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

Author

Poppelaars F, Gaya da Costa M, Faria B, Eskandari SK, Seelen MA, and Damman J

Subjects
cytokines, kidney transplantation, nephrology, genetics, Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950
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

6. Complement activation in Hidradenitis suppurativa:Covert low-grade inflammation or innocent bystander?

Author

van Straalen, K. R., Dudink, K., Aarts, P., van der Zee, H. H., van den Bosch, T. P.P., Giang, J., Prens, E. P., Damman, J., van Straalen, K. R., Dudink, K., Aarts, P., van der Zee, H. H., van den Bosch, T. P.P., Giang, J., Prens, E. P., and Damman, J.

Abstract

Hidradenitis suppurativa (HS) is a chronic auto-inflammatory skin disease with a complex and multifactorial pathogenesis involving both the innate and adaptive immune system. Despite limited evidence for local complement activation, conflicting results have been published on the role of systemic complement activation in HS. It was hypothesized that complement was consumed in highly inflamed HS skin, trapping complement from the circulation. Therefore, the aim of this study was to evaluate this local complement deposition in HS skin lesions using routine and commonly used complement antibodies.Direct immunofluorescence for C1q, C3c, C4d, C5b-9, and properdin was performed on frozen tissue sections of 19 HS patients and 6 controls. C5a receptor 1 (C5aR1) was visualized using immunohistochemistry. Overall, we found no significant local complement deposition in HS patients versus controls regarding C1q, C3c, C4d, C5b-9, or properdin on either vessels or immune cells. C5aR1 expression was exclusively found on immune cells, predominantly neutrophilic granulocytes, but not significantly different relatively to the total infiltrate in HS lesions compared with controls. In conclusion, despite not being able to confirm local complement depositions of C1q, C3c, C4d, or properdin using highly sensitive and widely accepted techniques, the increased presence of C5aR1 positive immune cells in HS suggests the importance of complement in the pathogenesis of HS and supports emerging therapies targeting this pathway.

Published
2022

11. Structured analysis of histopathological characteristics of vulvar lichen sclerosus in a juvenile population

Author

Morrel, B. (B.), Ewing, P.C. (Patricia), van der Avoort, I.A.M., Pasmans, S.G.M.A. (Suzanne), Damman, J. (Jeffrey), Morrel, B. (B.), Ewing, P.C. (Patricia), van der Avoort, I.A.M., Pasmans, S.G.M.A. (Suzanne), and Damman, J. (Jeffrey)

Abstract

Genital lichen sclerosus (LS), a chronic noninfectious dermatosis, is not rare in pediatric dermatology. The histopathological diagnosis in children and adults in both genital and nongenital LS is considered to be the same and encompasses a broad range of possible characteristics. Clinical manifestations and treatment options of genital LS in children are different depending on gender. The vast majority of boys are treated with circumcision, making for a larger amount of information on the histopathology of genital LS in boys, whereas substantial information on the histopathology of juvenile vulvar LS is lacking. In girls, vulvar LS almost always persists beyond puberty and, therefore, presents a particular challenge to clinicians and cause for concern for the patient. Vulvar LS in childhood and adolescence (juveniles) is underreported, and there are uncertainties with regard to the long-term course of the disease when it occurs at an age when the vulva is still developing. The present study investigates biopsie

Published
2020
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12. Een patiënt met een granulomateuze ontstekingsreactie ter plaatse van een tatoeage en een panuveïtis

Author

Wennekers, M.M. (Mèdelyn M.), Damman, J. (Jeffrey), Doorn, M.B.A. (Martijn) van, Wennekers, M.M. (Mèdelyn M.), Damman, J. (Jeffrey), and Doorn, M.B.A. (Martijn) van

Abstract

Tatoeages zijn cosmetische versieringen van de huid die we steeds vaker om ons heen zien. Desondanks is dat niet zonder risico op complicaties. Wij presenteren een patiënte die een granulomateuze reactie ontwikkelde in specifieke delen van haar tatoeage, jaren nadat deze was geplaatst. Wegens een co-existente panuveïtis werd de diagnose sarcoïdose overwogen.

Published
2020

13. 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

Damman, J. (Jeffrey), Mooyaart, A.L. (Antien), Seelen, M.A., Doorn, M.B.A. (Martijn) van, Damman, J. (Jeffrey), Mooyaart, A.L. (Antien), Seelen, M.A., and Doorn, M.B.A. (Martijn) van

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 HUVand 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.

Published
2020
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15. Influence of probenecid on the pharmacokinetics and pharmacodynamics of sorafenib

Author

Hussaarts, K.G.A.M. (Koen), Doorn, L. (Leni) van, Eechoute, K. (Karel), Damman, J. (Jeffrey), Fu, Q. (Qiang), van Doorn, N. (Nadia), Eisenmann, E.D. (Eric D.), Gibson, A.A., Hoop, E.O. (Esther Oomen-De), Bruijn, P.J. (Peter) de, Baker, S.D. (Sharyn), Koolen, S.L.W. (Stijn), Gelder, T. (Teun) van, Leeuwen, R.W.F. (Roelof) van, Mathijssen, A.H.J. (Ron), Sparreboom, A. (Alex), Bins, S. (Sander), Hussaarts, K.G.A.M. (Koen), Doorn, L. (Leni) van, Eechoute, K. (Karel), Damman, J. (Jeffrey), Fu, Q. (Qiang), van Doorn, N. (Nadia), Eisenmann, E.D. (Eric D.), Gibson, A.A., Hoop, E.O. (Esther Oomen-De), Bruijn, P.J. (Peter) de, Baker, S.D. (Sharyn), Koolen, S.L.W. (Stijn), Gelder, T. (Teun) van, Leeuwen, R.W.F. (Roelof) van, Mathijssen, A.H.J. (Ron), Sparreboom, A. (Alex), and Bins, S. (Sander)

Abstract

Prior studies have demonstrated an organic anion transporter 6 (OAT6)-mediated accumulation of sorafenib in keratinocytes. The OAT6 inhibitor probenecid decreases sorafenib uptake in skin and might, therefore, decrease sorafenib-induced cutaneous adverse events. Here, the influence of probenecid on sorafenib pharmacokinetics and toxicity was investigated. Pharmacokinetic sampling was performed in 16 patients on steady-state sorafenib treatment at days 1 and 15 of the study. Patients received sorafenib (200–800 mg daily) in combination with probenecid (500 mg two times daily (b.i.d.)) on days 2–15. This study was designed to determine bioequivalence with geometric mean Area under the curve from zero to twelve hours (AUC0–12 h) as primary endpoint. During concomitant probenecid, so

Published
2020
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18. Trichoblastic carcinosarcoma with panfollicular differentiation (panfollicular carcinosarcoma) and CTNNB1 (beta-catenin) mutation

Author

Giang, J., Biswas, A. (Asok), Mooyaart, A.L. (Antien), Groenendijk, F.H. (Floris H.), Dikrama, P.K. (Petra), Damman, J. (Jeffrey), Giang, J., Biswas, A. (Asok), Mooyaart, A.L. (Antien), Groenendijk, F.H. (Floris H.), Dikrama, P.K. (Petra), and Damman, J. (Jeffrey)

Abstract

We present a case of trichoblastic carcinosarcoma with panfollicular differentiation. An 80-year-old man presented with a lesion on the left ear, which had

Published
2020
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23. Clinical and histopathological characterization of paradoxical head and neck erythema in patients with atopic dermatitis treated with dupilumab: a case series

Author

de Wijs, L.E.M. (L. E.M.), Nguyen, N.T. (N. T.), Kunkeler, A.C.M., Nijsten, T.E.C. (Tamar), Damman, J. (Jeffrey), Hijnen, D.-J. (Dirk-Jan), de Wijs, L.E.M. (L. E.M.), Nguyen, N.T. (N. T.), Kunkeler, A.C.M., Nijsten, T.E.C. (Tamar), Damman, J. (Jeffrey), and Hijnen, D.-J. (Dirk-Jan)

Abstract

Dupilumab is the first biologic registered for the treatment of atopic dermatitis (AD). We report on seven patients with AD presenting with a paradoxical head and neck erythema that appeared 10–39 weeks after the start of dupilumab treatment. The patients presented with a relatively sharply demarcated, patchy erythema in the head and neck area that showed no or less scaling compared with their usual eczema. Only one patient experienced symptoms of itch and burning, although this was notably different from his pre-existent facial AD. Except for a notable ‘red face’, eczema on other body parts had greatly improved in six of the seven patients, with a mean numerical rating scale for treatment satisfaction of 9 out of 10 at the time of biopsy. Treatment of the erythema with topical and systemic drugs was unsuccessful. Despite the presence of this erythema, none of our patients discontinued dupilumab treatment. Lesional skin biopsies showed an increased number of ectatic capillaries, and a perivascular lymphohistiocytic infiltration in all patients. In addition, epidermal hyperplasia with elongation of the rete ridges was observed in four patients, resembling a psoriasiform dermatitis. Additional immunohistochemical stainings revealed increased numbers of plasma cells, histiocytes and T lymphocytes. Interestingly, spongiosis was largely absent in all biopsies. We report on patients with AD treated with dupilumab developing a paradoxical erythema in a head and neck distribution. Both clinically and histopathologically we found a heterogeneous response, which was most suggestive of a drug-induced skin reaction.

Published
2019
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24. Banff lesions and renal allograft survival in chronic-active antibody mediated rejection

Author

Sablik, K.A. (Kasia), Clahsen-van Groningen, M.C. (Marian), Damman, J. (Jeffrey), Roelen, D.L. (Dave), Betjes, M.G.H. (Michiel), Sablik, K.A. (Kasia), Clahsen-van Groningen, M.C. (Marian), Damman, J. (Jeffrey), Roelen, D.L. (Dave), and Betjes, M.G.H. (Michiel)

Abstract

Aims: Chronic-active antibody mediated rejection (c-aABMR) is a major cause of kidney graft loss. Currently, little is known about the relation between histopathologic parameters and renal allograft survival. Methods and results: Between 2008 and 2014, 41 patients with a progressive decrease in renal function were diagnosed with c-aABMR according to Banff 2015 and followed up for at least 3 years. Clinical and renal biopsy characteristics were analyzed for association with graft survival. During follow-up 26 cases lost their graft because of c-aABMR at a median follow up of 40 months after diagnosis. Cases with v-lesions in their biopsy had a significant higher loss of eGFR prior to diagnosis. The total inflammation score (r = −0.45 p =.007) and the severity of interstitial fibrosis (r = −0.38 p =.023) were related to the eGFR at time of biopsy. Univariate regression analysis showed that eGFR at time of biopsy, total inflammation, interstitial fibrosis and the sum chronicity score were significantly related to the risk for graft failure during follow-up. In a multivariate analysis only the severity of interstitial fibrosis remained associated with decreased graft survival (HR 1.9 per score point, 95% CI 1.2–2.8, p =.004). Conclusion: Severity of renal interstitial fibrosis and not inflammation predicts graft survival in cases of c-aABMR.

Published
2019
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25. Treatment with intravenous immunoglobulins and methylprednisolone may significantly decrease loss of renal function in chronic-active antibody-mediated rejection

Author

Sablik, K.A. (Kasia), Clahsen-van Groningen, M.C. (Marian), Looman, C.W.N. (Caspar), Damman, J. (Jeffrey), Agteren, M. (Madelon), Betjes, M.G.H. (Michiel), Sablik, K.A. (Kasia), Clahsen-van Groningen, M.C. (Marian), Looman, C.W.N. (Caspar), Damman, J. (Jeffrey), Agteren, M. (Madelon), and Betjes, M.G.H. (Michiel)

Abstract

Background: Chronic-active antibody mediated rejection (c-aABMR) is a major contributor to long-term kidney allograft loss. We conducted a retrospective analysis to establish the efficacy of treatment with intravenous immunoglobulins (IVIG) and pulse methylprednisolone (MP) of patients with c-aABMR. Methods: Sixty-nine patients, in the period 2005-2017, with the diagnosis (suspicious for) c-aABMR that were treated with IVIG and MP were included. Patients were administered three doses of 1 g intravenous MP combined with a single dose of IVIG (1 g/kg body weight). Primary outcome was the decline in allograft function one year post treatment. Responders to IVIG-MP therapy were defined by an eGFR one year after treatment which was at least 25% above the projected allograft function. Results: Patients showed an average decline in eGFR of 9.8 ml/min/1.73m2 the year prior to treatment. Following treatment, a significant reduction (p < 0.001) in eGFR decline was observed (6.3 ml/min/1.73m2). Furthermore, a significant improvement in proteinuria was observed upon treatment (p < 0.001). Sixty-two percent (n = 43) of the patients were considered a responder and showed considerable slowing of graft function deterioration in the year after treatment (p < 0.001). Three and 5-year graft survival was significantly superior in responders. Conclusions: More than 60% of patients with c-aABMR with a progressive decline in eGFR respond favorably to treatment with IVIG-MP resulting in a significant improvement of graft survival (Sablik, Am J Transplant 18, 2018).

Published
2019
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26. Complement activation in autoimmune bullous dermatoses: A comprehensive review

Author

Edwards, G. (Gareth), Diercks, G.F.H., Seelen, M.A.J., Horvath, B.H. (Barbara), Doorn, M.B.A. (Martijn) van, Damman, J. (Jeffrey), Edwards, G. (Gareth), Diercks, G.F.H., Seelen, M.A.J., Horvath, B.H. (Barbara), Doorn, M.B.A. (Martijn) van, and Damman, J. (Jeffrey)

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
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27. Trans-ethnic kidney function association study reveals putative causal genes and effects on kidney-specific disease aetiologies

Author

Morris, AP, Le, TH, Wu, H, Akbarov, A, van der Most, PJ, Hemani, G, Smith, GD, Mahajan, A, Gaulton, KJ, Nadkarni, GN, Valladares-Salgado, A, Wacher-Rodarte, N, Mychaleckyj, JC, Dueker, ND, Guo, X, Hai, Y, Haessler, J, Kamatani, Y, Stilp, AM, Zhu, G, Cook, JP, Arnlov, J, Blanton, SH, de Borst, MH, Bottinger, EP, Buchanan, TA, Cechova, S, Charchar, FJ, Chu, P-L, Damman, J, Eales, J, Gharavi, AG, Giedraitis, V, Heath, AC, Ipp, E, Kiryluk, K, Kramer, HJ, Kubo, M, Larsson, A, Lindgren, CM, Lu, Y, Madden, PAF, Montgomery, GW, Papanicolaou, GJ, Raffel, LJ, Sacco, RL, Sanchez, E, Stark, H, Sundstrom, J, Taylor, KD, Xiang, AH, Zivkovic, A, Lind, L, Ingelsson, E, Martin, NG, Whitfield, JB, Cai, J, Laurie, CC, Okada, Y, Matsuda, K, Kooperberg, C, Chen, Y-DI, Rundek, T, Rich, SS, Loos, RJF, Parra, EJ, Cruz, M, Rotter, J, Snieder, H, Tomaszewski, M, Humphreys, BD, Franceschini, N, Morris, AP, Le, TH, Wu, H, Akbarov, A, van der Most, PJ, Hemani, G, Smith, GD, Mahajan, A, Gaulton, KJ, Nadkarni, GN, Valladares-Salgado, A, Wacher-Rodarte, N, Mychaleckyj, JC, Dueker, ND, Guo, X, Hai, Y, Haessler, J, Kamatani, Y, Stilp, AM, Zhu, G, Cook, JP, Arnlov, J, Blanton, SH, de Borst, MH, Bottinger, EP, Buchanan, TA, Cechova, S, Charchar, FJ, Chu, P-L, Damman, J, Eales, J, Gharavi, AG, Giedraitis, V, Heath, AC, Ipp, E, Kiryluk, K, Kramer, HJ, Kubo, M, Larsson, A, Lindgren, CM, Lu, Y, Madden, PAF, Montgomery, GW, Papanicolaou, GJ, Raffel, LJ, Sacco, RL, Sanchez, E, Stark, H, Sundstrom, J, Taylor, KD, Xiang, AH, Zivkovic, A, Lind, L, Ingelsson, E, Martin, NG, Whitfield, JB, Cai, J, Laurie, CC, Okada, Y, Matsuda, K, Kooperberg, C, Chen, Y-DI, Rundek, T, Rich, SS, Loos, RJF, Parra, EJ, Cruz, M, Rotter, J, Snieder, H, Tomaszewski, M, Humphreys, BD, and Franceschini, N

Abstract

Chronic kidney disease (CKD) affects ~10% of the global population, with considerable ethnic differences in prevalence and aetiology. We assemble genome-wide association studies of estimated glomerular filtration rate (eGFR), a measure of kidney function that defines CKD, in 312,468 individuals of diverse ancestry. We identify 127 distinct association signals with homogeneous effects on eGFR across ancestries and enrichment in genomic annotations including kidney-specific histone modifications. Fine-mapping reveals 40 high-confidence variants driving eGFR associations and highlights putative causal genes with cell-type specific expression in glomerulus, and in proximal and distal nephron. Mendelian randomisation supports causal effects of eGFR on overall and cause-specific CKD, kidney stone formation, diastolic blood pressure and hypertension. These results define novel molecular mechanisms and putative causal genes for eGFR, offering insight into clinical outcomes and routes to CKD treatment development.

Published
2019

30. Dermatopathologie

Author

Middelburg, T.A. (Tom), Schrader, A.M.R. (Anne-Roos), Dikrama, P.K. (Petra), Damman, J. (J.), Middelburg, T.A. (Tom), Schrader, A.M.R. (Anne-Roos), Dikrama, P.K. (Petra), and Damman, J. (J.)

Published
2018

32. Clinical and histopathological characterization of paradoxical head and neck erythema in patients with atopic dermatitis treated with dupilumab: a case series.

Author

Wijs, L.E.M., Nguyen, N.T., Kunkeler, A.C.M., Nijsten, T., Damman, J., and Hijnen, D.J.

Subjects
ATOPIC dermatitis, ERYTHEMA, T cells, NECK, PLASMA cells, PLASMACYTOMA, ERYTHEMA multiforme
Abstract

Summary: Dupilumab is the first biologic registered for the treatment of atopic dermatitis (AD). We report on seven patients with AD presenting with a paradoxical head and neck erythema that appeared 10–39 weeks after the start of dupilumab treatment. The patients presented with a relatively sharply demarcated, patchy erythema in the head and neck area that showed no or less scaling compared with their usual eczema. Only one patient experienced symptoms of itch and burning, although this was notably different from his pre‐existent facial AD. Except for a notable 'red face', eczema on other body parts had greatly improved in six of the seven patients, with a mean numerical rating scale for treatment satisfaction of 9 out of 10 at the time of biopsy. Treatment of the erythema with topical and systemic drugs was unsuccessful. Despite the presence of this erythema, none of our patients discontinued dupilumab treatment. Lesional skin biopsies showed an increased number of ectatic capillaries, and a perivascular lymphohistiocytic infiltration in all patients. In addition, epidermal hyperplasia with elongation of the rete ridges was observed in four patients, resembling a psoriasiform dermatitis. Additional immunohistochemical stainings revealed increased numbers of plasma cells, histiocytes and T lymphocytes. Interestingly, spongiosis was largely absent in all biopsies. We report on patients with AD treated with dupilumab developing a paradoxical erythema in a head and neck distribution. Both clinically and histopathologically we found a heterogeneous response, which was most suggestive of a drug‐induced skin reaction. What's already known about this topic? Dupilumab has proven to be an efficacious and effective treatment for atopic dermatitis with an acceptable safety profile.The most frequently observed side‐effects in patients with atopic dermatitis treated with dupilumab are conjunctivitis, herpes infections and injection‐site reactions. What does this study add? For the first time, we report on patients with atopic dermatitis treated with dupilumab who developed a paradoxical, mainly asymptomatic erythema in a head and neck distribution.Histological examination of skin biopsies revealed a psoriasiform reaction pattern suggestive of a drug‐induced skin reaction. [ABSTRACT FROM AUTHOR]

Published
2020
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34. ANGIOPOIETIN IN LIVING AND DECEASED BRAIN DEAD KIDNEY DONORS

Author

Westendorp, WH, Koudstaal, LG, Damman, J, Burgerhof, JG, Seelen, MA, Goor, HV, Ploeg, RJ, Leuvenink, HG, Life Course Epidemiology (LCE), Groningen Institute for Organ Transplantation (GIOT), and Groningen Kidney Center (GKC)

Published
2016

45. Functional EPO gene polymorphism rs1617640 affects graft survival after deceased donor kidney transplantation

Author

van Rijt, W.G., primary, Damman, J., additional, Snieder, H., additional, Seelen, M., additional, van Goor, H., additional, Navis, G., additional, van den Born, J., additional, de Borst, M.H., additional, Hepkema, B.G., additional, Hillebrands, J.L., additional, Ploeg, R.J., additional, Bakker, S.J.L., additional, and Leuvenink, H.G.D., additional

Published
2014
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46. CUBN as a novel locus for end-stage renal disease: insights from renal transplantation.

Author

Reznichenko, A., Snieder, H., Born, J. van den, Borst, M.H. de, Damman, J., Dijk, M.C.R.F. van, Goor, H. van, Hepkema, B.G., Hillebrands, J.L., Leuvenink, H.G., Niesing, J., Bakker, S.J., Seelen, M., Navis, G., Reznichenko, A., Snieder, H., Born, J. van den, Borst, M.H. de, Damman, J., Dijk, M.C.R.F. van, Goor, H. van, Hepkema, B.G., Hillebrands, J.L., Leuvenink, H.G., Niesing, J., Bakker, S.J., Seelen, M., and Navis, G.

Abstract

Contains fulltext : 110462.pdf (publisher's version ) (Open Access), Chronic kidney disease (CKD) is a complex disorder. As genome-wide association studies identified cubilin gene CUBN as a locus for albuminuria, and urinary protein loss is a risk factor for progressive CKD, we tested the hypothesis that common genetic variants in CUBN are associated with end-stage renal disease (ESRD) and proteinuria. First, a total of 1142 patients with ESRD, admitted for renal transplantation, and 1186 donors were genotyped for SNPs rs7918972 and rs1801239 (case-control study). The rs7918972 minor allele frequency (MAF) was higher in ESRD patients comparing to kidney donors, implicating an increased risk for ESRD (OR 1.39, p = 0.0004) in native kidneys. Second, after transplantation recipients were followed for 5.8 [3.8-9.2] years (longitudinal study) documenting ESRD in transplanted kidneys--graft failure (GF). During post-transplant follow-up 92 (9.6%) cases of death-censored GF occurred. Donor rs7918972 MAF, representing genotype of the transplanted kidney, was 16.3% in GF vs 10.7% in cases with functioning graft. Consistently, a multivariate Cox regression analysis showed that donor rs7918972 is a predictor of GF, although statistical significance was not reached (HR 1.53, p = 0.055). There was no association of recipient rs7918972 with GF. Rs1801239 was not associated with ESRD or GF. In line with an association with the outcome, donor rs7918972 was associated with elevated proteinuria levels cross-sectionally at 1 year after transplantation. Thus, we identified CUBN rs7918972 as a novel risk variant for renal function loss in two independent settings: ESRD in native kidneys and GF in transplanted kidneys.

Published
2012

47. Lectin complement pathway gene profile of the donor and recipient does not influence graft outcome after kidney transplantation.

Author

Damman, J., Kok, J.L., Snieder, H., Leuvenink, H.G., Goor, H. van, Hillebrands, J.L., Dijk, M.C.R.F. van, Hepkema, B.G., Reznichenko, A., Born, J. van den, Borst, M.H. de, Bakker, S.J., Navis, G.J., Ploeg, R.J., Seelen, M.A., Damman, J., Kok, J.L., Snieder, H., Leuvenink, H.G., Goor, H. van, Hillebrands, J.L., Dijk, M.C.R.F. van, Hepkema, B.G., Reznichenko, A., Born, J. van den, Borst, M.H. de, Bakker, S.J., Navis, G.J., Ploeg, R.J., and Seelen, M.A.

Abstract

01 februari 2012, Contains fulltext : 108497.pdf (publisher's version ) (Closed access), In kidney transplantation, complement activation was found to be induced by donor brain death, renal ischemia-reperfusion injury and allograft rejection. There are three known pathways of complement activation: the classical, lectin and the alternative pathway. The lectin complement pathway can be activated upon pattern recognition by mannan binding lectin (MBL) or ficolins (FCN). Single nucleotide polymorphisms (SNPs) in the genes encoding the lectin pathway proteins determine their functional activity and serum levels. The aim of this study was to investigate the role of the lectin gene profile of the donor and recipient on post-transplant outcome. A total of 12 functional SNPs in the MBL2, FCN2 and MBL-associated serine proteases 2 (MASP2) genes of 1271 donor-recipient pairs were determined. Lectin genotypic variants were analyzed for association with primary non-function (PNF), delayed graft function (DGF), biopsy proven acute rejection, death-censored graft survival and patient survival. Multivariate analyses found no association of donor and recipient MBL2 and MASP2 genotype with allograft outcome. Analysis of separate functional SNPs and haplotypes in the FCN2 gene of the donor and recipient did not reveal an association with transplant outcome. Also, the joint effect of the MBL2 and FCN2 genotype was not associated with allograft outcome.This study shows that the genetic profile of the lectin pathway of complement activation of the donor and recipient is not associated with allograft outcome after kidney transplantation.

Published
2012

48. Op weg naar kritisch democratisch burgerschap?

Author

Damman, J., Koster, B. (Thesis Advisor), Damman, J., and Koster, B. (Thesis Advisor)

Abstract

Onderzoek naar burgerschapsvorming op het Griftland college Wat zijn de wettelijke vereisten? Wat gebeurt er al? Wat is de schooleigen kijk op dit thema en wat moet er dan in het verlengde daarvan nog gebeuren?

Published
2008

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