptidase B2 gene (CPB2) polymorphisms on graft survival following kidney transplantation.MethodsWe performed a longitudinal cohort study to evaluate the association of functionalCPB2polymorphisms (rs2146881, rs3742264, rs1926447, rs3818477) and complement polymorphisms (rs2230199, rs17611) with long-term allograft survival in 1,271 kidney transplant pairs from the University Medical Center Groningen in The Netherlands.ResultsThe high-producingCPB2rs3742264 polymorphism in the donor was associated with a reduced risk of graft loss following kidney transplantation (hazard ratio, 0.71 for the A-allele; 95%-CI, 0.55–0.93;P=0.014). In fully adjusted models, the association between the CPB2 polymorphism in the donor and graft loss remained significant. The protective effect of the high-producingCPB2variant in the donor could be mitigated by the hazardous effect of gain-of-function complement polymorphisms. Additionally, we compiled a genetic risk score of the fourCPB2variants in the recipients and donors, which was independently associated with long-term allograft survival. Furthermore, this genetic risk score substantially improved risk prediction for graft loss beyond currently used clinical predictors.ConclusionKidney allografts from deceased donors possessing a high-producing CPB2 polymorphism are at a lower risk of graft loss after kidney transplantation. Furthermore, our findings suggest that CPB2 might have a protective effect on graft loss through its ability to inactivate complement anaphylatoxins.EssentialsCarboxypeptidase B2 (CPB2) is a metalloprotease with anti-fibrinolytic and anti-inflammatory properties.We investigated the impact ofCPB2polymorphisms on graft loss after kidney transplantation.The rs3742264-A SNP in the donor, linked to higher CPB2 levels, decreased the risk of graft loss.CPB2 could have a protective effect on graft survival by inactivating complement anaphylatoxins.

Published

2023

15. Tumor Necrosis Factor-α Gene Polymorphism is Associated with Short-and Long-Term Kidney Allograft Outcomes

Author

Felix Poppelaars, Mariana Gaya da Costa, Bernardo Faria, Siawosh K Eskandari, Marc A Seelen, Jeffrey Damman, and Pathology

Subjects

DONOR PRETREATMENT, Immunology, nephrology, kidney transplantation, TRANSPLANT RECIPIENTS, TNF-ALPHA, cytokines, ISCHEMIA-REPERFUSION, surgical procedures, operative, SAFETY, INFLIXIMAB, THERAPEUTICS, MACHINE PERFUSION, INJURY, Immunology and Allergy, genetics, Journal of Inflammation Research

Abstract

Felix Poppelaars,1 Mariana Gaya da Costa,1,2 Bernardo Faria,1,3 Siawosh K Eskandari,1 Marc A Seelen,1 Jeffrey Damman4 1Department of Internal Medicine, Division of Nephrology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands; 2Department of Anesthesiology, University of Groningen, University Medical Center Groningen, Groningen, The Netherlands; 3Nephrology and Infectious Disease R&D Group, INEB, Institute of Investigation and Innovation in Health (i3S), University of Porto, Porto, Portugal; 4Department of Pathology, Erasmus Medical Center, University Medical Center, Rotterdam, The NetherlandsCorrespondence: Felix Poppelaars, Tel +31 50 3610544, Fax +31 50 3619320, Email f.poppelaars@umcg.nlIntroduction: Kidney transplantation has excellent short-term results with current immunosuppression regimes, but long-term outcomes have barely improved over the past two decades. Hence, there is a need for new therapeutic options to increase long-term survival of kidney grafts. Drug development for kidney transplantation has slowly plateaued, limiting progress while making drug repurposing an attractive alternative. We, therefore, investigated the impact of tumor necrosis factor-alpha (TNF-α) gene (TNF) polymorphisms on kidney graft survival after transplantation.Methods: We performed a prospective cohort study to assess the association of TNF polymorphisms (rs1800629 G>A and rs3093662 A>G) with primary non-function and death-censored kidney allograft survival in 1271 kidney transplant pairs from the University Medical Center Groningen in The Netherlands.Results: The G-allele of the TNF rs3093662 polymorphism in donor kidneys was associated with a higher risk of immediate graft loss (odds ratio: 2.05; 95%-CI: 1.06– 3.97; P = 0.032). Furthermore, the G-allele of this TNF rs3093662 polymorphism in the donor was also associated with worse 5-year, 10-year, and 15-year death-censored kidney graft survival (P < 0.05). The cumulative incidence of graft loss was 15.9% in the reference AA-genotype group and 25.2% in the AG/GG-genotype group, respectively. In multivariable analysis, the association between the TNF rs3093662 polymorphism in the donor and 15-year death-censored kidney graft survival remained significant (hazard ratio: 1.51; 95%-CI: 1.05– 2.19, P = 0.028).Discussion: In conclusion, kidney allografts possessing a high-producing TNF polymorphism have a greater risk of immediate and late graft loss. Our study adds to a growing body of literature indicating the potential of TNF-α blockade in improving kidney transplantation outcomes.Keywords: cytokines, kidney transplantation, nephrology, genetics

Published

2022

16. A functional TGFB1 polymorphism in the donor associates with long-term graft survival after kidney transplantation

Author

Siawosh K. Eskandari, Jeffrey Damman, Bernardo Faria, Marc A. Seelen, Felix Poppelaars, Mariana Gaya da Costa, and Pathology

Subjects

medicine.medical_specialty, nephrology, kidney transplantation, ACUTE REJECTION, Gastroenterology, THERAPY, DISEASE, Polymorphism (computer science), Internal medicine, medicine, FIBROSIS, genetics, TGF-beta, TGF-BETA-1, Kidney transplantation, Transplantation, Kidney, business.industry, GROWTH-FACTOR-BETA, Incidence (epidemiology), ALLOGRAFT SURVIVAL, medicine.disease, TNF-ALPHA, Genotype frequency, TRANSFORMING GROWTH-FACTOR-BETA-1 GENE, medicine.anatomical_structure, surgical procedures, operative, Graft survival, business, Cohort study

Abstract

Background Improvement of long-term outcomes in kidney transplantation remains one of the most pressing challenges, yet drug development is stagnating. Human genetics offers an opportunity for much-needed target validation in transplantation. Conflicting data exist about the effect of transforming growth factor-beta 1 (TGF-β1) on kidney transplant survival, since TGF-β1 has pro-fibrotic and protective effects. We investigated the impact of a recently discovered functional TGFB1 polymorphism on kidney graft survival. Methods We performed an observational cohort study analysing recipient and donor DNA in 1271 kidney transplant pairs from the University Medical Centre Groningen in The Netherlands, and associated a low-producing TGFB1 polymorphism (rs1800472-C > T) with 5-, 10- and 15-year death-censored kidney graft survival. Results Donor genotype frequencies of rs1800472 in TGFB1 differed significantly between patients with and without graft loss (P = 0.014). Additionally, the low-producing TGFB1 polymorphism in the donor was associated with an increased risk of graft loss following kidney transplantation (hazard ratio = 2.12 for the T-allele; 95% confidence interval 1.18–3.79; P = 0.012). The incidence of graft loss within 15 years of follow-up was 16.4% in the CC-genotype group and 31.6% in the CT-genotype group. After adjustment for transplant-related covariates, the association between the TGFB1 polymorphism in the donor and graft loss remained significant. In contrast, there was no association between the TGFB1 polymorphism in the recipient and graft loss. Conclusions Kidney allografts possessing a low-producing TGFB1 polymorphism have a higher risk of late graft loss. Our study adds to a growing body of evidence that TGF-β1 is beneficial, rather than harmful, for kidney transplant survival.

Published

2022

17. No Evident Systemic Terminal Complement Pathway Activation in Hidradenitis Suppurativa

Author

Lisette M. Prens, Jeffrey Damman, Barbara Horváth, Marc A. Seelen, Hessel H. van der Zee, Kelsey R. van Straalen, Jon D. Laman, Christine B. Ardon, Errol P. Prens, Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), Translational Immunology Groningen (TRIGR), Dermatology, and Pathology

Subjects

Adult, Male, Complement C5a, Dermatology, Biochemistry, Humans, Medicine, Hidradenitis suppurativa, Complement Activation, Molecular Biology, Clinical Trials as Topic, business.industry, Complement System Proteins, Cell Biology, Middle Aged, medicine.disease, Hidradenitis Suppurativa, Complement system, Cell biology, Terminal (electronics), Case-Control Studies, Female, Immunotherapy, Complement membrane attack complex, business, SKIN

Published

2021

18. Machine-perfused donor kidneys as a source of human renal endothelial cells

Author

Stefan P Berger, Lisanne M Lagendijk, Henri G. D. Leuvenink, Wendy Dam, Marc A. Seelen, Rosa G.M. Lammerts, Mohamed R. Daha, Gesa Tiller, Bouke G. Hepkema, Robert A. Pol, Harriet L Lancaster, Jacob van den Born, Grietje Molema, Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), ​Basic and Translational Research and Imaging Methodology Development in Groningen (BRIDGE), and Critical care, Anesthesiology, Peri-operative and Emergency medicine (CAPE)

Subjects

0301 basic medicine, CD31, EXPRESSION, Pathology, medicine.medical_specialty, kidney, HLA ANTIBODIES, Physiology, Population, PATHOPHYSIOLOGY, 030232 urology & nephrology, CD34, Human leukocyte antigen, Cell Separation, COMPLEMENT, CULTURE, 03 medical and health sciences, 0302 clinical medicine, Organ Culture Techniques, PHENOTYPIC HETEROGENEITY, medicine, INJURY, Humans, education, Cells, Cultured, education.field_of_study, Kidney, CLASS-II, Chemistry, Monocyte, CROSS-MATCH TEST, Histocompatibility Antigens Class I, machine perfusion, donation, Tissue Donors, endothelial cells, Transplantation, 030104 developmental biology, Lymphatic system, medicine.anatomical_structure, REJECTION, perfusate, transplantation

Abstract

Renal endothelial cells (ECs) play crucial roles in vasorelaxation, ultrafiltration, and selective transport of electrolytes and water, but also in leakage of the glomerular filtration barrier and inflammatory processes like complement activation and leukocyte recruitment. In addition, they are target cells for both cellular and antibody-mediated rejection in the transplanted kidney. To study the molecular and cellular processes underlying EC behavior in renal disease, well-characterized primary renal ECs are indispensible. In this report, we describe a straightforward procedure to isolate ECs from the perfusion fluid of human donor kidneys by a combination of negative selection of monocytes/macrophages, positive selection by CD31 Dynabeads, and propagation in endothelium-specific culture medium. Thus, we isolated and propagated renal ECs from 102 donor kidneys, representative of all blood groups and major human leukocyte antigen (HLA) class I and II antigens. The obtained ECs were positive for CD31 and von Willebrand factor, expressed other endothelial markers such as CD34, VEGF receptor-2, TIE2, and plasmalemmal vesicle associated protein-1 to a variable extent, and were negative for the monocyte marker CD14 and lymphatic endothelial marker podoplanin. HLA class II was either constitutively expressed or could be induced by interferon-y. Furthermore, as a proof of principle, we showed the diagnostic value of this renal endothelial biobank in renal endothelium-specific cross-matching tests for HLA antibodies.NEW & NOTEWORTHY We describe a new and widely accessible approach to obtain human primary renal endothelial cells in a \standardized fashion, by isolating from the perfusate of machine-perfused donor kidneys. Characterization of the cells showed a mixed population originating from different compartments of the kidney. As a proof of principle, we demonstrated a possible diagnostic application in an endothelium-specific cross-match. Next to transplantation, we foresee further applications in the field renal endothelial research.

Published

2021

19. Weak Expression of Terminal Complement in Active Antibody-Mediated Rejection of the Kidney

Author

Gesa Tiller, Rosa G. M. Lammerts, Jessy J. Karijosemito, Firas F. Alkaff, Arjan Diepstra, Robert A. Pol, Anita H. Meter-Arkema, Marc. A. Seelen, Marius C. van den Heuvel, Bouke G. Hepkema, Mohamed R. Daha, Jacob van den Born, Stefan P. Berger, Stem Cell Aging Leukemia and Lymphoma (SALL), Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), and ​Basic and Translational Research and Imaging Methodology Development in Groningen (BRIDGE)

Subjects

Graft Rejection, Male, RENAL-ALLOGRAFT REJECTION, Immunology, INHIBITION, kidney transplantation, chemical and pharmacologic phenomena, Complement Membrane Attack Complex, Kidney, THERAPY, Antibodies, C4D, membrane-attack complex, ACTIVATION, ECULIZUMAB, Complement C4b, Immunology and Allergy, Humans, TH17, DEPOSITION, complement system, C5b-9, Endothelial Cells, Complement System Proteins, CELLS, antibody-mediated rejection, Female, Kidney Diseases, CD59

Abstract

BackgroundThe role of the complement system in antibody-mediated rejection (ABMR) is insufficiently understood. We aimed to investigate the role of local and systemic complement activation in active (aABMR). We quantified complement activation markers, C3, C3d, and C5b-9 in plasma of aABMR, and acute T-cell mediated rejection (aTCMR), and non-rejection kidney transplant recipients. Intra-renal complement markers were analyzed as C4d, C3d, C5b-9, and CD59 deposition. We examined in vitro complement activation and CD59 expression on renal endothelial cells upon incubation with human leukocyte antigen antibodies.MethodsWe included 50 kidney transplant recipients, who we histopathologically classified as aABMR (n=17), aTCMR (n=18), and non-rejection patients (n=15).ResultsComplement activation in plasma did not differ across groups. C3d and C4d deposition were discriminative for aABMR diagnosis. Particularly, C3d deposition was stronger in glomerular (Pin vitro using renal endothelial cells and found complement pathway activation with C4d and C3d, but without terminal C5b-9 deposition. Complement regulator CD59 was variably present in biopsies and constitutively expressed on renal endothelial cells in vitro.ConclusionOur results indicate that terminal complement might only play a minor role in late aABMR, possibly indicating the need to re-evaluate the applicability of terminal complement inhibitors as treatment for aABMR.

Published

2022

20. Dermal C4d Deposition and Neutrophil Alignment Along the Dermal–Epidermal Junction as a Diagnostic Adjunct for Hypocomplementemic Urticarial Vasculitis (Anti-C1q Vasculitis) and Underlying Systemic Disease

Author

Martijn B. A. van Doorn, Jeffrey Damman, Antien Mooyaart, Marc A. Seelen, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Pathology, and Dermatology

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Systemic disease, hypocomplementemia, Hypocomplementemic urticarial vasculitis, Dermatology, Autoantigens, Pathology and Forensic Medicine, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, systemic lupus erythematosus, neutrophils, Anti c1q, Biopsy, Complement C4b, medicine, Humans, Lupus Erythematosus, Systemic, complement, Urticarial vasculitis, Autoantibodies, Retrospective Studies, Dermoepidermal junction, SPECTRUM, medicine.diagnostic_test, business.industry, Complement C1q, General Medicine, Middle Aged, medicine.disease, Peptide Fragments, C4d, urticarial vasculitis, Vasculitis, Leukocytoclastic, Cutaneous, Female, Vasculitis, business, Normocomplementemic urticarial vasculitis

Abstract

Urticarial vasculitis (UV) is a clinicopathologic entity characterized by persistent urticarial lesions with biopsy features of vasculitis. Currently, only certain clinical features such as arthralgia and serum complement concentrations are used to identify UV patients at risk for an underlying systemic disease. Hypocomplementemic urticarial vasculitis (HUV) is in contrast to normocomplementemic urticarial vasculitis (NUV), strongly associated with underlying systemic disease, especially systemic lupus erythematosus (SLE). The aim of this study was to find specific histopathological features associated with HUV and underlying systemic disease in UV. In addition, the use of complement C4d deposition in skin biopsies was evaluated as a diagnostic adjunct for HUV- and UV-associated systemic disease. In this retrospective study, the clinical, histopathological, and immunohistological (C4d) features of 43 patients with UV were compared between HUV and NUV and analyzed for association with UV-associated systemic disease. Eight of 43 patients with UV (19%) had hypocomplementemia. Patients with HUV showed a significantly higher number of perivascular neutrophils and lower number of eosinophils compared to NUV. Of all histopathological features, alignment of neutrophils along the dermal-epidermal junction (DEJ) and dermal granular C4d deposition were found to be strongly associated with HUV and underlying SLE. This study shows that both the alignment of neutrophils along the DEJ and dermal C4d deposition are strongly associated with HUV and SLE. Therefore, these (immuno)histopathological features can be used as an easy diagnostic adjunct for early detection of underlying systemic disease in UV.

Published

2020

21. Regulatory CD8 T cells that recognize Qa-1 expressed by CD4 T-helper cells inhibit rejection of heart allografts

Author

Amr Mansouri, Siawosh K. Eskandari, Harvey Cantor, John Choi, Jamil Azzi, Melissa Y. Yeung, Eman Alhussain, Saif A. Muhsin, Songjie Cai, Hye-Jung Kim, Hazim Allos, Jean Pierre Assaker, Marc A. Seelen, Ina Sulkaj, Juliano B. Alhaddad, Groningen Institute for Organ Transplantation (GIOT), and Groningen Kidney Center (GKC)

Subjects

Graft Rejection, DISRUPTION, 0301 basic medicine, Isoantigens, HLA-E, Receptors, Antigen, T-Cell, chemical and pharmacologic phenomena, Human leukocyte antigen, Biology, Major histocompatibility complex, T-Lymphocytes, Regulatory, ANTIBODY-MEDIATED REJECTION, Mice, 03 medical and health sciences, 0302 clinical medicine, CD8 Treg, Ab-mediated rejection, Isoantibodies, Immune Tolerance, Animals, Humans, Point Mutation, Transplantation, Homologous, Cytotoxic T cell, follicular helper T cell, Immunologic Tolerance, Multidisciplinary, Myocardium, Qa-1, Graft Survival, Histocompatibility Antigens Class I, T-cell receptor, T-Lymphocytes, Helper-Inducer, Biological Sciences, Allografts, Disease Models, Animal, 030104 developmental biology, Immunology, biology.protein, Heart Transplantation, Antibody, CD8, 030215 immunology

Abstract

Induction of longstanding immunologic tolerance is essential for survival of transplanted organs and tissues. Despite recent advances in immunosuppression protocols, allograft damage inflicted by antibody specific for donor organs continues to represent a major obstacle to graft survival. Here we report that activation of regulatory CD8 T cells (CD8 Treg) that recognize the Qa-1 class Ib major histocompatibility complex (MHC), a mouse homolog of human leukocyte antigen-E (HLA-E), inhibits antibody-mediated immune rejection of heart allografts. We analyzed this response using a mouse model that harbors a point mutation in the class Ib MHC molecule Qa-1, which disrupts Qa-1 binding to the T cell receptor (TCR)-CD8 complex and impairs the CD8 Treg response. Despite administration of cytotoxic T lymphocyte antigen 4 (CTLA-4) immunoglobulin (Ig), Qa-1 mutant mice developed robust donor-specific antibody responses and accelerated heart graft rejection. We show that these allo-antibody responses reflect diminished Qa-1-restricted CD8 Treg-mediated suppression of host follicular helper T cell-dependent antibody production. These findings underscore the critical contribution of this Qa-1/HLA-E-dependent regulatory pathway to maintenance of transplanted organs and suggest therapeutic approaches to ameliorate allograft rejection.

Published

2020

22. Lectin and alternative complement pathway activation in cutaneous manifestations of IgA-vasculitis: A new target for therapy?

Author

Jeffrey Damman, Antien L. Mooyaart, Thierry P.P. van den Bosch, Marc AJ Seelen, Martijn BA van Doorn, Pathology, Dermatology, Groningen Kidney Center (GKC), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

Adult, Male, Nephritis, IgA Vasculitis, Immunology, Immunofluorescence, Complement Pathway, Alternative, Middle Aged, Kidney, Mannose-Binding Lectin, C3c, Young Adult, Treatment Outcome, Innate, Humans, Female, Molecular Targeted Therapy, Molecular Biology, Complement Activation, Aged, Skin

Abstract

IgA-vasculitis is a systemic small-vessel leucocytoclastic vasculitis and is associated with a high morbidity. The disease can progress to IgA-vasculitis with nephritis (IgAVN) which can result in chronic renal failure. Complement activation is involved in the pathogenesis of IgA-vasculitis. A recent study has shown that cutaneous C3c deposition in IgA-vasculitis is associated with a higher risk to develop IgAVN. In the current study we investigated the different complement pathways that are activated in cutaneous IgA-vasculitis in order to reveal potential targets for intervention. In addition, we analyzed the association of complement factors with IgAVN and the clinical course of the disease. In this retrospective study, the clinicopathological features of 17 patients with IgA-vasculitis were compared with 25 non-IgA-vasculitis cases. Deposition of immunoglobulins and complement was analyzed by direct immunofluorescence for IgA, IgG, IgM, C1q, C4d, properdin, mannan-binding lectin (MBL), ficolin-2 (FCN2), MBL-associated serine protease 1/3 (MASP1/3), MASP2 and C3c. The vascular intensity and positive area was scored on a nominal scale and cumulative score was calculated by multiplying the intensity x area. Properdin was positive in 82% of IgA-vasculitis cases, reflecting alternative pathway activation. C4d was positive in 88% of IgA-vasculitis cases reflecting classical and/or lectin pathway activation, although only 12% of cases were positive for C1q. Lectin pathway activation was demonstrated by deposition of MBL (47%), MASP1/3 (53%) and MASP2 (6%) while FCN2 was found negative. Significantly more deposition of MASP1/3 was found in IgA-vasculitis versus non-IgA-vasculitis. This study demonstrates for the first time activation of lectin and alternative pathways in cutaneous manifestations of IgA-vasculitis. Hence, drugs that intervene in these complement pathways may be an interesting more targeted alternative to the current drugs, in reducing local cutaneous symptoms of the disease, with potentially less side-effects. No association was found between complement activation and IgAVN and/or response to therapy. Therefore, it is unlikely that intervention in complement activation will lead to a better clinical course of the disease.

Published

2021

23. A functional

Author

Felix, Poppelaars, Mariana, Gaya da Costa, Bernardo, Faria, Siawosh K, Eskandari, Jeffrey, Damman, and Marc A, Seelen

Abstract

Improvement of long-term outcomes in kidney transplantation remains one of the most pressing challenges, yet drug development is stagnating. Human genetics offers an opportunity for much-needed target validation in transplantation. Conflicting data exist about the effect of transforming growth factor-beta 1 (TGF-β1) on kidney transplant survival, since TGF-β1 has pro-fibrotic and protective effects. We investigated the impact of a recently discovered functionalWe performed an observational cohort study analysing recipient and donor DNA in 1271 kidney transplant pairs from the University Medical Centre Groningen in The Netherlands, and associated a low-producingDonor genotype frequencies of rs1800472 inKidney allografts possessing a low-producing

Published

2021

24. Soluble CD59 in peritoneal dialysis: a potential biomarker for peritoneal membrane function

Author

Stefan P Berger, Manuel Pestana, Carla Lima, Bernardo Faria, Marc A. Seelen, Mariana Gaya da Costa, Loek Willems, Mohamed R. Daha, Ricardo Brandwijk, Felix Poppelaars, Groningen Kidney Center (GKC), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

0301 basic medicine, Nephrology, medicine.medical_specialty, medicine.medical_treatment, 030232 urology & nephrology, Complement, Renal function, CD59 Antigens, CD59, Gastroenterology, Peritoneal dialysis, 03 medical and health sciences, 0302 clinical medicine, Dialysis Solutions, Internal medicine, Chronic kidney disease, medicine, Humans, Dialysis, Innate immunity, business.industry, Complement System Proteins, medicine.disease, 030104 developmental biology, Kidney Failure, Chronic, Biomarker (medicine), Original Article, Hemodialysis, Peritoneum, business, Peritoneal Dialysis, Biomarkers, Kidney disease

Abstract

Introduction Various studies have reported the importance of complement regulators in preventing mesothelial damage during peritoneal dialysis (PD). Its assessment, however, is limited in clinical practice due to the lack of easy access to the peritoneal membrane. Recently, a soluble form of the complement regulatory protein CD59 (sCD59) has been described. We therefore aimed to investigate the role of sCD59 in PD. Methods Plasma sCD59 was measured in 48 PD patients, 41 hemodialysis patients, 15 non-dialysis patients with chronic kidney disease and 14 healthy controls by ELISA (Hycult; HK374-02). Additionally, sCD59 and sC5b-9 were assessed in the peritoneal dialysate. Results sCD59 and sC5b-9 were detectable in the peritoneal dialysate of all patients, and marginally correlated (r = 0.27, P = 0.06). Plasma sCD59 levels were significantly higher in PD patients than in patients with chronic kidney disease and healthy controls, but did not differ from hemodialysis patients. During follow-up, 19% of PD patients developed peritoneal membrane failure and 27% of PD patients developed loss of residual renal function. In adjusted models, increased sCD59 levels in the dialysate (HR 3.44, 95% CI 1.04–11.40, P = 0.04) and in plasma (HR 1.08, 95% CI 1.01–1.17, P = 0.04) were independently associated with the occurrence of peritoneal membrane failure. Higher plasma levels of sCD59 were also associated with loss of residual renal function (HR 1.10, 95% CI 1.04–1.17, P Conclusions Our study suggests that sCD59 has potential as a biomarker to predict peritoneal membrane function and loss of residual renal function in PD, thereby offering a tool to improve patient management. Graphic abstract

Published

2021

25. A paired kidney analysis on the impact of pre-transplant anti-HLA antibodies on graft survival

Author

Annechien J. A. Lambeck, Maarten H. L. Christiaans, Frans H.J. Claas, Wendy Swelsen, Paul J M van der Boog, Mariëlle A C J Gelens, Marc A. Seelen, Eric Spierings, Caroline Roozendaal, Laura Bungener, Luuk B. Hilbrands, Laura A. Michielsen, Bouke G. Hepkema, Lotte Wieten, N M Lardy, Marije C. Baas, Arjan D. van Zuilen, Sebastiaan Heidt, Karlijn A M I van der Pant, Wil A. Allebes, Arnold van der Meer, Frederike J. Bemelman, Bram W. Wisse, Michiel L. Bots, Ineke J. M. ten Berge, Franka E. van Reekum, Henderikus G. Otten, Cornelis E. Hack, Jan-Stephan F. Sanders, Frans J. van Ittersum, Marcel G.J. Tilanus, Andries J. Hoitsma, Christien Voorter, Dave L. Roelen, Adriaan C.A.D. Drop, Neelke C. van der Weerd, Johan W. de Fijter, Shaikh A. Nurmohamed, Irma Joosten, Loes Plaisier, Marianne C. Verhaar, Elena G. Kamburova, Elizabeth M. van Duijnhoven, Michiel G. H. Betjes, Internal Medicine, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Interne Geneeskunde, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, MUMC+: DA TI Staf (9), MUMC+: DA TI Laboratorium (9), MUMC+: MA Nefrologie (9), RS: NUTRIM - R3 - Respiratory & Age-related Health, Nephrology, AII - Inflammatory diseases, APH - Aging & Later Life, ACS - Atherosclerosis & ischemic syndromes, ACS - Diabetes & metabolism, and Cardiology

Subjects

Nephrology, Graft Rejection, Male, 030232 urology & nephrology, graft survival, 030204 cardiovascular system & hematology, Gastroenterology, acute rejection, Kidney transplantation, immunology, 0302 clinical medicine, HLA Antigens, Isoantibodies, Medicine, DONOR-SPECIFIC ANTIBODIES, Netherlands, Kidney, biology, INDUCTION, Middle Aged, HLA antibodies, BEAD ASSAY, Tissue Donors, medicine.anatomical_structure, surgical procedures, operative, DP-SPECIFIC ANTIBODIES, Acute rejection, Female, Antibody, Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5], Adult, Risk, medicine.medical_specialty, CLINICAL-RELEVANCE, kidney transplantation, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], Human leukocyte antigen, 03 medical and health sciences, Young Adult, Antigen, MEDIATED REJECTION, RISK-FACTOR, Internal medicine, Journal Article, Humans, Risk factor, Transplantation, LOSS EVEN, business.industry, Histocompatibility Antigens Class I, HUMAN-LEUKOCYTE ANTIGEN, medicine.disease, RECIPIENTS, biology.protein, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], business

Abstract

Item does not contain fulltext BACKGROUND: Pre-transplant donor-specific anti-human leucocyte antigen (HLA) antibodies (DSAs) are associated with impaired kidney graft survival while the clinical relevance of non-donor-specific anti-HLA antibodies (nDSAs) is more controversial. The aim of the present paired kidney graft study was to compare the clinical relevance of DSAs and nDSAs. METHODS: To eliminate donor and era-dependent factors, a post hoc paired kidney graft analysis was performed as part of a Dutch multicentre study evaluating all transplantations between 1995 and 2005 with available pre-transplant serum samples. Anti-HLA antibodies were detected with a Luminex single-antigen bead assay. RESULTS: Among 3237 deceased donor transplantations, we identified 115 recipient pairs receiving a kidney from the same donor with one recipient being DSA positive and the other without anti-HLA antibodies. Patients with pre-transplant DSAs had a significantly lower 10-year death-censored graft survival (55% versus 82%, P=0.0001). We identified 192 pairs with one recipient as nDSA positive (against Class I and/or II) and the other without anti-HLA antibodies. For the patients with nDSAs against either Class I or II, graft survival did not significantly differ compared with patients without anti-HLA antibodies (74% versus 77%, P = 0.79). Only in patients with both nDSAs Class I and II was there a trend towards a lower graft survival (58%, P = 0.06). Lastly, in a small group of 42 recipient pairs, 10-year graft survival in recipients with DSAs was 49% compared with 68% in recipients with nDSAs (P=0.11). CONCLUSION: This paired kidney analysis confirms that the presence of pre-transplant DSAs in deceased donor transplantations is a risk marker for graft loss, whereas nDSAs in general are not associated with a lower graft survival. Subgroup analysis indicated that only in broadly sensitized patients with nDSAs against Class I and II, nDSAs may be a risk marker for graft loss in the long term.

Published

2019

26. The lectin pathway in renal disease

Author

Mohamed R. Daha, Stefan P Berger, Mariana Gaya da Costa, Marc A. Seelen, and Felix Poppelaars

Subjects

0301 basic medicine, kidney, NEPHROPATHY, PATHOGENESIS, Lupus nephritis, GLOMERULAR ACTIVATION, lectin pathway, BINDING PROTEIN, C4D, Nephropathy, 03 medical and health sciences, Complement inhibitor, Lectins, medicine, Animals, Humans, complement, DEPOSITION, Transplantation, Kidney, Complement component 3, Effector, business.industry, MASP-2, ASSOCIATION, medicine.disease, Complement system, PATTERN, 030104 developmental biology, medicine.anatomical_structure, Nephrology, DEFECT, Lectin pathway, Immunology, ischaemia reperfusion injury, Kidney Diseases, business, COMPLEMENT ACTIVATION, Signal Transduction

Abstract

The complement system is composed of a network of at least 40 proteins, which significantly contributes to health and disease. The lectin pathway (LP) is one of three pathways that can activate the complement system. Next to protection of the host against pathogens, the LP has been shown to play a crucial role in multiple renal diseases as well as during renal replacement therapy. Therefore, several complement-targeted drugs are currently being explored in clinical trials. Among these complement inhibitors, specific LP inhibitors are also being tested in renal abnormalities such as in immunoglobulin A nephropathy and lupus nephritis. Using various in vitro models, Yaseen et al. (Lectin pathway effector enzyme mannan-binding lectin-associated serine protease-2 can activate native complement component 3 (C3) in absence of C4 and/or C2. FASEB J 2017; 31: 2210-2219) showed that Mannan-associated serine protease2 can directly activate C3 thereby bypassing C2 and C4 in the activation of the LP. These new findings broaden our understanding of the mechanisms of complement activation and could potentially impact our strategies to inhibit the LP in renal diseases. In support of these findings, we present data of human renal biopsies, demonstrating the occurrence of the LP bypass mechanism in vivo. In conclusion, this review provides a detailed overview of the LP and clarifies the recently described bypass mechanism and its relevance. Finally, we speculate on the role of the C4 bypass mechanism in other renal diseases.

Published

2018

27. Arteriolar C4d in IgA nephropathy: a cohort study

Author

Bernardo Faria, Pedro Canão, Roberto Silva, Felix Poppelaars, Qingqing Cai, Mohamed R. Daha, Carla Henriques, Marc A. Seelen, Ana Matos, Manuel Pestana, Mariana Gaya da Costa, Groningen Kidney Center (GKC), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

Adult, Male, medicine.medical_specialty, OXFORD CLASSIFICATION, Biopsy, Kidney Glomerulus, 030232 urology & nephrology, Renal function, PROGRESSION, DEPOSITS, urologic and male genital diseases, Gastroenterology, COMPLEMENT, Nephropathy, ACTIVATION, PATHWAY, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Complement C4b, medicine, Humans, 030212 general & internal medicine, Complement Activation, Retrospective Studies, OUTCOMES, medicine.diagnostic_test, business.industry, Microangiopathy, Glomerulonephritis, IGA, Glomerulonephritis, Retrospective cohort study, Prognosis, medicine.disease, Nephrology, Disease Progression, RISK-FACTORS, Biomarker (medicine), Female, business, Biomarkers, Follow-Up Studies, Glomerular Filtration Rate, Kidney disease

Abstract

Rationale & Objective: Glomerular C4d (C4dG) as an indicator of the lectin pathway of complement activation in immunoglobulin A nephropathy (IgAN) has been associated with more severe kidney damage. Recent studies have suggested that vascular lesions in IgAN biopsy specimens with complement deposition are also associated with disease progression. We aimed to study the clinical significance of arteriolar C4d (C4dA) in IgAN kidney biopsy tissue.Study Design: Retrospective cohort study.Setting & Participants: Kidney biopsy specimens from 126 adults with IgAN diagnosed by Oxford classification criteria were stained using immunohistochemistry and classified according to C4dG and C4dA deposition. Additionally, vascular lesions including acute and chronic microangiopathy, arteriolar hyalinosis, and arterial intima fibrosis were characterized.Predictor: C4dA.Outcome: Progressive kidney disease, defined as a decline in estimated glomerular filtration rate by >= 50% or occurrence of kidney failure.Analytical Approach: The association of C4dA and C4dG with baseline clinical and histologic characteristics, as well as progressive kidney disease, were assessed with survival analysis using multivariable Cox regression analysis.Results: C4dA was identified in 21 (17%) patients and was associated with mean arterial pressure, arterial intima fibrosis, and chronic microangiopathy. C4dA was also significantly associated with C4dG and both were associated with progressive kidney disease. In regression analysis, C4dA remained significantly associated with progressive kidney disease after adjusting for other significant predictors, including baseline estimated glomerular filtration rate, mean arterial pressure, and the presence of crescents.Limitations: Findings based on the retrospective evaluation of a single center's experience, limited number of events, a small number of patients with a broad range of kidney disease stages, and use of immunohistochemistry rather than immunofluorescence to detect C4d.Conclusions: C4dA is a potential biomarker for disease progression in IgAN. It should be further investigated in larger cohorts to determine the value of C4dA in improving prediction of IgAN disease progression.

Published

2020

28. Brain death-induced lung injury is complement dependent, with a primary role for the classical/lectin pathway

Author

Zwanida J. Veldhuis, Henri G. D. Leuvenink, Marc A. Seelen, Judith E. van Zanden, Neeltina M. Jager, Michiel E. Erasmus, Mohamed R. Daha, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), and Cardiovascular Centre (CVC)

Subjects

basic (laboratory) research/science, translational research/science, donors and donation, DONORS, basic (laboratory) research, immunosuppression/immune modulation, 030230 surgery, IMMUNOLOGY, ACTIVATION, complement biology, Mice, 0302 clinical medicine, Basic Science, lung transplantation/pulmonology, Lectins, Immunology and Allergy, Medicine, Pharmacology (medical), donors and donation: donation after brain death (DBD), Complement Activation, pulmonology, science, immunosuppression, Interleukin, Lung Injury, Lectin pathway, Original Article, medicine.symptom, Brain Death, PROTEINS, Inflammation, Lung injury, 03 medical and health sciences, lung transplantation, Animals, C3, donation after brain death (DBD), Transplantation, immune modulation, business.industry, CHRONIC REJECTION, Complement deficiency, medicine.disease, Complement system, MODEL, translational research, Immunology, Properdin, ORIGINAL ARTICLES, business

Abstract

In brain‐dead donors immunological activation occurs, which deteriorates donor lung quality. Whether the complement system is activated and which pathways are herein involved, remain unknown. We aimed to investigate whether brain death (BD)‐induced lung injury is complement dependent and dissected the contribution of the complement activation pathways. BD was induced and sustained for 3 hours in wild‐type (WT) and complement deficient mice. C3−/− mice represented total complement deficiency, C4−/− mice represented deficiency of the classical and lectin pathway, and factor properdin (P)−/− mice represented alternative pathway deficiency. Systemic and local complement levels, histological lung injury, and pulmonary inflammation were assessed. Systemic and local complement levels were reduced in C3−/− mice. In addition, histological lung injury and inflammation were attenuated, as corroborated by influx of neutrophils and gene expressions of interleukin (IL)‐6, IL‐8–like KC, TNF‐α, E‐selectin, and MCP‐1. In C4−/− mice, complement was reduced on both systemic and local levels and histological lung injury and inflammatory status were ameliorated. In P−/− mice, histological lung injury was attenuated, though systemic and local complement levels, IL‐6 and KC gene expressions, and neutrophil influx were not affected. We demonstrated that BD‐induced lung injury is complement dependent, with a primary role for the classical/lectin activation pathway., In a mouse model, brain death–induced lung injury is complement‐dependent, elucidating a primary role for the classical/lectin complement activation pathway.

Published

2020

29. Properdin Pattern Recognition on Proximal Tubular Cells Is Heparan Sulfate/Syndecan-1 but Not C3b Dependent and Can Be Blocked by Tick Protein Salp20

Author

Stefan P Berger, Jacob van den Born, Wendy Dam, Mohamed R. Daha, Ditmer T. Talsma, Marc A. Seelen, Rosa G.M. Lammerts, Groningen Institute for Organ Transplantation (GIOT), and Groningen Kidney Center (GKC)

Subjects

0301 basic medicine, urologic and male genital diseases, Syndecan 1, law.invention, Kidney Tubules, Proximal, PATHWAY, chemistry.chemical_compound, 0302 clinical medicine, FUNCTIONAL-CHARACTERIZATION, law, Immunology and Allergy, complement, Original Research, SALIVARY PROTEIN, LOCALIZATION, Heparin, Heparan sulfate, female genital diseases and pregnancy complications, DEFICIENCY, properdin, Receptors, Pattern Recognition, Complement C3b, Recombinant DNA, Insect Proteins, COMPLEMENT ACTIVATION, Protein Binding, Signal Transduction, medicine.drug, lcsh:Immunologic diseases. Allergy, FACTOR-H, Immunology, INHIBITION, chemical and pharmacologic phenomena, Peptides, Cyclic, Cell Line, 03 medical and health sciences, medicine, Animals, Humans, Salivary Proteins and Peptides, C3, Ixodes, IDENTIFICATION, business.industry, syndecan-1, Epithelial Cells, Pattern recognition, In vitro, Complement system, Complement Inactivating Agents, 030104 developmental biology, chemistry, Alternative complement pathway, Properdin, Heparitin Sulfate, Artificial intelligence, Salp20, lcsh:RC581-607, business, 030215 immunology, BINDS

Abstract

Introduction: Proteinuria contributes to progression of renal damage, partly by complement activation on proximal tubular epithelial cells. By pattern recognition, properdin has shown to bind to heparan sulfate proteoglycans on tubular epithelium and can initiate the alternative complement pathway (AP). Properdin however, also binds to C3b(Bb) and properdin binding to tubular cells might be influenced by the presence of C3b(Bb) on tubular cells and/or by variability in properdin proteinsin vitro. In this study we carefully evaluated the specificity of the properdin - heparan sulfate interaction and whether this interaction could be exploited in order to block alternative complement activation.Methods: Binding of various properdin preparations to proximal tubular epithelial cells (PTEC) and subsequent AP activation was determined in the presence or absence of C3 inhibitor Compstatin and properdin inhibitor Salp20. Heparan sulfate proteoglycan dependency of the pattern recognition of properdin was evaluated on PTEC knocked down for syndecan-1 by shRNA technology. Solid phase binding assays were used to evaluate the effectivity of heparin(oids) and recombinant Salp20 to block the pattern recognition of properdin.Results: Binding of serum-derived and recombinant properdin preparations to PTECs could be dose-dependently inhibited (P heparin(oid) > C3b.Discussion: In this study we showed that all properdin preparations recognize heparan sulfate/syndecan-1 on PTECs with and without Compstatin C3 blocking conditions. In contrast to Compstatin, recombinant Salp20 prevents heparan sulfate pattern recognition by properdin on PTECs. Both complement inhibitors prevented properdin-mediated C3 activation. Binding of properdin to C3b could also be blocked by heparin(oids) and recombinant Salp20. This work indicates that properdin serves as a docking station for AP activation on PTECs and a Salp20 analog or heparinoids may be viable inhibitors in properdin mediated AP activation.

Published

2020

30. The influence of electronic health record use on collaboration among medical specialties

Author

Janita F.J. Vos, Marjolein van Offenbeek, Albert Boonstra, Arjen Kooistra, Marc A. Seelen, Research programme I&O, Value, Affordability and Sustainability (VALUE), Groningen Kidney Center (GKC), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

Knowledge management, 020205 medical informatics, TEAMS, Interprofessional Relations, 02 engineering and technology, ORGANIZATION, Health informatics, Health administration, 03 medical and health sciences, 0302 clinical medicine, Documentation, ROUTINES, health services administration, 0202 electrical engineering, electronic engineering, information engineering, Collaborative affordances, Medicine, Outpatient clinic, Humans, Electronic health records, 030212 general & internal medicine, Use, health care economics and organizations, INFORMATION-TECHNOLOGY, business.industry, Health Policy, Nursing research, lcsh:Public aspects of medicine, Information technology, lcsh:RA1-1270, CARE, DOCUMENTATION, Collaboration, Information overload, Workflow, INTERDISCIPLINARY, PAPER, AFFORDANCE, business, Research Article

Abstract

Background One of the main objectives of Electronic Health Records (EHRs) is to enhance collaboration among healthcare professionals. However, our knowledge of how EHRs actually affect collaborative practices is limited. This study examines how an EHR facilitates and constrains collaboration in five outpatient clinics. Methods We conducted an embedded case study at five outpatient clinics of a Dutch hospital that had implemented an organization-wide EHR. Data were collected through interviews with representatives of medical specialties, administration, nursing, and management. Documents were analyzed to contextualize these data. We examined the following collaborative affordances of EHRs: (1) portability, (2) co-located access, (3) shared overviews, (4) mutual awareness, (5) messaging, and (6) orchestrating. Results Our findings demonstrate how an EHR will both facilitate and constrain collaboration among specialties and disciplines. Affordances that were inscribed in the system for collaboration purposes were not fully actualized in the hospital because: (a) The EHR helps health professionals coordinate patient care on an informed basis at any time and in any place but only allows asynchronous patient record use. (b) The comprehensive patient file affords joint clinical decision-making based on shared data, but specialty- and discipline-specific user-interfaces constrain mutual understanding of that data. Moreover, not all relevant information can be easily shared across specialties and outside the hospital. (c) The reduced necessity for face-to-face communication saves time but is experienced as hindering collective responsibility for a smooth workflow. (d) The EHR affords registration at the source and registration of activities through orders, but the heightened administrative burden for physicians and the strict authorization rules on inputting data constrain the flexible, multidisciplinary collaboration. (e) While the EHR affords a complete overview, information overload occurs due to the parallel generation of individually owned notes and the high frequency of asynchronous communication through messages of varying clinical priority. Conclusions For the optimal actualization of EHRs’ collaborative affordances in hospitals, coordinated use of these affordances by health professionals is a prerequisite. Such coordinated use requires organizational, technical, and behavioral adaptations. Suggestions for hospital-wide policies to enhance trust in both the EHR and in its coordinated use for effective collaboration are offered.

Published

2020

31. Dysregulation of Complement Activation and Placental Dysfunction: A Potential Target to Treat Preeclampsia?

Author

Marc A. Seelen, Gustaaf A. Dekker, Harry van Goor, Jelmer R. Prins, Mohamed R. Daha, E. Pierik, and Sicco A. Scherjon

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Placenta Diseases, Placenta, Immunology, placental dysfunction, Inflammation, Review, Bioinformatics, NORMAL-PREGNANCY, ANGIOGENESIS, Preeclampsia, preeclampsia, 03 medical and health sciences, 0302 clinical medicine, Immune system, Pre-Eclampsia, Pregnancy, MANNOSE-BINDING LECTIN, medicine, Humans, Immunology and Allergy, complement, Complement Activation, reproductive and urinary physiology, Innate immune system, PATHWAY ACTIVATION, PRETERM, treatment, business.industry, MOLECULAR-WEIGHT HEPARIN, Complement System Proteins, Acquired immune system, medicine.disease, PREVENTION, DEFECTIVE PLACENTATION, COMPONENT, Complement system, Complement (complexity), ASPIRIN, 030104 developmental biology, embryonic structures, Female, medicine.symptom, lcsh:RC581-607, business, 030215 immunology

Abstract

Preeclampsia is one of the leading causes of maternal and neonatal mortality and morbidity worldwide, affecting 2–8% of all pregnancies. Studies suggest a link between complement activation and preeclampsia. The complement system plays an essential role in the innate immunity, leading to opsonization, inflammation, and elimination of potential pathogens. The complement system also provides a link between innate and adaptive immunity and clearance of immune complexes and apoptotic cells. During pregnancy there is increased activity of the complement system systemically. However, locally at the placenta, complement inhibition is crucial for the maintenance of a normal pregnancy. Inappropriate or excessive activation of the complement system at the placenta is likely involved in placental dysfunction, and is in turn associated with pregnancy complications like preeclampsia. Therefore, modulation of the complement system could be a potential therapeutic target to prevent pregnancy complications such as preeclampsia. This review, based on a systematic literature search, gives an overview of the complement system and its activation locally in the placenta and systemically during healthy pregnancies and during complicated pregnancies, with a focus on preeclampsia. Furthermore, this review describes results of animal and human studies with a focus on the complement system in pregnancy, and the role of the complement system in placental dysfunction. Various clinical and animal studies provide evidence that dysregulation of the complement system is associated with placental dysfunction and therefore with preeclampsia. Several drugs are used for prevention and treatment of preeclampsia in humans and animal models, and some of these drugs work through complement modulation. Therefore, this review further discusses these studies examining pharmaceutical interventions as treatment for preeclampsia. These observations will help direct research to generate new target options for prevention and treatment of preeclampsia, which include direct and indirect modulation of the complement system.

Published

2020

32. Inhibition of tyrosine kinase receptor signaling attenuates fibrogenesis in an ex vivo model of human renal fibrosis

Author

Emilia Bigaeva, Miriam Boersema, Bram Piersma, Lutz Wollin, Henricus A. M. Mutsaers, Anna M. Leliveld, Peter Olinga, Elisabeth G. D. Stribos, Marc A. Seelen, Harry van Goor, Igle J. de Jong, Ruud A. Bank, Pharmaceutical Technology and Biopharmacy, Guided Treatment in Optimal Selected Cancer Patients (GUTS), Groningen Kidney Center (GKC), Restoring Organ Function by Means of Regenerative Medicine (REGENERATE), Groningen Institute for Organ Transplantation (GIOT), Biopharmaceuticals, Discovery, Design and Delivery (BDDD), and Nanomedicine & Drug Targeting

Subjects

0301 basic medicine, Precision-cut kidney slices, Indoles, Physiology, medicine.medical_treatment, Kidney, NINTEDANIB, Receptor tyrosine kinase, CELL CANCER, ANGIOGENESIS, Mice, chemistry.chemical_compound, 0302 clinical medicine, Fibrosis, Renal fibrosis, CUT KIDNEY SLICES, Phosphorylation, BIBF 1120, precision-cut kidney slices, biology, renal fibrosis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Disease Progression, Kidney Diseases, Nintedanib, Signal Transduction, EXPRESSION, GROWTH-FACTOR, EARLY-ONSET, Tyrosine kinase receptor, 03 medical and health sciences, Growth factor receptor, medicine, Animals, Humans, LIVER SLICES, Protein Kinase Inhibitors, Cell Proliferation, Growth factor, medicine.disease, 030104 developmental biology, chemistry, biology.protein, Cancer research, tyrosine kinase receptor, ANGIOKINASE INHIBITOR

Abstract

Poor translation from animal studies to human clinical trials is one of the main hurdles in the development of new drugs. Here, we used precision-cut kidney slices (PCKS) as a translational model to study renal fibrosis and to investigate whether inhibition of tyrosine kinase receptors, with the selective inhibitor nintedanib, can halt fibrosis in murine and human PCKS. We used renal tissue of murine and human origins to obtain PCKS. Control slices and slices treated with nintedanib were studied to assess viability, activation of tyrosine kinase receptors, cell proliferation, collagen type I accumulation, and gene and protein regulation. During culture, PCKS spontaneously develop a fibrotic response that resembles in vivo fibrogenesis. Nintedanib blocked culture-induced phosphorylation of platelet-derived growth factor receptor and vascular endothelial growth factor receptor. Furthermore, nintedanib inhibited cell proliferation and reduced collagen type I accumulation and expression of fibrosis-related genes in healthy murine and human PCKS. Modulation of extracellular matrix homeostasis was achieved already at 0.1 μM, whereas high concentrations (1 and 5 μM) elicited possible nonselective effects. In PCKS from human diseased renal tissue, nintedanib showed limited capacity to reverse established fibrosis. In conclusion, nintedanib attenuated the onset of fibrosis in both murine and human PCKS by inhibiting the phosphorylation of tyrosine kinase receptors; however, the reversal of established fibrosis was not achieved.

Published

2020

33. Antibodies against ARHGDIB are associated with long-term kidney graft loss

Author

Karlijn A M I van der Pant, Michiel G. H. Betjes, Elena G. Kamburova, Irma Joosten, Jan-Stephan F. Sanders, Laura Bungener, Henny G. Otten, Bram W. Wisse, Adriaan C.A.D. Drop, Elly M. van Duijnhoven, Franka E. van Reekum, Maartje L Gruijters, Mariëlle A C J Gelens, Maarten H. L. Christiaans, Wendy Swelsen, Marc A. Seelen, Sebastiaan Heidt, Johan W. de Fijter, Cornelis E. Hack, Shaikh A. Nurmohamed, Michiel L. Bots, Loes Plaisier, Frederike J. Bemelman, Annechien J. A. Lambeck, Luuk B. Hilbrands, Bouke G. Hepkema, Arjan D. van Zuilen, Frans J. van Ittersum, Andries J. Hoitsma, Neelke C. van der Weerd, Marianne C. Verhaar, Frans H.J. Claas, Eric Spierings, N M Lardy, Paul J M van der Boog, Marije C. Baas, Arnold van der Meer, Tineke Kardol-Hoefnagel, Ineke J. M. ten Berge, Dave L. Roelen, Marcel G.J. Tilanus, Wil A. Allebes, Lotte Wieten, Rowena C A Melchers, Caroline Roozendaal, Christina E.M. Voorter, Nephrology, ACS - Atherosclerosis & ischemic syndromes, ACS - Diabetes & metabolism, AII - Inflammatory diseases, Cardiology, APH - Aging & Later Life, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Interne Geneeskunde, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, MUMC+: DA TI Staf (9), MUMC+: DA TI Laboratorium (9), MUMC+: MA Nefrologie (9), RS: NUTRIM - R3 - Respiratory & Age-related Health, Oral and Maxillofacial Surgery, Erasmus MC other, and Internal Medicine

Subjects

Graft Rejection, Male, ARHGDIB, 030230 surgery, Gastroenterology, Postoperative Complications, 0302 clinical medicine, rho Guanine Nucleotide Dissociation Inhibitor beta, HLA Antigens, Isoantibodies, Risk Factors, Living Donors, Immunology and Allergy, Pharmacology (medical), Kidney transplantation, education.field_of_study, Kidney, biology, Graft Survival, Hazard ratio, PRETRANSPLANT SENSITIZATION, Clinical Science, Middle Aged, Prognosis, non-HLA antibodies, TARGET, medicine.anatomical_structure, REJECTION, II TYPE-1 RECEPTOR, Original Article, Female, Antibody, non‐HLA antibodies, Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5], Adult, medicine.medical_specialty, Population, kidney transplantation, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], ANTIGENS, 03 medical and health sciences, RISK-FACTOR, Internal medicine, medicine, Journal Article, Humans, Clinical significance, education, Autoantibodies, Retrospective Studies, Transplantation, IDENTIFICATION, business.industry, Autoantibody, medicine.disease, PHOSPHOLIPASE-A2 RECEPTOR, biology.protein, Kidney Failure, Chronic, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], ORIGINAL ARTICLES, business, Follow-Up Studies

Abstract

The clinical significance of non‐HLA antibodies on renal allograft survival is a matter of debate, due to differences in reported results and lack of large‐scale studies incorporating analysis of multiple non‐HLA antibodies simultaneously. We developed a multiplex non‐HLA antibody assay against 14 proteins highly expressed in the kidney. In this study, the presence of pretransplant non‐HLA antibodies was correlated to renal allograft survival in a nationwide cohort of 4770 recipients transplanted between 1995 and 2006. Autoantibodies against Rho GDP‐dissociation inhibitor 2 (ARHGDIB) were significantly associated with graft loss in recipients transplanted with a deceased‐donor kidney (N = 3276) but not in recipients of a living‐donor kidney (N = 1496). At 10 years after deceased‐donor transplantation, recipients with anti‐ARHGDIB antibodies (94/3276 = 2.9%) had a 13% lower death‐censored covariate‐adjusted graft survival compared to the anti‐ARHGDIB‐negative (3182/3276 = 97.1%) population (hazard ratio 1.82; 95% confidence interval, 1.32‐2.53; P = .0003). These antibodies occur independently from donor‐specific anti‐HLA antibodies (DSA) or other non‐HLA antibodies investigated. No significant relations with graft loss were found for the other 13 non‐HLA antibodies. We suggest that pretransplant risk assessment can be improved by measuring anti‐ARHGDIB antibodies in all patients awaiting deceased‐donor transplantation., From a multicenter evaluation of kidney transplants, the authors report that the pretransplant presence of autoantibodies against ARHGDIB are associated with long‐term graft loss in recipients transplanted with a deceased donor kidney, independent from donor‐specific HLA antibodies.

Published

2019

34. Pretransplant C3d-Fixing Donor-Specific Anti-HLA Antibodies Are Not Associated with Increased Risk for Kidney Graft Failure

Author

Frederike J. Bemelman, Neelke C. van der Weerd, Bram W. Wisse, Luuk B. Hilbrands, Wendy Swelsen, Ineke J. M. ten Berge, Michiel G. H. Betjes, Arjan D. van Zuilen, Christina E.M. Voorter, Johan W. de Fijter, Arnold van der Meer, Henny G. Otten, Laura Bungener, Sebastiaan Heidt, Maarten H. L. Christiaans, Lotte Wieten, Wil A. Allebes, Marije C. Baas, Marc A. Seelen, M. Gelens, Dave L. Roelen, Elly M. van Duijnhoven, Karlijn A M I van der Pant, Frans J. van Ittersum, Bouke G. Hepkema, N M Lardy, Andries J. Hoitsma, Paul J M van der Boog, Franka E. van Reekum, Loes Plaisier, Caroline Roozendaal, Jan-Stephan F. Sanders, Annechien J. A. Lambeck, Elena G. Kamburova, Shaikh A. Nurmohamed, Michiel L. Bots, Cornelis E. Hack, Adriaan C.A.D. Drop, Frans H.J. Claas, Eric Spierings, Marcel G.J. Tilanus, Irma Joosten, Marianne C. Verhaar, Internal Medicine, Nephrology, Amsterdam institute for Infection and Immunity, AII - Inflammatory diseases, APH - Aging & Later Life, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, MUMC+: DA Transplantatie Immunologie (5), MUMC+: DA TI Staf (9), MUMC+: DA TI Laboratorium (9), MUMC+: MA Nefrologie (9), Interne Geneeskunde, RS: NUTRIM - R3 - Respiratory & Age-related Health, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Clinical chemistry, Rehabilitation medicine, ACS - Atherosclerosis & ischemic syndromes, ACS - Diabetes & metabolism, AII - Infectious diseases, and Internal medicine

Subjects

Graft Rejection, Male, Nephrology, 030232 urology & nephrology, 030230 surgery, Gastroenterology, Cohort Studies, 0302 clinical medicine, HLA Antigens, Registries, Kidney transplantation, chronic allograft failure, Kidney, biology, Incidence, Hazard ratio, General Medicine, Middle Aged, Tissue Donors, Antibodies, Anti-Idiotypic, medicine.anatomical_structure, Complement C3d, SURVIVAL, Female, Antibody, Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5], Rapid Communication, Adult, medicine.medical_specialty, kidney transplantation, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], chemical and pharmacologic phenomena, Human leukocyte antigen, Risk Assessment, 03 medical and health sciences, Age Distribution, Transplantation Immunology, Internal medicine, Preoperative Care, medicine, Humans, Sex Distribution, Contraindication, Antilymphocyte Serum, Retrospective Studies, TRANSPLANTATION, business.industry, anti-HLA antibodies, medicine.disease, Transplant Recipients, body regions, Transplantation, RECIPIENTS, complement-fixing antibodies, C1Q ASSAY, biology.protein, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], business, Follow-Up Studies

Abstract

Background Complement-fixing antibodies against donor HLA are considered a contraindication for kidney transplant. A modification of the IgG single-antigen bead (SAB) assay allows detection of anti-HLA antibodies that bind C3d. Because early humoral graft rejection is considered to be complement mediated, this SAB-based technique may provide a valuable tool in the pretransplant risk stratification of kidney transplant recipients.Methods Previously, we established that pretransplant donor-specific anti-HLA antibodies (DSAs) are associated with increased risk for long-term graft failure in complement-dependent cytotoxicity crossmatch-negative transplants. In this study, we further characterized the DSA-positive serum samples using the C3d SAB assay.Results Among 567 pretransplant DSA-positive serum samples, 97 (17%) contained at least one C3d-fixing DSA, whereas 470 (83%) had non-C3d-fixing DSA. At 10 years after transplant, patients with C3d-fixing antibodies had a death-censored, covariate-adjusted graft survival of 60%, whereas patients with non-C3d-fixing DSA had a graft survival of 64% (hazard ratio, 1.02; 95% confidence interval, 0.70 to 1.48 for C3d-fixing DSA compared with non-C3d-fixing DSA; P=0.93). Patients without DSA had a 10-year graft survival of 78%.Conclusions The C3d-fixing ability of pretransplant DSA is not associated with increased risk for graft failure.

Published

2018

35. C1-inhibitor Treatment Decreases Renal Injury in an Established Brain-dead Rat Model

Author

Juha Kotimaa, Cees van Kooten, Neeltina M. Jager, Henri G. D. Leuvenink, Felix Poppelaars, Jeffrey Damman, Marc A. Seelen, Mohamed R. Daha, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), and Other departments

Subjects

0301 basic medicine, Male, 030232 urology & nephrology, Pharmacology, 030230 surgery, C1-inhibitor, PATHWAY, chemistry.chemical_compound, 0302 clinical medicine, Kidney transplantation, GENE-EXPRESSION, Brain dead, biology, HEREDITARY ANGIOEDEMA, Kidney Diseases, C1 INHIBITOR CONCENTRATE, COMPLEMENT ACTIVATION, Complement C1 Inhibitor Protein, medicine.medical_specialty, Brain Death, KIDNEY-TRANSPLANTATION, Immunology, Rat model, Renal function, ISCHEMIA/REPERFUSION INJURY, 03 medical and health sciences, Renal injury, Internal medicine, medicine, Journal Article, Animals, Organ donation, ORGAN DONATION, DONOR KIDNEYS, Molecular Biology, Transplantation, Creatinine, business.industry, Interleukin-6, Balloon catheter, medicine.disease, Kidney Transplantation, Rats, Inbred F344, DYSFUNCTION, Complement system, Rats, Disease Models, Animal, 030104 developmental biology, Endocrinology, chemistry, biology.protein, business

Abstract

Background Kidneys derived from brain-dead (BD) donors have lower graft survival rates compared with kidneys from living donors. Complement activation plays an important role in brain death. The aim of our study was therefore to investigate the effect of C1-inhibitor (C1-INH) on BD-induced renal injury. Methods Brain death was induced in rats by inflating a subdurally placed balloon catheter. Thirty minutes after BD, rats were treated with saline, low-dose or high-dose C1-INH. Sham-operated rats served as controls. After 4 hours of brain death, renal function, injury, inflammation, and complement activation were assessed. Results High-dose C1-INH treatment of BD donors resulted in significantly lower renal gene expression and serum levels of IL-6. Treatment with C1-INH also improved renal function and reduced renal injury, reflected by the significantly lower kidney injury marker 1 gene expression and lower serum levels of lactate dehydrogenase and creatinine. Furthermore, C1-INH effectively reduced complement activation by brain death and significantly increased functional levels. However, C1-INH treatment did not prevent renal cellular influx. Conclusions Targeting complement activation after the induction of brain death reduced renal inflammation and improved renal function before transplantation. Therefore, strategies targeting complement activation in human BD donors might clinically improve donor organ viability and renal allograft survival.

Published

2018

36. Corrigendum to ‘Propofol-based anaesthesia versus sevoflurane-based anaesthesia for living donor kidney transplantation: results of the VAPOR-1 randomized controlled trial’ (Br J Anaesth 2017; 118: 720–32)

Author

Michel Struys, Johannes G. M. Burgerhof, Vincent B. Nieuwenhuijs, Petra J Ottens, Marc A. Seelen, Gertrude J. Nieuwenhuijs-Moeke, Marius C. van den Heuvel, Rutger J. Ploeg, Henri G. D. Leuvenink, and Stefan P Berger

Subjects

business.industry, MEDLINE, medicine.disease, Living donor, Sevoflurane, law.invention, Anesthesiology and Pain Medicine, Randomized controlled trial, law, Anesthesia, medicine, Propofol, business, Kidney transplantation, medicine.drug

Published

2021

37. Propofol-based anaesthesia versus sevoflurane-based anaesthesia for living donor kidney transplantation: results of the VAPOR-1 randomized controlled trial

Author

Stefan P Berger, P.J. Ottens, Henri G. D. Leuvenink, Michel Struys, Rutger J. Ploeg, Vincent B. Nieuwenhuijs, M.C. van den Heuvel, Gertrude J. Nieuwenhuijs-Moeke, Marc A. Seelen, Johannes G. M. Burgerhof, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Life Course Epidemiology (LCE), and Critical care, Anesthesiology, Peri-operative and Emergency medicine (CAPE)

Subjects

Male, CELL INJURY, 030232 urology & nephrology, Pilot Projects, ISCHEMIA-REPERFUSION INJURY, VOLATILE ANESTHETICS, MOLECULE-1, 0302 clinical medicine, 030202 anesthesiology, Living Donors, Hepatitis A Virus Cellular Receptor 1, Prospective Studies, Kidney transplantation, Acute kidney injury, ALLOGRAFT SURVIVAL, Acute Kidney Injury, Middle Aged, reperfusion injury, Neoplasm Proteins, GRAFT FUNCTION, Anesthesia, Anesthetics, Inhalation, Anesthesia, Intravenous, Female, Propofol, Fatty Acid Binding Protein 3, Anesthetics, Intravenous, medicine.drug, Adult, Adolescent, Urinary system, sevoflurane, Remifentanil, kidney transplantation, Renal function, Sevoflurane, Young Adult, 03 medical and health sciences, RENAL ISCHEMIA, medicine, Humans, REMIFENTANIL, Aged, Immunosuppression Therapy, propofol, business.industry, biomarkers, medicine.disease, BETA-D-GLUCOSAMINIDASE, Transplantation, Anesthesiology and Pain Medicine, Anesthesia, Inhalation, URINARY BIOMARKERS, business

Abstract

Background Kidney transplantation is associated with harmful processes affecting the viability of the graft. One of these processes is associated with the phenomenon of ischaemia–reperfusion injury. Anaesthetic conditioning is a widely described strategy to attenuate ischaemia–reperfusion injury. We therefore conducted the Volatile Anaesthetic Protection of Renal Transplants-1 trial, a pilot project evaluating the influence of two anaesthetic regimens, propofol- vs sevoflurane-based anaesthesia, on biochemical and clinical outcomes in living donor kidney transplantation. Methods Sixty couples were randomly assigned to the following three groups: PROP (donor and recipient propofol), SEVO (donor and recipient sevoflurane), and PROSE (donor propofol and recipient sevoflurane). The primary outcome was renal injury reflected by urinary biomarkers. The follow-up period was 2 yr. Results Three couples were excluded, leaving 57 couples for analysis. Concentrations of kidney injury molecule-1 (KIM-1), N-acetyl-β-d-glucosaminidase (NAG), and heart-type fatty acid binding protein (H-FABP) in the first urine upon reperfusion showed no differences. On day 2, KIM-1 concentrations were higher in SEVO [952.8 (interquartile range 311.8–1893.0) pg mmol−1] compared with PROP [301.2 (202.0–504.7) pg mmol−1]. This was the same for NAG: SEVO, 1.835 (1.162–2.457) IU mmol−1vs PROP, 1.078 (0.819–1.713) IU mmol−1. Concentrations of H-FABP showed no differences. Measured glomerular filtration rate at 3, 6, and 12 months showed no difference. After 2 yr, there was a difference in the acute rejection rate (P=0.039). Post hoc testing revealed a difference between PROP (35%) and PROSE (5%; P=0.020). The difference between PROP and SEVO (11%) was not significant (P=0.110). Conclusions The SEVO group showed higher urinary KIM-1 and NAG concentrations in living donor kidney transplantation on the second day after transplantation. This was not reflected in inferior graft outcome. Clinical trial registration NCT01248871.

Published

2017

38. Complement-mediated inflammation and injury in brain dead organ donors

Author

Felix Poppelaars, Marc A. Seelen, Groningen Institute for Organ Transplantation (GIOT), and Groningen Kidney Center (GKC)

Subjects

0301 basic medicine, Brain Death, KIDNEY-TRANSPLANTATION, medicine.medical_treatment, Immunology, THYROID-HORMONE, Inflammation, CD59, 030230 surgery, ISCHEMIA/REPERFUSION INJURY, ACTIVATION, PATHWAY, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Mediator, Donor brain death, medicine, Animals, Humans, Lung transplantation, Molecular Biology, Kidney transplantation, LUNG TRANSPLANTATION, Transplantation, RENAL-TRANSPLANTATION, business.industry, LECTIN, medicine.disease, GENE, Tissue Donors, Complement activation, Complement system, 030104 developmental biology, REJECTION, medicine.symptom, business

Abstract

The importance of the complement system in renal ischemia-reperfusion injury and acute rejection is widely recognized, however its contribution to the pathogenesis of tissue damage in the donor remains underexposed. Brain-dead (BD) organ donors are still the primary source of organs for transplantation. Brain death is characterized by hemodynamic changes, hormonal dysregulation, and immunological activation. Recently, the complement system has been shown to be involved. In BD organ donors, complement is activated systemically and locally and is an important mediator of inflammation and graft injury. Furthermore, complement activation can be used as a clinical marker for the prediction of graft function after transplantation. Experimental models of BD have shown that inhibition of the complement cascade is a successful method to reduce inflammation and injury of donor grafts, thereby improving graft function and survival after transplantation. Consequently, complement-targeted therapeutics in BD organ donors form a new opportunity to improve organ quality for transplantation. Future studies should further elucidate the mechanism responsible for complement activation in BD organ donors. (C) 2016 Elsevier Ltd. All rights reserved.

Published

2017

39. Urinary Properdin and sC5b-9 Are Independently Associated With Increased Risk for Graft Failure in Renal Transplant Recipients

Author

Marc A. Seelen, Stefan P Berger, Jan-Stephan F. Sanders, Stephan J. L. Bakker, Jacob van den Born, Mohammed Alyami, Rosa G.M. Lammerts, Michele F Eisenga, Robert A. Pol, Mohamed R. Daha, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Lifestyle Medicine (LM), and ​Basic and Translational Research and Imaging Methodology Development in Groningen (BRIDGE)

Subjects

0301 basic medicine, lcsh:Immunologic diseases. Allergy, Adult, Graft Rejection, Male, medicine.medical_specialty, Urinary system, Immunology, Urology, chemical and pharmacologic phenomena, Complement Membrane Attack Complex, Kidney Function Tests, urologic and male genital diseases, Models, Biological, 03 medical and health sciences, 0302 clinical medicine, Interquartile range, chronic renal failure, Medicine, Humans, Immunology and Allergy, Complement Activation, Proportional Hazards Models, Original Research, Kidney, Proteinuria, Properdin, business.industry, Proportional hazards model, C5b-9, Complement System Proteins, Middle Aged, Prognosis, Kidney Transplantation, Transplant Recipients, Transplantation, 030104 developmental biology, medicine.anatomical_structure, Cross-Sectional Studies, Treatment Outcome, Alternative complement pathway, Female, medicine.symptom, business, lcsh:RC581-607, Biomarkers, 030215 immunology, transplantation

Abstract

The pathophysiology of late kidney-allograft failure remains complex and poorly understood. Activation of filtered or locally produced complement may contribute to the progression of renal failure through tubular C5b-9 formation. This study aimed to determine urinary properdin and sC5b-9 excretion and assess their association with long-term outcome in renal transplant recipients (RTR). Methods: We measured urinary properdin and soluble C5b-9 in a well-defined cross-sectional cohort of RTR. Urinary specimens were taken from a morning urine portion, and properdin and sC5b-9 were measured using an enzyme-linked-immunosorbent assay (ELISA). Cox proportional hazard regression analyses were used to investigate prospective associations with death-censored graft failure. Results: We included 639 stable RTR at a median [interquartile range] 5.3 (1.8-12.2) years after transplantation. Urinary properdin and sC5b-9 excretion were detectable in 161 (27%) and 102 (17%) RTR, respectively, with a median properdin level of 27.6 (8.6-68.1) ng/mL and a median sC5b-9 level of 5.1 (2.8-12.8) ng/mL. In multivariable-adjusted Cox regression analyses, including adjustment for proteinuria, urinary properdin (HR, 1.12; 95% CI 1.02-1.28; P = 0.008) and sC5b-9 excretion (HR, 1.34; 95% CI 1.10-1.63; P = 0.003) were associated with an increased risk of graft failure. If both urinary properdin and sC5b-9 were detectable, the risk of graft failure was further increased (HR, 3.12; 95% CI 1.69-5.77; P < 0.001). Conclusions: Our findings point toward a potential role for urinary complement activation in the pathogenesis of chronic allograft failure. Urinary properdin and sC5b-9 might be useful biomarkers for complement activation and chronic kidney allograft deterioration, suggesting a potential role for an alternative pathway blockade in RTR.

Published

2019

40. Allocation to highly sensitized patients based on acceptable mismatches results in low rejection rates comparable to nonsensitized patients

Author

Karlijn A M I van der Pant, Henny G. Otten, Sebastiaan Heidt, Ineke J. M. ten Berge, Bram W. Wisse, Mariëlle A C J Gelens, Michiel L. Bots, Paul J M van der Boog, Marissa J. H. van der Linden-van Oevelen, Annechien J. A. Lambeck, Wendy Swelsen, N M Lardy, Frans J. van Ittersum, Dave L. Roelen, Andries J. Hoitsma, Franka E. van Reekum, Arnold van der Meer, Johan W. de Fijter, Jan-Stephan F. Sanders, Adriaan C.A.D. Drop, Shaikh A. Nurmohamed, Elena G. Kamburova, Bouke G. Hepkema, Cornelis E. Hack, Marije C. Baas, Geert W. Haasnoot, Marian D. Witvliet, Luuk B. Hilbrands, Caroline Roozendaal, Arjan D. van Zuilen, Wil A. Allebes, Michiel G. H. Betjes, Marcel G.J. Tilanus, Loes Plaisier, Elly M. van Duijnhoven, Lotte Wieten, Frans H.J. Claas, Maarten H. L. Christiaans, Neelke C. van der Weerd, Marc A. Seelen, Frederike J. Bemelman, Christina E.M. Voorter, Eric Spierings, Laura Bungener, Irma Joosten, Marianne C. Verhaar, Nephrology, ACS - Atherosclerosis & ischemic syndromes, ACS - Diabetes & metabolism, AII - Inflammatory diseases, APH - Aging & Later Life, Oral and Maxillofacial Surgery, Erasmus MC other, Internal Medicine, Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, Interne Geneeskunde, MUMC+: DA TI Staf (9), MUMC+: DA TI Laboratorium (9), MUMC+: MA Nefrologie (9), and RS: NUTRIM - R3 - Respiratory & Age-related Health

Subjects

Graft Rejection, Male, Nephrology, kidney transplantation/nephrology, 030230 surgery, 0302 clinical medicine, HLA Antigens, Isoantibodies, Risk Factors, PROGRAM, DONOR-SPECIFIC ANTIBODIES, Immunology and Allergy, histocompatibility, Pharmacology (medical), Kidney transplantation, RISK, Histocompatibility Testing, Incidence (epidemiology), Graft Survival, Middle Aged, Prognosis, Tissue Donors, practice, Cohort, SURVIVAL, Female, rejection, Brief Communications, Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5], medicine.medical_specialty, major histocompatibility complex (MHC), Tissue and Organ Procurement, CLINICAL-RELEVANCE, KIDNEY ALLOCATION, nephrology, kidney transplantation, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], Human leukocyte antigen, Brief Communication, clinical research/practice, 03 medical and health sciences, Transplantation Immunology, Internal medicine, medicine, alloantibody, Journal Article, Humans, Transplantation, business.industry, Patient Selection, medicine.disease, HLA Mismatch, Histocompatibility, immunogenetics, MATERNAL HLA ANTIGENS, clinical research, Kidney Failure, Chronic, Immunization, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], business, Follow-Up Studies

Abstract

Whereas regular allocation avoids unacceptable mismatches on the donor organ, allocation to highly sensitized patients within the Eurotransplant Acceptable Mismatch (AM) program is based on the patient's HLA phenotype plus acceptable antigens. These are HLA antigens to which the patient never made antibodies, as determined by extensive laboratory testing. AM patients have superior long‐term graft survival compared with highly sensitized patients in regular allocation. Here, we questioned whether the AM program also results in lower rejection rates. From the PROCARE cohort, consisting of all Dutch kidney transplants in 1995‐2005, we selected deceased donor single transplants with a minimum of 1 HLA mismatch and determined the cumulative 6‐month rejection incidence for patients in AM or regular allocation. Additionally, we determined the effect of minimal matching criteria of 1 HLA‐B plus 1 HLA‐DR, or 2 HLA‐DR antigens on rejection incidence. AM patients showed significantly lower rejection rates than highly immunized patients in regular allocation, comparable to nonsensitized patients, independent of other risk factors for rejection. In contrast to highly sensitized patients in regular allocation, minimal matching criteria did not affect rejection rates in AM patients. Allocation based on acceptable antigens leads to relatively low‐risk transplants for highly sensitized patients with rejection rates similar to those of nonimmunized individuals., The authors show that kidney allocation to highly sensitized patients based on proven acceptable HLA antigens results in a significantly lower incidence of rejection episodes when compared to allocation based on the avoidance of unacceptable HLA antigens only.

Published

2019

41. Toward a sensible single antigen bead cut-off based on kidney graft survival

Author

Bram W. Wisse, Johan W. de Fijter, Shaikh A. Nurmohamed, Karlijn A M I van der Pant, N M Lardy, Ineke J. M. ten Berge, M. Gelens, Sebastiaan Heidt, Michiel L. Bots, Andries J. Hoitsma, Adriaan C.A.D. Drop, Arnold van der Meer, Luuk B. Hilbrands, Frans J. van Ittersum, Frederike J. Bemelman, Dave L. Roelen, Paul J M van der Boog, Jan-Stephan F. Sanders, Arjan D. van Zuilen, Loes Plaisier, Wendy Swelsen, Michiel G. H. Betjes, Cornelis E. Hack, Franka E. van Reekum, Elly M. van Duijnhoven, Laura Bungener, Caroline Roozendaal, Henny G. Otten, Marije C. Baas, Bouke G. Hepkema, Neelke C. van der Weerd, Christina E.M. Voorter, Frans H.J. Claas, Eric Spierings, Lotte Wieten, Wil A. Allebes, Irma Joosten, Marianne C. Verhaar, Marcel G.J. Tilanus, Annechien J. A. Lambeck, Elena G. Kamburova, Maarten H. L. Christiaans, Marc A. Seelen, Oral and Maxillofacial Surgery, Erasmus MC other, Internal Medicine, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Nephrology, ACS - Atherosclerosis & ischemic syndromes, ACS - Diabetes & metabolism, AII - Inflammatory diseases, Interne Geneeskunde, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, MUMC+: DA TI Staf (9), MUMC+: DA TI Laboratorium (9), MUMC+: MA Nefrologie (9), and APH - Aging & Later Life

Subjects

medicine.medical_specialty, Urology, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], Human leukocyte antigen, 030230 surgery, Fluorescence, 03 medical and health sciences, 0302 clinical medicine, HLA Antigens, Isoantibodies, STRENGTH, Medicine, Cutoff, Humans, Single antigen bead, Kidney transplantation, Kidney, Transplantation, business.industry, Graft Survival, Original Clinical Science—General, medicine.disease, Kidney Transplantation, Tissue Donors, body regions, HLA, medicine.anatomical_structure, Risk stratification, ANTIBODIES, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, 030211 gastroenterology & hepatology, Graft survival, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], business, Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5]

Abstract

Supplemental Digital Content is available in the text., Background. There is no consensus in the literature on the interpretation of single-antigen bead positive for a specific HLA antibody. Methods. To inform the debate, we studied the relationship between various single-antigen bead positivity algorithms and the impact of resulting donor-specific HLA antibody (DSA) positivity on long-term kidney graft survival in 3237 deceased-donor transplants. Results. First, we showed that the interassay variability can be greatly reduced when working with signal-to-background ratios instead of absolute median fluorescence intensities (MFIs). Next, we determined pretransplant DSA using various MFI cutoffs, signal-to-background ratios, and combinations thereof. The impact of the various cutoffs was studied by comparing the graft survival between the DSA-positive and DSA-negative groups. We did not observe a strong impact of various cutoff levels on 10-year graft survival. A stronger relationship between the cutoff level and 1-year graft survival for DSA-positive transplants was found when using signal-to-background ratios, most pronounced for the bead of the same HLA locus with lowest MFI taken as background. Conclusions. With respect to pretransplant risk stratification, we propose a signal-to-background ratio-6 (using the bead of the same HLA-locus with lowest MFI as background) cutoff of 15 combined with an MFI cutoff of 500, resulting in 8% and 21% lower 1- and 10-year graft survivals, respectively, for 8% DSA-positive transplants.

Published

2019

42. Complement Activation in Autoimmune Bullous Dermatoses: A Comprehensive Review

Author

Marc A. Seelen, Gilles F. H. Diercks, Martijn B. A. van Doorn, Gareth Edwards, Barbara Horváth, Jeffrey Damman, Dermatology, and Pathology

Subjects

0301 basic medicine, SUBEPIDERMAL BLISTERS, MONOCLONAL-ANTIBODY, Basement Membrane, epidermolysis bullosa acquisita, 0302 clinical medicine, Medicine, Immunology and Allergy, complement, skin and connective tissue diseases, Complement Activation, integumentary system, C4D IMMUNOHISTOCHEMISTRY, pemphigus, FORMALIN-FIXED TISSUE, Bullous pemphigoid, Epidermolysis bullosa acquisita, lcsh:Immunologic diseases. Allergy, MANNAN-BINDING LECTIN, Mini Review, Immunology, MEMBRANE ATTACK COMPLEX, ALTERNATIVE PATHWAY, Autoimmune Diseases, 03 medical and health sciences, bullous pemphigod, Animals, Humans, Autoantibodies, Skin Diseases, Vesiculobullous, business.industry, Pemphigus vulgaris, Autoantibody, dermatitis herpetiformis, Complement System Proteins, medicine.disease, Complement system, Pemphigus, XVII COLLAGEN, 030104 developmental biology, auto-immune bullous dermatosis, PASSIVE TRANSFER, Alternative complement pathway, mucus membrane pemphigoid, business, Complement membrane attack complex, lcsh:RC581-607, PEMPHIGUS-VULGARIS, 030215 immunology, linear IgA bullous dermatoses

Abstract

Autoimmune bullous dermatoses (AIBD) are characterized by circulating autoantibodies that are either directed against epidermal antigens or deposited as immune complexes in the basement membrane zone (BMZ). The complement system (CS) can be activated by autoantibodies, thereby triggering activation of specific complement pathways. Local complement activation induces a pathogenic inflammatory response that eventually results in the formation of a sub- or intraepidermal blister. Deposition of complement components is routinely used as a diagnostic marker for AIBD. Knowledge from different animal models mimicking AIBD and deposition of complement components in human skin biopsies provides more insight into the role of complement in the pathogenesis of the different AIBD. This review outlines the role of the CS in several AIBD including bullous pemphigoid, epidermolysis bullosa acquisita, mucous membrane pemphigoid (MMP), pemphigus, linear IgA-disease, and dermatitis herpetiformis. We also discuss potential therapeutic approaches targeting key complement components, pathways and pathogenic complement-mediated events.

Published

2019

43. Taming hemodialysis-induced inflammation: Are complement C3 inhibitors a viable option?

Author

Markus Huber-Lang, Edimara S. Reis, Mohamed R. Daha, Ali Reza Biglarnia, Richard J. Quigg, John D. Lambris, Marc A. Seelen, Dimitrios C. Mastellos, Meryl Waldman, Groningen Institute for Organ Transplantation (GIOT), and Groningen Kidney Center (GKC)

Subjects

0301 basic medicine, CHRONIC KIDNEY-DISEASE, medicine.medical_treatment, Immunology, Inflammation, Disease, Bioinformatics, ALTERNATIVE PATHWAY, Article, AMY-101, Proinflammatory cytokine, ACTIVATION, 03 medical and health sciences, Therapeutic approach, 0302 clinical medicine, Renal Dialysis, medicine, Humans, Immunology and Allergy, Compstatins, Cp40, Thromboinflammation, business.industry, Complement C3, medicine.disease, Complement system, Complement Inactivating Agents, 030104 developmental biology, CARDIOVASCULAR-DISEASE, Hemodialysis, Alternative complement pathway, medicine.symptom, business, SYSTEM, 030215 immunology, Kidney disease

Abstract

Owing to an increasing shortage of donor organs, the majority of patients with end-stage kidney disease remains reliant on extracorporeal hemodialysis (HD) in order to counter the lifelong complications of a failing kidney. While HD remains a life-saving option for these patients, mounting evidence suggests that it also fuels a vicious cycle of thromboinflammation that can increase the risk of cardiovascular disease. During HD, blood-borne innate immune systems become inappropriately activated on the biomaterial surface, instigating proinflammatory reactions that can alter endothelial and vascular homeostasis. Complement activation, early during the HD process, has been shown to fuel a multitude of detrimental thromboinflammatory reactions that collectively contribute to patient morbidity. Here we discuss emerging aspects of complement's involvement in HD-induced inflammation and put forth the concept that targeted intervention at the level of C3 might constitute a promising therapeutic approach in HD patients.

Published

2019

44. Effect of initial immunosuppression on long-term kidney transplant outcome in immunological low-risk patients

Author

Elizabeth M. van Duijnhoven, Arnold van der Meer, Sebastiaan Heidt, Irma Joosten, Lotte Wieten, Marianne C. Verhaar, Marije C. Baas, Mariëlle A C J Gelens, Johan W. de Fijter, Neelke C. van der Weerd, Shaikh A. Nurmohamed, Laura A. Michielsen, Elena G. Kamburova, Marcel G.J. Tilanus, Caroline Roozendaal, N M Lardy, Maarten H. L. Christiaans, Michiel G. H. Betjes, Wil A. Allebes, Paul J M van der Boog, Marc A. Seelen, Karlijn A M I van der Pant, Frans H.J. Claas, Frederike J. Bemelman, Loes Plaisier, Michiel L. Bots, Eric Spierings, Bram W. Wisse, Annechien J. A. Lambeck, Andries J. Hoitsma, Laura Bungener, Frans J. van Ittersum, Christien Voorter, Franka E. van Reekum, Adriaan C.A.D. Drop, Henderikus G. Otten, Luuk B. Hilbrands, Arjan D. van Zuilen, Bouke G. Hepkema, Cornelis E. Hack, Ineke J. M. ten Berge, Jan-Stephan F. Sanders, Dave L. Roelen, Wendy Swelsen, Nephrology, AII - Inflammatory diseases, APH - Aging & Later Life, Oral and Maxillofacial Surgery, Erasmus MC other, Internal Medicine, ACS - Atherosclerosis & ischemic syndromes, ACS - Diabetes & metabolism, Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, Interne Geneeskunde, MUMC+: DA TI Staf (9), MUMC+: DA Transplantatie Immunologie (5), MUMC+: DA TI Laboratorium (9), MUMC+: MA Nefrologie (9), and RS: NUTRIM - R3 - Respiratory & Age-related Health

Subjects

Graft Rejection, Male, Nephrology, medicine.medical_treatment, TACROLIMUS, 030232 urology & nephrology, graft survival, 030230 surgery, Kidney, Gastroenterology, DISEASE, Cohort Studies, 0302 clinical medicine, HLA Antigens, INFECTION, Medicine, FAILURE, Kidney transplantation, Netherlands, immunosuppression, RENAL-TRANSPLANTATION, Immunosuppression, Middle Aged, medicine.anatomical_structure, REJECTION, Cohort, Prednisolone, Female, MINIMIZATION, Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5], Immunosuppressive Agents, medicine.drug, Adult, medicine.medical_specialty, NEPHROPATHY, kidney transplantation, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], Disease-Free Survival, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Internal medicine, Journal Article, Humans, Immunosuppression Therapy, GRAFT-SURVIVAL, Transplantation, business.industry, Mycophenolic Acid, anti-HLA antibodies, medicine.disease, Tacrolimus, CYCLOSPORINE, Renal disorders Radboud Institute for Health Sciences [Radboudumc 11], business, immunological low-risk

Abstract

Background Few studies have evaluated the effect of different immunosuppressive strategies on long-term kidney transplant outcomes. Moreover, as they were usually based on historical data, it was not possible to account for the presence of pretransplant donor-specific human-leukocyte antigen antibodies (DSA), a currently recognized risk marker for impaired graft survival. The aim of this study was to evaluate to what extent frequently used initial immunosuppressive therapies increase graft survival in immunological low-risk patients. Methods We performed an analysis on the PROCARE cohort, a Dutch multicentre study including all transplantations performed in the Netherlands between 1995 and 2005 with available pretransplant serum (n = 4724). All sera were assessed for the presence of DSA by a luminex single-antigen bead assay. Patients with a previous kidney transplantation, pretransplant DSA or receiving induction therapy were excluded from the analysis. Results Three regimes were used in over 200 patients: cyclosporine (CsA)/prednisolone (Pred) (n = 542), CsA/mycophenolate mofetil (MMF)/Pred (n = 857) and tacrolimus (TAC)/MMF/Pred (n = 811). Covariate-adjusted analysis revealed no significant differences in 10-year death-censored graft survival between patients on TAC/MMF/Pred therapy (79%) compared with patients on CsA/MMF/Pred (82%, P = 0.88) or CsA/Pred (79%, P = 0.21). However, 1-year rejection-free survival censored for death and failure unrelated to rejection was significantly higher for TAC/MMF/Pred (81%) when compared with CsA/MMF/Pred (67%, P Conclusion These results suggest that in immunological low-risk patients excellent long-term kidney graft survival can be achieved irrespective of the type of initial immunosuppressive therapy (CsA or TAC; with or without MMF), despite differences in 1-year rejection-free survival.

Published

2019

45. Physiological hypoxia restrains the senescence-associated secretory phenotype via AMPK-mediated mTOR suppression

Author

Michela Borghesan, Boshi Wang, Konstantinos Evangelou, Thijmen van Vliet, Rossana Franzin, Simone Brandenburg, Marco Demaria, Marta Varela-Eirin, Marc A. Seelen, Vassilis G. Gorgoulis, Groningen Kidney Center (GKC), Groningen Institute for Organ Transplantation (GIOT), Damage and Repair in Cancer Development and Cancer Treatment (DARE), and Restoring Organ Function by Means of Regenerative Medicine (REGENERATE)

Subjects

AMP-Activated Protein Kinases, OXYGEN, ACTIVATION, 0302 clinical medicine, Hydroxybenzoates, Hypoxia, DAMAGE, 0303 health sciences, Antibiotics, Antineoplastic, TOR Serine-Threonine Kinases, CELLULAR SENESCENCE, Age Factors, NF-kappa B, Phenotype, Cell Hypoxia, Cell biology, PARTIAL-PRESSURE, GROWTH, Inflammation Mediators, medicine.symptom, RESTRICTION, Signal Transduction, EXPRESSION, Senescence, Glycine, Cellular senescence, Biology, DIET, 03 medical and health sciences, Paracrine signalling, Cell Line, Tumor, Paracrine Communication, medicine, Animals, Humans, Muscle Strength, Molecular Biology, PI3K/AKT/mTOR pathway, Cell Proliferation, 030304 developmental biology, Senescence-Associated Secretory Phenotype, fungi, AMPK, Cell Biology, Hypoxia (medical), Isoquinolines, Mice, Inbred C57BL, Doxorubicin, CELLS, 030217 neurology & neurosurgery

Abstract

Cellular senescence is a state of stable proliferative arrest triggered by damaging signals. Senescent cells persist during aging and promote age-related pathologies via the pro-inflammatory senescence-associated secretory phenotype (SASP), whose regulation depends on environmental factors. In vivo, a major environmental variable is oxygenation, which varies among and within tissues. Here, we demonstrate that senescent cells express lower levels of detrimental pro-inflammatory SASP factors in physiologically hypoxic environments, as measured in culture and in tissues. Mechanistically, exposure of senescent cells to low-oxygen conditions leads to AMPK activation and AMPK-mediated suppression of the mTOR-NF-kappa B signaling loop. Finally, we demonstrate that treatment with hypoxia-mimetic compounds reduces SASP in cells and tissues and improves strength in chemotherapy-treated and aged mice. Our findings highlight the importance of oxygen as a determinant for pro-inflammatory SASP expression and offer a potential new strategy to reduce detrimental paracrine effects of senescent cells.

Published

2021

46. Distinct in vitro Complement Activation by Various Intravenous Iron Preparations

Author

Mariana Gaya da Costa, Felix Poppelaars, Thomas P G de Vlaam, Casper F. M. Franssen, Julia Cordelia Hempel, Marc A. Seelen, Carlo A. J. M. Gaillard, Mohamed R. Daha, Stefan P Berger, Groningen Kidney Center (GKC), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

0301 basic medicine, Iron dextran, medicine.medical_treatment, HEMODIALYSIS-PATIENTS, Complement Membrane Attack Complex, Pharmacology, Disaccharides, Ferric Compounds, Glucaric Acid, chemistry.chemical_compound, PSEUDOALLERGY, Medicine, Complement Activation, HYPERSENSITIVITY, FERRIC GLUCONATE COMPLEX, Ferric Oxide, Saccharated, Anemia, Iron-Deficiency, Pseudoallergy, Complement activation, Dextran, Complement C3d, Nephrology, Lectin pathway, Administration, Intravenous, Iron-Dextran Complex, Hemodialysis, HUMAN SERUM, medicine.drug, Complement activation related pseudo allergy, Anemia, ADVERSE REACTIONS, In Vitro Techniques, Iron sucrose, Mannose-Binding Lectin, DEXTRAN, MECHANISMS, LECTIN PATHWAY, 03 medical and health sciences, Intravenous iron, Renal Dialysis, Hypersensitivity reaction, Humans, Maltose, Properdin, business.industry, Complement C1q, medicine.disease, Ferrosoferric Oxide, In vitro, PRODUCTS, Complement system, 030104 developmental biology, chemistry, Immunology, Hematinics, Kidney Failure, Chronic, business, Iron Compounds

Abstract

Background: Intravenous (IV) iron preparations are widely used in the treatment of anemia in patients undergoing hemodialysis (HD). All IV iron preparations carry a risk of causing hypersensitivity reactions. However, the pathophysiological mechanism is poorly understood. We hypothesize that a relevant number of these reactions are mediated by complement activation, resulting in a pseudo-anaphylactic clinical picture known as complement activation-related pseudo allergy (CARPA). Methods: First, the in-vitro complement-activating capacity was determined for 5 commonly used IV iron preparations using functional complement assays for the 3 pathways. Additionally, the preparations were tested in an ex-vivo model using the whole blood of healthy volunteers and HD patients. Lastly, in-vivo complement activation was tested for one preparation in HD patients. Results: In the in-vitro assays, iron dextran, and ferric carboxymaltose caused complement activation, which was only possible under alternative pathway conditions. Iron sucrose may interact with complement proteins, but did not activate complement in-vitro. In the ex-vivo assay, iron dextran significantly induced complement activation in the blood of healthy volunteers and HD patients. Furthermore, in the ex-vivo assay, ferric carboxymaltose and iron sucrose only caused significant complement activation in the blood of HD patients. No in-vitro or ex-vivo complement activation was found for ferumoxytol and iron isomaltoside. IV iron therapy with ferric carboxymaltose in HD patients did not lead to significant in-vivo complement activation. Conclusion: This study provides evidence that iron dextran and ferric carboxymaltose have complement-activating capacities in-vitro, and hypersensitivity reactions to these drugs could be CARPA-mediated.

Published

2016

47. How can we reduce costs of solid-phase multiplex-bead assays used to determine anti-HLA antibodies?

Author

Marije C. Baas, Christina E.M. Voorter, Maarten H. L. Christiaans, E.M. van Duijnhoven, A. J. Hoitsma, Michiel L. Bots, Marc A. Seelen, Barbara Wisse, Azam S. Nurmohamed, I. J. M. ten Berge, Sebastiaan Heidt, Frans H.J. Claas, N. C. van der Weerd, Henny G. Otten, Luuk B. Hilbrands, F. van Reekum, Marcel G.J. Tilanus, A D van Zuilen, Frederike J. Bemelman, J.W. de Fijter, Eric Spierings, Adriaan C.A.D. Drop, Elena G. Kamburova, Bouke G. Hepkema, Joris Vanderlocht, Wendy Swelsen, Annechien J. A. Lambeck, N M Lardy, Jan-Stephan F. Sanders, Irma Joosten, Dave L. Roelen, F. J. van Ittersum, Marianne C. Verhaar, Lotte Wieten, Michiel G. H. Betjes, Wil A. Allebes, P.J.M. van der Boog, Caroline Roozendaal, Loes Plaisier, Laura Bungener, K. A. M. I. van Donselaar-van der Pant, A. F. G. van der Meer, Cornelis E. Hack, and M. Gelens

Subjects

Immunology, High resolution, Context (language use), Human leukocyte antigen, 030230 surgery, Biology, Molecular biology, Transplantation, 03 medical and health sciences, 0302 clinical medicine, Genetics, biology.protein, Immunology and Allergy, 030211 gastroenterology & hepatology, Hla antibodies, Multiplex, Antibody, Single antigen bead

Abstract

Solid-phase multiplex-bead assays are widely used in transplantation to detect anti-human leukocyte antigen (HLA) antibodies. These assays enable high resolution detection of low levels of HLA antibodies. However, multiplex-bead assays are costly and yield variable measurements that limit the comparison of results between laboratories. In the context of a Dutch national Consortium study we aimed to determine the inter-assay and inter-machine variability of multiplex-bead assays, and we assessed how to reduce the assay reagents costs. Fifteen sera containing a variety of HLA antibodies were used yielding in total 7092 median fluorescence intensities (MFI) values. The inter-assay and inter-machine mean absolute relative differences (MARD) of the screening assay were 12% and 13%, respectively. The single antigen bead (SAB) inter-assay MARD was comparable, but showed a higher lot-to-lot variability. Reduction of screening assay reagents to 50% or 40% of manufacturers' recommendations resulted in MFI values comparable to 100% of the reagents, with an MARD of 12% or 14%, respectively. The MARD of the 50% and 40% SAB assay reagent reductions were 11% and 22%, respectively. From this study, we conclude that the reagents can be reliably reduced at least to 50% of manufacturers' recommendations with virtually no differences in HLA antibody assignments.

Published

2016

48. Functional Studies on Primary Tubular Epithelial Cells Indicate a Tumor Suppressor Role of SETD2 in Clear Cell Renal Cell Carcinoma

Author

Helga Westers, Joost Kluiver, Jan Osinga, Maaike B. van Werkhoven, Klaas Kok, Jun Li, Rolf H. Sijmons, Anke van den Berg, Marc A. Seelen, Groningen Institute for Organ Transplantation (GIOT), Groningen Kidney Center (GKC), Guided Treatment in Optimal Selected Cancer Patients (GUTS), Stem Cell Aging Leukemia and Lymphoma (SALL), and Translational Immunology Groningen (TRIGR)

Subjects

0301 basic medicine, Cancer Research, H3K36 TRIMETHYLATION, GENES, Tumor suppressor gene, Biology, lcsh:RC254-282, DISEASE, Malignant transformation, Small hairpin RNA, 03 medical and health sciences, medicine, E2F1, REPAIR, Gene knockdown, IDENTIFICATION, Cell growth, HUMAN KIDNEY, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, CANCER, Molecular biology, ALPHA, Clear cell renal cell carcinoma, 030104 developmental biology, SENESCENCE, Cell culture, Cancer research

Abstract

SET domain-containing 2 (SETD2) is responsible for the trimethylation of histone H3 lysine36 (H3K36me3) and is one of the genes most frequently mutated in clear cell renal cell carcinoma (ccRCC). It is located at 3p21, one copy of which is lost in the majority of ccRCC tumors, suggesting that SETD2 might function as a tumor suppressor gene. However, the manner in which loss of SETD2 contributes to ccRCC development has not been studied in renal primary tubular epithelial cells (PTECs). Therefore, we studied the consequences of SETD2 knockdown through lentiviral shRNA in human PTECs. Consistent with its known function, SETD2 knockdown (SETD-KD) led to loss of H3K36me3 in PTECs. In contrast to SETD2 wild-type PTECs, which have a limited proliferation capacity; the SETD2-KD PTECs continued to proliferate. The expression profiles of SETD2-KD PTECs showed a large overlap with the expression profile of early-passage, proliferating PTECs, whereas nonproliferating PTECs showed a significantly different expression profile. Gene set enrichment analysis revealed a significant enrichment of E2F targets in SETD2-KD and proliferating PTECs as compared with nonproliferating PTECs and in proliferating PTEC compared with SETD2-KD. The SETD2-KD PTECs maintained low expression of CDKN2A and high expression of E2F1, whereas their levels changed with continuing passages in untreated PTECs. In contrast to the nonproliferating PTECs, SETD2-KD PTECs showed no beta-galactosidase staining, confirming the protection against senescence. Our results indicate that SETD2 inactivation enables PTECs to bypass the senescence barrier, facilitating a malignant transformation toward ccRCC.

Published

2016

49. Precision-cut human kidney slices as a model to elucidate the process of renal fibrosis

Author

Theerut Luangmonkong, Jan-Luuk Hillebrands, Elisabeth G. D. Stribos, Willem J. van Son, Peter Olinga, Henricus A. M. Mutsaers, Igle J. de Jong, Anna M. Leliveld, Harry van Goor, Marc A. Seelen, Pharmaceutical Technology and Biopharmacy, Guided Treatment in Optimal Selected Cancer Patients (GUTS), Groningen Kidney Center (GKC), Vascular Ageing Programme (VAP), Groningen Institute for Organ Transplantation (GIOT), and Biopharmaceuticals, Discovery, Design and Delivery (BDDD)

Subjects

Male, 0301 basic medicine, LIVER, Gene Expression, Organic Anion Transporters, Kidney, DISEASE, Adenosine Triphosphate, 0302 clinical medicine, Transforming Growth Factor beta, Fibrosis, FAILURE, General Medicine, Middle Aged, Platelet Endothelial Cell Adhesion Molecule-1, medicine.anatomical_structure, Renal pathology, 030220 oncology & carcinogenesis, Female, Kidney Diseases, Adult, EXPRESSION, medicine.medical_specialty, FIBROBLASTS, TISSUES, OATP4C1, Biology, Collagen Type I, End stage renal disease, Nephrin, 03 medical and health sciences, Organ Culture Techniques, Organic Anion Transport Protein 1, Physiology (medical), Internal medicine, medicine, Renal fibrosis, Humans, Umbelliferones, HUMAN PODOCYTES, Aged, GLUCURONIDATION, MESENCHYMAL TRANSITION, GROWTH-FACTOR-BETA, Biochemistry (medical), Public Health, Environmental and Occupational Health, medicine.disease, Collagen Type I, alpha 1 Chain, 030104 developmental biology, Endocrinology, biology.protein, Biomarkers, Kidney disease

Abstract

Chronic kidney disease is a major health concern, and experimental models bridging the gap between animal studies and clinical research are currently lacking. Here, we evaluated precision-cut kidney slices (PCKSs) as a potential model for renal disease. PCKSs were prepared from human cortical tissue obtained from tumor nephrectomies and cultured up to 96 hours. Morphology, cell viability, and metabolic functionality (ie, uridine 5'-diphospho-glucuronosyltransferase and transporter activity) were determined to assess the integrity of PCKSs. Furthermore, inflammatory and fibrosis-related gene expressions were characterized. Finally, to validate the model, renal fibrogenesis was induced using transforming growth factor beta 1 (TGF-beta 1). Preparation of PCKSs induced an inflammatory tissue response, whereas long-term incubation (96 hours) induced fibrogenesis as shown by an increased expression of collagen type 1A1 (COL1A1) and fibronectin 1 (FN1). Importantly, PCKSs remained functional for more than 48 hours as evidenced by active glucuronidation and phenolsulfonphthalein uptake. In addition, cellular diversity appeared to be maintained, yet we observed a clear loss of nephrin messenger RNA levels suggesting that our model might not be suitable to study the role of podocytes in renal pathology. Moreover, TGF-beta 1 exposure augmented fibrosis, as illustrated by an increased expression of multiple fibrosis markers including COL1A1, FN1, and alpha-smooth muscle actin. In conclusion, PCKSs maintain their renal phenotype during culture and appear to be a promising model to investigate renal diseases, for example, renal fibrosis. Moreover, the human origin of PCKSs makes this model very suitable for translational research.

Published

2016

50. Complement Activation in Inflammatory Skin Diseases

Author

Robert Rissmann, Jenny Giang, Martijn B. A. van Doorn, Marc A. Seelen, Errol P. Prens, Jeffrey Damman, Pathology, and Dermatology

Subjects

bullous pemphigoid, 0301 basic medicine, HUMAN KERATINOCYTES PRODUCE, Dermatitis, Review, 030207 dermatology & venereal diseases, 0302 clinical medicine, Immunology and Allergy, Medicine, complement, Molecular Targeted Therapy, SYSTEMIC-LUPUS-ERYTHEMATOSUS, Complement Activation, innate immunity, Skin, URTICARIAL VASCULITIS SYNDROME, psoriasis, FORMALIN-FIXED TISSUE, Complement (complexity), Antibody opsonization, dermatology, ACNE-VULGARIS, skin diseases, medicine.symptom, lcsh:Immunologic diseases. Allergy, LEUKOCYTOCLASTIC VASCULITIS, Immunology, Inflammation, SMALL-VESSEL VASCULITIS, 03 medical and health sciences, Immune system, Animals, Humans, Immune Complex Diseases, Autoantibodies, Innate immune system, business.industry, Immune complex clearance, hidradenitis suppurativa, Complement System Proteins, Complement system, 030104 developmental biology, CUTANEOUS VASCULITIS, business, lcsh:RC581-607, CHRONIC IDIOPATHIC URTICARIA, lupus erythematosus, Immune complex disease

Abstract

The complement system is a fundamental part of the innate immune system, playing a crucial role in host defense against various pathogens, such as bacteria, viruses, and fungi. Activation of complement results in production of several molecules mediating chemotaxis, opsonization, and mast cell degranulation, which can contribute to the elimination of pathogenic organisms and inflammation. Furthermore, the complement system also has regulating properties in inflammatory and immune responses. Complement activity in diseases is rather complex and may involve both aberrant expression of complement and genetic deficiencies of complement components or regulators. The skin represents an active immune organ with complex interactions between cellular components and various mediators. Complement involvement has been associated with several skin diseases, such as psoriasis, lupus erythematosus, cutaneous vasculitis, urticaria, and bullous dermatoses. Several triggers including auto-antibodies and micro-organisms can activate complement, while on the other hand complement deficiencies can contribute to impaired immune complex clearance, leading to disease. This review provides an overview of the role of complement in inflammatory skin diseases and discusses complement factors as potential new targets for therapeutic intervention.

Published

2018