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1. Nefrologie

Author

Cransberg, K., van den Hoek, J., Derksen-Lubsen, G., editor, Moll, H.A., editor, Oudesluys-Murphy, A.M., editor, Sprij, A.J., editor, Bolt-Wieringa, J.W., editor, van den Elzen, A.P.M., editor, Leeuwenburgh-Pronk, W.G., editor, Ropers, F.G., editor, and Verhoeven, J.J., editor

Published
2018
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9. A Population Pharmacokinetic Model Does Not Predict the Optimal Starting Dose of Tacrolimus in Pediatric Renal Transplant Recipients in a Prospective Study: Lessons Learned and Model Improvement

Author

Andrews, L.M., Winter, B.C. de, Cornelissen, E.A.M., Jong, H. de, Hesselink, D.A., Schreuder, M.F., Bruggemann, R.J.M., Gelder, T. van, Cransberg, K., Andrews, L.M., Winter, B.C. de, Cornelissen, E.A.M., Jong, H. de, Hesselink, D.A., Schreuder, M.F., Bruggemann, R.J.M., Gelder, T. van, and Cransberg, K.

Abstract

Contains fulltext : 220506.pdf (Publisher’s version ) (Open Access), BACKGROUND AND OBJECTIVE: Bodyweight-based dosing of tacrolimus is considered standard care. Currently, at first steady state, a third of pediatric kidney transplant recipients has a tacrolimus pre-dose concentration within the target range. We investigated whether adaptation of the starting dose according to a validated dosing algorithm could increase this proportion. METHODS: This was a multi-center, single-arm, prospective trial with a planned interim analysis after 16 patients, in which the tacrolimus starting dose was based on bodyweight, cytochrome P450 3A5 genotype, and donor status (living vs. deceased donor). RESULTS: At the interim analysis, 31% of children had a tacrolimus pre-dose concentration within the target range. As the original dosing algorithm was poorly predictive of tacrolimus exposure, the clinical trial was terminated prematurely. Next, the original model was improved by including the data of the children included in this trial, thereby doubling the number of children in the model building cohort. Data were best described with a two-compartment model with inter-individual variability, allometric scaling, and inter-occasion variability on clearance. Cytochrome P450 3A5 genotype, hematocrit, and creatinine influenced the tacrolimus clearance. A new starting dose model was developed in which the cytochrome P450 3A5 genotype was incorporated. Both models were successfully internally and externally validated. CONCLUSIONS: The weight-normalized starting dose of tacrolimus should be higher in patients with a lower bodyweight and in those who are cytochrome P450 3A5 expressers.

Published
2020

10. Use of amlodipine oral solution for the treatment of hypertension in children

Author

Vossen, A.C.T.M., Cransberg, K., Winter, B.C. de, Schreuder, M.F., Rooij-Kouwenhoven, R.W.G. van, Vulto, A.G., Hanff, L.M., Vossen, A.C.T.M., Cransberg, K., Winter, B.C. de, Schreuder, M.F., Rooij-Kouwenhoven, R.W.G. van, Vulto, A.G., and Hanff, L.M.

Abstract

Contains fulltext : 220736.pdf (Publisher’s version ) (Closed access), Background Amlodipine is a widely used antihypertensive agent for the treatment of paediatric hypertension, but the commercially available tablets are not suitable to treat young patients, who need lower, flexible dosages and a liquid formulation. Objective To determine the pharmacokinetic properties of amlodipine and the acceptability of a standardised, extemporaneous oral solution. Method A newly developed liquid formulation of amlodipine was administered to hypertensive children between the age of 6 months and 11 years. Using a limited sampling strategy, population PK analysis was performed using nonlinear mixed effects modelling. Results Nine children, with a median age of 2.9 years (IQR 1.8-8.4), receiving stable amlodipine therapy in a median dose of 0.15 mg kg(-1) day(-1) (IQR 0.11-0.18), were switched to study medication. The population pharmacokinetic model was able to accurately predict the clearance of amlodipine in the study population. Based on the final model, clearance was reduced by 31.2% (RSE: 10%) in females. Patient reported outcomes on taste from a five-point hedonic scale were available for five patients, who scored the taste from positive to slightly negative. Conclusion The results from the PK study and the acceptability assessment show that the amlodipine oral solution presented in this study offers an appropriate treatment option for young children.

Published
2020

11. Epidemiology and Outcome of Critically Ill Pediatric Cancer and Hematopoietic Stem Cell Transplant Patients Requiring Continuous Renal Replacement Therapy: A Retrospective Nationwide Cohort Study

Author

Raymakers-Janssen, P., Lilien, M. (Marc), Tibboel, D. (Dick), Kneyber, M.C.J., Dijkstra, S., Woensel, J.B. (Job) van, Lemson, J. (J.), Cransberg, K. (Karlien), Heuvel-Eibrink, M.M. (Marry) van den, Wösten-van Asperen, R.M. (Roelie), van Woensel, J., Bem, R., van Heerden, M., Riedijk, M.A. (Maaike), de Hoog, M., Verbruggen, S.C.A.T. (Sascha), Kneyber, M., Van Waardenburg, D, Roeleveld, N. (Nel), Raymakers-Janssen, P., Lilien, M. (Marc), Tibboel, D. (Dick), Kneyber, M.C.J., Dijkstra, S., Woensel, J.B. (Job) van, Lemson, J. (J.), Cransberg, K. (Karlien), Heuvel-Eibrink, M.M. (Marry) van den, Wösten-van Asperen, R.M. (Roelie), van Woensel, J., Bem, R., van Heerden, M., Riedijk, M.A. (Maaike), de Hoog, M., Verbruggen, S.C.A.T. (Sascha), Kneyber, M., Van Waardenburg, D, and Roeleveld, N. (Nel)

Abstract

Objective: Acute kidney injury requiring continuous renal replacement therapy is a serious treatment-related complication in pediatric cancer and hematopoietic stem cell transplant patients. The purpose of this study was to assess epidemiology and outcome of these patients requiring continuous renal replacement therapy in the PICU. Design: A nationwide, multicenter, retrospective, observational study. Setting: Eight PICUs of a tertiary care hospitals in the Netherlands. Patients: Pediatric cancer and hematopoietic stem cell transplant

Published
2019
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12. Abstract P-286

Author

Raymakers-Janssen, P., primary, Tibboel, D., additional, Cransberg, K., additional, Kneyber, M., additional, van den Heuvel-Eibrink, M., additional, Lilien, M., additional, and Wösten-van Asperen, R., additional

Published
2018
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13. A Population Pharmacokinetic Model to Predict the Individual Starting Dose of Tacrolimus Following Pediatric Renal Transplantation

Author

Andrews, L.M. (Louise), Hesselink, D.A. (Dennis), Gelder, T. (Teun) van, Koch, B.C.P. (Birgit), Cornelissen, E.A.M. (Elisabeth), Brüggemann, M. (Monika), Schaik, R.H.N. (Ron) van, Wildt, S.N. (Saskia) de, Cransberg, K. (Karlien), Winter, B.C.M. (Brenda) de, Andrews, L.M. (Louise), Hesselink, D.A. (Dennis), Gelder, T. (Teun) van, Koch, B.C.P. (Birgit), Cornelissen, E.A.M. (Elisabeth), Brüggemann, M. (Monika), Schaik, R.H.N. (Ron) van, Wildt, S.N. (Saskia) de, Cransberg, K. (Karlien), and Winter, B.C.M. (Brenda) de

Abstract

Background: Multiple clinical, demographic, and genetic factors affect the pharmacokinetics of tacrolimus in children, yet in daily practice, a uniform body-weight based starting dose is used. It can take weeks to reach the target tacrolimus pre-dose concentration. Objectives: The objectives of this study were to determine the pharmacokinetics of tacrolimus immediately after kidney transplantation and to find relevant parameters for dose individualization using a population pharmacokinetic analysis. Methods: A total of 722 blood samples were collected from 46 children treated with tacrolimus over the first 6 weeks after renal transplantation. Non-linear mixed-effects modeling (NONMEM®) was used to develop a population pharmacokinetic model and perform a covariate analysis. Simulations were performed to determine the optimal starting dose and to develop dosing guidelines. Results: The data were accurately described by a two-compartment model with allometric scaling for bodyweight. Mean tacrolimus apparent clearance was 50.5 L/h, with an inter-patient variability of 25%. Higher bodyweight, lower estimated glomerular filtration rate, and higher hematocrit levels resulted in lower total tacrolimus clearance. Cytochrome P450 3A5 expressers and recipients who received a kidney from a deceased donor had a significantly higher tacrolimus clearance. The model was successfully externally validated. In total, these covariates explained 41% of the variability in clearance. From the significant covariates, the cytochrome P450 3A5 genotype, bodyweight, and donor type were useful to adjust the starting dose to reach the target pre-dose concentration. Dosing guidelines range from 0.27 to 1.33 mg/kg/day. Conclusion: During the first 6 weeks after transplantation, the tacrolimus weight-normalized starting dose should be higher in pediatric kidney transplant recipients with a lower bodyweight, those who express the cytochrome P450 3A5 genotype, and those who receive a kidney from a de

Published
2018
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14. Children on dialysis as well as renal transplanted children report severely impaired health-related quality of life

Author

Splinter, A. (Anouck), Tjaden, L.A. (Lidwien A.), Haverman, L. (Lotte), Adams, B. (Brigitte), Collard, L. (Laure), Cransberg, K. (Karlien), van Dyck, M. (Maria), Hoeck, K. (Koen) van, Hoppe, B. (Bernd), Koster-Kamphuis, L. (Linda), Lilien, M. (Marc), Raes, A.K. (Ann), Taylan, C. (Christina), Grootenhuis, M.A. (Martha), Groothoff, J.W. (Jaap W.), Splinter, A. (Anouck), Tjaden, L.A. (Lidwien A.), Haverman, L. (Lotte), Adams, B. (Brigitte), Collard, L. (Laure), Cransberg, K. (Karlien), van Dyck, M. (Maria), Hoeck, K. (Koen) van, Hoppe, B. (Bernd), Koster-Kamphuis, L. (Linda), Lilien, M. (Marc), Raes, A.K. (Ann), Taylan, C. (Christina), Grootenhuis, M.A. (Martha), and Groothoff, J.W. (Jaap W.)

Abstract

Objectives: To assess health-related quality of life (HRQoL) across three renal replacement therapy modalities (preemptive transplant, non-preemptive transplant, and dialysis) in comparison with the healthy norm and other chronic health conditions, and to explore related patient factors. Study design: All prevalent end-stage renal disease (ESRD) patients aged 8–18 years who spent at least 6 months on their current treatment modality in the Netherlands, Belgium, and part of Germany were approached to complete the Pediatric Quality of Life Inventory 4.0 (PedsQL™) questionnaire. We determined the differences between groups on PedsQL™ mean scores, the proportion of children with an impaired HRQoL (≥ 1 SD lower than the healthy norm), the proportion of problems on individual items of the PedsQL™, and the effect of time on current treatment. Linear regression models were used to explore determinants of HRQoL. Results: 192 out of 278 patients (20% preemptive transplant, 58% non-preemptive transplant, 22% dialysis) filled in the PedsQL™ (response rate 69%). Independent of treatment modality, patients had significantly lower mean scores and consequently higher proportions of impaired HRQoL on almost all domains compared to the healthy norm and other chronic health conditions. Patients with a preemptive transplant only reported higher scores on physical health compared to the other treatment modalities. Having comorbidities was the most important determinant associated with lower HRQoL scores. Conclusion: Dialysis and renal transplantation both have a severe impact on the HRQoL of children with ESRD. Physicians should be aware of this continuous burden. Furthermore, to develop tailored interventions for children with ESRD, qualitative studies are needed to gain more insight in the determinants of HRQoL in the different tre

Published
2018
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16. Supplementary Material for: Childhood Estimates of Glomerular Filtration Rate Based on Creatinine and Cystatin C: Importance of Body Composition

Author

Miliku, K., Bakker, H., Dorresteijn, E.M., Cransberg, K., Franco, O.H., Felix, J.F., and Jaddoe V.W.V.

Subjects
2. Zero hunger
Abstract

Background: Creatinine and cystatin C concentrations are commonly used to estimate glomerular filtration rate (eGFR) in clinical practice and epidemiological studies. To estimate the influence of different body composition measures on eGFR from creatinine and cystatin C blood concentrations, we compared the associations of different anthropometric and body composition measures with eGFR derived from creatinine (eGFRcreat) and cystatin C (eGFRcystC) blood concentrations. Methods: In a population-based cohort study among 4,305 children aged 6.0 years (95% range 5.7-8.0), we measured weight and height and calculated body mass index (BMI) and body surface area (BSA), and lean and fat mass using dual-energy X-ray absorptiometry. At the same age, we measured creatinine and cystatin C blood concentrations and estimated the GFR. Results: Correlation between eGFR based on creatinine and cystatin C concentrations was r = 0.40 (p value cystC but not with eGFRcreat. Higher BSA was associated with higher eGFRcreat and lower eGFRcystC (p value creat but not with eGFRcystC. Conclusion: Our findings suggest that both eGFRcreat and eGFRcystC are influenced by BMI and BSA. eGFRcreat is more strongly influenced by body composition than eGFRcystC.

Published
2017
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17. Epidemiology and management of hypertension in paediatric and young adult kidney transplant recipients in The Netherlands: Nephrology Dialysis Transplantation

Author

Dobrowolski, L. C., van Huis, A.M., van der Lee, J. H., Sengers, H. P., Lilien, M.R., Cransberg, K., Cornelissen, M., Bouts, A.H., de Fijter, Johan W., Berger, S.P., van Zuilen, Arjan, Nurmohamed, S. A., Betjes, M.G.H., Hilbrands, Luuk, Hoitsma, A.J., Bemelman, F.J., Krediet, C. T. P., Groothoff, J. W., Nephrology, and AII - Infectious diseases

Abstract

Hypertension in kidney transplant recipients (KTRs) is a risk factor for cardiovascular mortality and graft loss. Data on the prevalence of hypertension and uncontrolled hypertension (uHT) in paediatric and young adult KTRs are scarce. Also, it is unknown whether 'transition' (the transfer from paediatric to adult care) influences control of hypertension. We assessed the prevalence of hypertension and uHT among Dutch paediatric and young adult KTRs and analysed the effects of transition. Additionally, we made an inventory of variations in treatment policies in Dutch transplant centres. Cross-sectional and longitudinal national data from living KTRs a parts per thousand currency sign30 years of age (a parts per thousand yen1-year post-transplant, eGFR > 20 mL/min) were extracted from the 'RICH Q' database, which comprises information about all Dutch KTRs

Published
2016
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18. Childhood Estimates of Glomerular Filtration Rate Based on Creatinine and Cystatin C: Importance of Body Composition

Author

Miliku, K. (Kozeta), Bakker, H. (Hanneke), Dorresteijn, E.M. (Eiske), Cransberg, K. (Karlien), Franco, O.H. (Oscar), Felix, J.F. (Janine), Jaddoe, V.W.V. (Vincent), Miliku, K. (Kozeta), Bakker, H. (Hanneke), Dorresteijn, E.M. (Eiske), Cransberg, K. (Karlien), Franco, O.H. (Oscar), Felix, J.F. (Janine), and Jaddoe, V.W.V. (Vincent)

Abstract

__Background:__ Creatinine and cystatin C concentrations are commonly used to estimate glomerular filtration rate (eGFR) in clinical practice and epidemiological studies. To estimate the influence of different body composition measures on eGFR from creatinine and cystatin C blood concentrations, we compared the associations of different anthropometric and body composition measures with eGFR derived from creatinine (eGFRcreat) and cystatin C (eGFRcystC) blood concentrations. __Methods:__ In a population-based cohort study among 4,305 children aged 6.0 years (95% range 5.7-8.0), we measured weight and height and calculated body mass index (BMI) and body surface area (BSA), and lean and fat mass using dual-energy X-ray absorptiometry. At the same age, we measured creatinine and cystatin C blood concentrations and estimated the GFR. __Results:__ Correlation between eGFR based on creatinine and cystatin C concentrations was r = 0.40 (p value <0.01). Higher BMI was associated with lower eGFRcystC but not with eGFRcreat. Higher BSA was associated with higher eGFRcreat and lower eGFRcystC (p value <0.05). Lean and fat mass percentages were associated with eGFRcreat but not with eGFRcystC. __Conclusion:__ Our findings suggest that both eGFRcreat and eGFRcystC are influenced by BMI and BSA. eGFRcreat is more strongly influenced by body composition than eGFRcystC.

Published
2017
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19. Epidemiology and management of hypertension in paediatric and young adult kidney transplant recipients in The Netherlands

Author

Dobrowolski, L.C., Huis, M. van, Lee, J.H. van der, Peters Sengers, H., Liliën, M.R., Cransberg, K., Cornelissen, M., Bouts, A.H., Fijter, J.W. de, Berger, S.P., Zuilen, A.D. van, Nurmohamed, S.A., Betjes, M.H., Hilbrands, L.B., Hoitsma, A.J., Bemelman, F.J., Krediet, P., Groothoff, J.W., Dobrowolski, L.C., Huis, M. van, Lee, J.H. van der, Peters Sengers, H., Liliën, M.R., Cransberg, K., Cornelissen, M., Bouts, A.H., Fijter, J.W. de, Berger, S.P., Zuilen, A.D. van, Nurmohamed, S.A., Betjes, M.H., Hilbrands, L.B., Hoitsma, A.J., Bemelman, F.J., Krediet, P., and Groothoff, J.W.

Abstract

Contains fulltext : 172479.pdf (publisher's version ) (Closed access)

Published
2016

20. The Effect of Weight and CYP3A5 Genotype on the Population Pharmacokinetics of Tacrolimus in Stable Paediatric Renal Transplant Recipients

Author

Prytula, A.A., Cransberg, K., Bouts, A.H., Schaik, R.H. van, Jong, H. de, Wildt, S.N. de, Mathot, R.A.A., Prytula, A.A., Cransberg, K., Bouts, A.H., Schaik, R.H. van, Jong, H. de, Wildt, S.N. de, and Mathot, R.A.A.

Abstract

Item does not contain fulltext, BACKGROUND: The aim of this study was to develop a population pharmacokinetic model of tacrolimus in paediatric patients at least 1 year after renal transplantation and simulate individualised dosage regimens. PATIENTS AND METHODS: We included 54 children with median age of 11.1 years (range 3.8-18.4 years) with 120 pharmacokinetic profiles performed over 2 to 4 h. The pharmacokinetic analysis was performed using the non-linear mixed-effects modelling software (NONMEM((R))). The impact of covariates including concomitant medications, age, the cytochrome P450 (CYP) CYP3A5*3 gene and the adenosine triphosphate binding cassette protein B1 (ABCB1) 3435 C-->T gene polymorphism on tacrolimus pharmacokinetics was analysed. The final model was externally validated on an independent dataset and dosing regimens were simulated. RESULTS: A two-compartment model adequately described tacrolimus pharmacokinetics. Apparent oral clearance (CL/F) was associated with weight (allometric scaling) but not age. Children with lower weight and CYP3A5 expressers required higher weight-normalised tacrolimus doses. CL/F was inversely associated with haematocrit (P < 0.05) and gamma-glutamyl transpeptidase (gammaGT) (P < 0.001) and was increased by 45 % in carriers of the CYP3A5*1 allele (P < 0.001). CL/F was not associated with concomitant medications. Dose simulations show that a daily tacrolimus dose of 0.2 mg/kg generates a pre-dose concentration (C 0) ranging from 5 to 10 microg/L depending on the weight and CYP3A5 polymorphism. The median area under the plasma concentration-time curve (AUC) corresponding with a tacrolimus C 0 of 4-8 microg/L was 97 h.microg/L (interquartile range 80-120). CONCLUSIONS: In patients beyond the first year after transplantation, there is a cumulative effect of CYP3A5*1 polymorphism and weight on the tacrolimus C 0. Children with lower weight and carriers of the CYP3A5*1 allele have higher weight-normalised tacrolimus dose requirements.

Published
2016

21. The impact of estimated glomerular filtration rate equations on chronic kidney disease staging in pediatric renal or heart transplant recipients

Author

Vroling, A.B. (Aram Ben), Dorresteijn, E.M. (Eiske), Cransberg, K. (Karlien), Rijke, Y.B. (Yolanda) de, Vroling, A.B. (Aram Ben), Dorresteijn, E.M. (Eiske), Cransberg, K. (Karlien), and Rijke, Y.B. (Yolanda) de

Abstract

Background: The aim of this study was to evaluate the performance of selected pediatric estimated glomerular filtration rate (eGFR) equations in relation to the clinical management of children after renal or heart transplantation or post-chemotherapy treatment. Methods: This study was a retrospective cross-sectional analysis of 61 children whose glomerular function (GFR) had been determined using a single-dose inulin clearance (iGFR) method. Eight equations for estimating the GFR were evaluated for bias, agreement, accuracy, and clinical stratification. Results: The outcome of all eight eGFR equations differed from the value determined using the iGFR method, with the mean bias ranging from −3.4 to 20.7 ml/min/1.73 m2 and 90 % accuracy ranging from 16 to 26 %. All eGFR equations overestimated renal function in patients with decreased kidney function as determined by the iGFR method and underestimated renal function in patients with normal kidney function. Consequently, based on the eGFR values, patients with low GFR values according to the iGFR method were staged in a less severe chronic kidney disease (CKD) category, and patients with normal GFR values according to the iGFR method were staged in a more severe CKD category. The percentage of correctly classified patients ranged from 32.6 to 41.6 %. Conclusions: In our cohort we found the CKiDIII equation to be the best alternative to calculating the GFR using the inulin clearance method, closely followed by the Hoste and the revised Grubb equations. The performances of all eight eGFR equations assessed were moderate at best and only slightly better than the easy-to-do bedside Schwartz equation.

Published
2016
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24. Urinary neutrophil gelatinase-associated lipocalin identifies critically ill young children with acute kidney injury following intensive care admission

Author

Zwiers, A.J.M. (Alexandra), Wildt, S.N. (Saskia) de, Rosmalen, J.M. (Joost) van, Rijke, Y.B. (Yolanda) de, Buijs, E.A.B. (Erik ), Tibboel, D. (Dick), Cransberg, K. (Karlien), Zwiers, A.J.M. (Alexandra), Wildt, S.N. (Saskia) de, Rosmalen, J.M. (Joost) van, Rijke, Y.B. (Yolanda) de, Buijs, E.A.B. (Erik ), Tibboel, D. (Dick), and Cransberg, K. (Karlien)

Abstract

__Introduction__ Children admitted to a pediatric intensive care unit (ICU) are at high risk of developing acute kidney injury (AKI). Although serum creatinine (SCr) levels are used in clinical practice, they are insensitive for early diagnosis of AKI. Urinary neutrophil gelatinase-associated lipocalin (uNGAL) and kidney injury molecule-1 (KIM-1) are novel AKI biomarkers whose performance in pediatric ICU patients is largely unknown. In this study, we aimed to characterize uNGAL and KIM-1 patterns in children following ICU admission and to assess their properties in relation to identifying children at risk for AKI development. __Methods__ From June 2010 until January 2014, we conducted a prospective observational cohort study of term-born children ages 1day to 1year on mechanical ventilation. Blood and urine samples were obtained every 6 to 12hours up to 72hours post-admission. Blood samples were assayed for SCr, and urine samples were assayed for uNGAL and KIM-1. The RIFLE (risk, injury, failure, loss, end-stage renal disease) classification as 150%, 200% or 300% of median SCr reference values was used to define AKI. __Results__ A total of 100 children were included (80 survived). Their median age at admission was 27.7days (interquartile range (IQR), 1.5 to 85.5). The median duration of mechanical ventilation was 5.8days (IQR, 3.1 to 11.4). Thirty-five patients had evidence of AKI within the first 48hours post-admission, of whom 24 (69%) already had AKI when they entered the ICU. uNGAL and KIM-1 concentrations in AKI peaked between 6 to 12hours and between 12 to 24hours post-admission, respectively. The maximal area under the receiver operating characteristic curve (AUC) for uNGAL was 0.815 (95% confidence interval (CI), 0.685 to 0.945, P <0.001) at 0 to 6hours post-admission. The discriminative ability of KIM-1 was moderate, with a largest AUC of 0.737 (95% CI, 0.628 to 0.847; P <0.001) at 12 to 24hours post-admission. At the optimal cutoff point (126ng/ml), uNGAL

Published
2015
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26. Children of non-Western origin with end-stage renal disease in the Netherlands, Belgium and a part of Germany have impaired health-related quality of life compared with Western children

Author

Schoenmaker, N.J., Haverman, L., Tromp, W.F., Lee, J.H. van der, Offringa, M., Adams, B., Bouts, A.H.M., Collard, L., Cransberg, K., Dyck, M. van, Godefroid, N., Hoeck, K. van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Taylan, C., Grootenhuis, M.A., Groothoff, J.W., Schoenmaker, N.J., Haverman, L., Tromp, W.F., Lee, J.H. van der, Offringa, M., Adams, B., Bouts, A.H.M., Collard, L., Cransberg, K., Dyck, M. van, Godefroid, N., Hoeck, K. van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Taylan, C., Grootenhuis, M.A., and Groothoff, J.W.

Abstract

Item does not contain fulltext, BACKGROUND: Many children with end-stage renal disease (ESRD) living in Western Europe are of non-Western European origin. They have unfavourable somatic outcomes compared with ESRD children of Western origin. In this study, we compared the Health-related Quality of Life (HRQoL) of both groups. METHODS: All children (5-18 years) with ESRD included in the RICH-Q project (Renal Insufficiency therapy in Children-Quality assessment and improvement) or their parents were asked to complete the generic version of the Paediatric Quality-of-Life Inventory 4.0 (PedsQL). RICH-Q comprises the Netherlands, Belgium and a part of Germany. Children were considered to be of non-Western origin if they or at least one parent was born outside Western-European countries. Impaired HRQoL for children with ESRD of Western or non-Western origin was defined as a PedsQL score less than fifth percentile for healthy Dutch children of Western or non-Western origin, respectively. RESULTS: Of the 259 eligible children, 230 agreed to participate. One hundred and seventy-four children responded (response rate 67%) and 55 (32%) were of non-Western origin. Overall, 31 (56%) of the ESRD children of non-Western origin, and 58 (49%) of Western origin had an impaired total HRQoL score. Total HRQoL scores of children with ESRD of Western origin and non-Western origin were comparable, but scores on emotional functioning and school functioning were lower in non-Western origin (P=0.004 and 0.01, respectively). The adjusted odds ratios (95% confidence interval) for ESRD children of non-Western origin to have impaired emotional functioning and school functioning, compared with Western origin, were 3.3(1.5-7.1) and 2.2(1.1-4.2), respectively. CONCLUSION: Children with ESRD of non-Western origin in three Western countries were found to be at risk for impaired HRQoL on emotional and school functioning. These children warrant special attention.

Published
2014

27. CKD and hypertension during long-term follow-up in children and adolescents previously treated with extracorporeal membrane oxygenation

Author

Zwiers, A.J.M. (Alexandra), IJsselstijn, H. (Hanneke), Rosmalen, J.M. (Joost) van, Gischler, S.J. (Saskia), Wildt, S.N. (Saskia) de, Tibboel, D. (Dick), Cransberg, K. (Karlien), Zwiers, A.J.M. (Alexandra), IJsselstijn, H. (Hanneke), Rosmalen, J.M. (Joost) van, Gischler, S.J. (Saskia), Wildt, S.N. (Saskia) de, Tibboel, D. (Dick), and Cransberg, K. (Karlien)

Abstract

__Abstract__ Background and objectives Many children receiving extracorporeal membrane oxygenation develop AKI. If AKI leads to permanent nephron loss, it may increase the risk of developing CKD. The prevalence of CKD and hypertension and its predictive factors during long-term follow-up of children and adolescents previously treated with neonatal extracorporeal membrane oxygenation were determined. Design, setting, participants, & measurements Between November of 2010 and February of 2014, neonatal survivors of extracorporeal membrane oxygenation who visited the prospective follow-up program at 1, 2, 5, 8, 12, and 18 years of age were screened for CKD and hypertension (BP³95th percentile of reference values). CKD was suspected in children with either an eGFR<90 ml/min per 1.73 m2 or proteinuria (urinary protein-tocreatinine ratio >0.50 for children ages £24 months and >0.20 at >24 months). The RIFLE classification (risk, injury, or failure as 150%, 200%, or 300% of serum creatinine reference values) was used to define AKI during extracorporeal membrane oxygenation without preemptive hemofiltration. Results Median follow-up of 169 screened participants was 8.2 years (interquartile range=5.2–12.1 years). Nine children had a lower eGFR, but all rates were >60 ml/min per 1.73 m2. Proteinuria was observed in 20 children (median=0.26 mg protein/mg creatinine; interquartile range=0.23–0.32 mg protein/mg creatinine), and 32 children had hypertension. Only history of AKI was associated with CKD (P=0.004). Children with RIFLE scores injury and failure had 4.3 times higher odds of CKD signs or hypertension than those without AKI (95% confidence interval, 1.6 to 12.1; P=0.004). Conclusions Altogether, 54 participants (32%) had at least one sign of CKD and/or hypertension. However, most values were marginally abnormal, with no immediate consequences for clinical care. Nevertheless, a prevalence of 32% clearly indicates that survivors of neonatal extracorporeal membrane oxygenat

Published
2014
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29. Cytomegalovirus prophylaxis in pediatric kidney transplantation: the Dutch experience.

Author

Jongsma, H., Bouts, A.H.M., Cornelissen, E.A.M., Beersma, M.F., Cransberg, K., Jongsma, H., Bouts, A.H.M., Cornelissen, E.A.M., Beersma, M.F., and Cransberg, K.

Abstract

1 september 2013, Item does not contain fulltext, Many children receiving a kidney transplant are seronegative for CMV and therefore, highly susceptible to a primary CMV infection. This study aims at evaluating incidence, time of occurrence, and severity of CMV infection in the first year post-transplantation in relation to different types of CMV prophylaxis. Transplantations in three centers in the Netherlands between 1999 and 2010 were included. Retrospective, observational, multicenter study. Clinical data and PCR measurements of CMV were collected. Prophylaxis in high-risk patients (CMV serostatus D+R-) consisted of (val)ganciclovir during three months, or acyclovir plus CMV immunoglobulin at a former stage. Intermediate-risk patients (R+) received (val)acyclovir, or acyclovir plus CMV immunoglobulin at a former stage. Low-risk patients (D-R-) did not receive prophylaxis. Infection was defined as CMV PCR above 50 geq/mL plasma or whole blood, a clinically relevant infection above 1000 geq/mL. One hundred and fifty-nine transplantations were included. CMV infection was documented for 41% of high-risk, 24% of intermediate-risk, and 13% of low-risk patients, in the latter two groups typically during the first three months. The infection rate was highest in the high-risk group after cessation of valganciclovir prophylaxis. Valganciclovir provided better protection than did acyclovir + CMV immunoglobulin. Adding an IL2-receptor blocker to the immunosuppressive regimen did not affect the infection rate. Acute graft rejection was not related with CMV infection. Valganciclovir prophylaxis effectively prevents CMV infection in high-risk pediatric kidney recipients, but only during prophylaxis. Valacyclovir prophylaxis in intermediate-risk patients is less effective.

Published
2013

30. Acute kidney injury is a frequent complication in critically ill neonates receiving extracorporeal membrane oxygenation: A 14-year cohort study

Author

Zwiers, A.J.M. (Alexandra), Wildt, S.N. (Saskia) de, Hop, W.C.J. (Wim), Dorresteijn, E.M. (Eiske), Gischler, S.J. (Saskia), Tibboel, D. (Dick), Cransberg, K. (Karlien), Zwiers, A.J.M. (Alexandra), Wildt, S.N. (Saskia) de, Hop, W.C.J. (Wim), Dorresteijn, E.M. (Eiske), Gischler, S.J. (Saskia), Tibboel, D. (Dick), and Cransberg, K. (Karlien)

Abstract

Introduction: Newborns in need of extracorporeal membrane oxygenation (ECMO) support are at high risk of developing acute kidney injury (AKI). AKI may occur as part of multiple organ failure and can be aggravated by exposure to components of the extracorporeal circuit. AKI necessitates adjustment of dosage of renally eliminated drugs and avoidance of nephrotoxic drugs. We aimed to define systematically the incidence and clinical course of AKI in critically ill neonates receiving ECMO support. Methods: This study reviewed prospectively collected clinical data (including age, diagnosis, ECMO course, and serum creatinine (SCr)) of all ECMO-treated neonates within our institution spanning a 14-year period. AKI was defined by using the Risk, Injury, Failure, Loss of renal function, and End-stage renal disease (RIFLE) classification. SCr data were reviewed per ECMO day and compared with age-specific SCr reference values. Accordingly, patients were assigned to RIFLE categories (Risk, Injury, or Failure as 150%, 200%, or 300% of median SCr reference values). Data are presented as median and interquartile range (IQR) or number and percentage. Results: Of 242 patients included, 179 (74%) survived. Median age at the start of

Published
2013
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31. Policy variation in donor and recipient status in 11 pediatric renal transplantation centers.

Author

Huis, M. van, Schoenmaker, N.J., Groothoff, J.W., Lee, J.H. van der, Cransberg, K., Bouts, A.H.M., Collard, L., Dyck, M. van, Godefroid, N., Hoeck, K. van, Taylan, C., Koster-Kamphuis, L., Lilien, M.R., Raes, A., Ranguelov, N., Huis, M. van, Schoenmaker, N.J., Groothoff, J.W., Lee, J.H. van der, Cransberg, K., Bouts, A.H.M., Collard, L., Dyck, M. van, Godefroid, N., Hoeck, K. van, Taylan, C., Koster-Kamphuis, L., Lilien, M.R., Raes, A., and Ranguelov, N.

Abstract

01 juni 2013, Item does not contain fulltext, BACKGROUND: Evidence-based guidelines for pediatric renal transplantation (Tx) are lacking. This may lead to unwanted treatment variations. We aimed to quantify the variation in treatment policies and its consequences in daily practice in 11 centers that provide renal Tx for children in three European countries. METHODS: We surveyed Tx policies in all ten centers in the Netherlands and Belgium and one center in Germany. We compared Tx policies with the therapies actually provided and with recommendations from available published guidelines and existing literature. Information on treatment policies was obtained by a questionnaire; information on care actually provided was registered prospectively from 2007 to 2011. The clinical guidelines were identified by searches of MEDLINE and websites of pediatric nephrology organizations. RESULTS: Between centers, we found discrepancies in policies on: the minimum accepted recipient weight (8-12 kg), the maximum living and deceased donor age (50-75 and 45-60 years, respectively). HLA-match policies varied between acceptation of all mismatches to at least 1A1B1DR match donor transplantations amounting to 49 % in the Netherlands versus 26 % in Belgium (p = 0.006). CONCLUSIONS: Management policies for renal Tx in children vary considerably between centers and nations. This has a direct impact on the delivered care, and by extrapolation, on health outcome.

Published
2013

32. Important differences in management policies for children with end-stage renal disease in the Netherlands and Belgium--report from the RICH-Q study.

Author

Tromp, W.F., Schoenmaker, N.J., Lee, J.H., Adams, B., Bouts, A.H.M., Collard, L., Cransberg, K., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K. van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Offringa, M., Groothoff, J.W., Tromp, W.F., Schoenmaker, N.J., Lee, J.H., Adams, B., Bouts, A.H.M., Collard, L., Cransberg, K., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K. van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Offringa, M., and Groothoff, J.W.

Abstract

1 mei 2012, Item does not contain fulltext, BACKGROUND: The low prevalence of childhood end-stage renal disease and the small centre sizes have been a barrier for clinical studies and the development of evidence-based guidelines for chronic renal replacement therapy (cRRT) in children. Few data exist on the quality of care for these patients and the applicability of existing guidelines. The aim of this study is to quantify variation in treatment policies and actually delivered care in nine centres that deliver cRRT for children. METHODS: We surveyed treatment policies in all nine centres in the Netherlands and Belgium and compared them with the actually provided therapies and with recommendations from available guidelines. Data on treatment policies were gathered by questionnaires; actually provided care and outcomes were registered prospectively from 2007 to 2010. RESULTS: Data on policies and actual patient care were obtained from all nine centres. We found relevant differences between centres in treatment policies on various topics, e.g. estimated glomerular filtration rate threshold as an indication for initiation of cRRT, preferred initial mode of cRRT, peritoneal dialysis catheter care, haemodialysis frequency and vascular access. Discrepancies were seen between stated treatment policies and actual performed therapies. For the majority of policies, no evidence-based guidelines are available. CONCLUSIONS: Health care disparities exist due to large and unwanted variation in treatment policies between hospitals providing cRRT for children. Delivered care does not live up to stated policies, for which clear and internationally accepted guidelines are lacking.

Published
2012

33. Disparities in dialysis treatment and outcomes for Dutch and Belgian children with immigrant parents.

Author

Schoenmaker, N.J., Tromp, W.F., Lee, J.H., Adams, B., Bouts, A.H.M., Collard, L., Cransberg, K., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K.J. Van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Groothoff, J.W., Schoenmaker, N.J., Tromp, W.F., Lee, J.H., Adams, B., Bouts, A.H.M., Collard, L., Cransberg, K., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K.J. Van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., and Groothoff, J.W.

Abstract

1 augustus 2012, Item does not contain fulltext, BACKGROUND: In Belgium and the Netherlands, up to 40% of the children on dialysis are children with immigrant parents of non-Western European origin (non-Western). Concerns exist regarding whether these non-Western patients receive the same quality of care as children with parents of Western European origin (Western). We compared initial dialysis, post-initial treatment, and outcomes between non-Western and Western patients on dialysis. METHODS: All children <19 years old on chronic dialysis in the Netherlands and Belgium between September 2007 and May 2011 were included in the study. Non-Western patients were defined as children of whom one or both parents were born in non-Western countries. RESULTS: Seventy-nine of the 179 included patients (44%) were non-Western children. Compared to Western patients, non-Western patients more often were treated with hemodialysis (HD) instead of peritoneal dialysis (PD) as first dialysis mode (52 vs. 37%, p = 0.046). Before renal transplantation, non-Western patients were on dialysis for a median (range) of 30 (5-99) months, vs. 15 (0-66) months in Western patients (p = 0.007). Renal osteodystrophy was diagnosed in 34% of non-Western vs. 18% of Western patients (p = 0.028). The incidence rate ratio [95% confidence interval] for acute peritonitis was 2.44 [1.43-4.17] (p = 0.032) for non-Western compared to Western patients. CONCLUSIONS: There are important disparities between children on chronic dialysis with parents from Western European origin and those from non-Western European origin in the choice of modality, duration, and outcomes of dialysis therapy.

Published
2012

34. Eculizumab as rescue therapy for atypical hemolytic uremic syndrome with normal platelet count.

Author

Dorresteijn, E.M., Kar, N.C.A.J. van de, Cransberg, K., Dorresteijn, E.M., Kar, N.C.A.J. van de, and Cransberg, K.

Abstract

01 juli 2012, Item does not contain fulltext, BACKGROUND: Atypical hemolytic uremic syndrome (aHUS) in childhood is a rare disease with frequent progression to end-stage renal disease and a high recurrence after kidney transplantation. Eculizumab, a humanized monoclonal antibody that binds to complement protein C5, may be beneficial in the treatment of aHUS. CASE-DIAGNOSIS/TREATMENT: A 6-year-old girl developed aHUS with only slightly elevated C3d (4.4%), no mutations in complement factors, and no antibodies against factor H. Plasma exchange treatment was successful initially, until aHUS recurred. After reinitiating plasma exchange, normalization of the platelet count and improvement of hemolysis occurred, but renal function worsened. Renal function then improved dramatically promptly after the switch to eculizumab. CONCLUSIONS: This case demonstrates that platelet count is not always a reliable marker for improvement of aHUS and that eculizumab can prevent dialysis in plasma-resistant aHUS patients.

Published
2012

35. Eculizumab as rescue therapy for atypical hemolytic uremic syndrome with normal platelet count

Author

Dorresteijn, E.M. (Eiske), Kar, N.C. (Nicole) van de, Cransberg, K. (Karlien), Dorresteijn, E.M. (Eiske), Kar, N.C. (Nicole) van de, and Cransberg, K. (Karlien)

Abstract

Background Atypical hemolytic uremic syndrome (aHUS) in childhood is a rare disease with frequent progression to end-stage renal disease and a high recurrence after kidney transplantation. Eculizumab, a humanized monoclonal antibody that binds to complement protein C5, may be beneficial in the treatment of aHUS. Case-diagnosis/treatment A 6-year-old girl developed aHUS with only slightly elevated C3d (4.4%), no mutations in complement factors, and no antibodies against factor H. Plasma exchange treatment was successful initially, until aHUS recurred. After reinitiating plasma exchange, normalization of the platelet count and improvement of hemolysis occurred, but renal function worsened. Renal function then improved dramatically promptly after the switch to eculizumab. Conclusions This case demonstrates that platelet count is not always a reliable marker for improvement of aHUS and that eculizumab can prevent dialysis in plasma-resistant aHUS patients.

Published
2012
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36. Disparities in dialysis treatment and outcomes for Dutch and Belgian children with immigrant parents

Author

Schoenmaker, N.J. (Nikki), Tromp, W.F. (Wilma), Lee, J.H. (Johanna) van der, Adams, B. (Brigitte), Bouts, A.H. (Antonia), Collard, L. (Laure), Cransberg, K. (Karlien), Damme-Lombaerts, R. (Rita) van, Godefroid, N. (Nathalie), Hoeck, K. (Koen) van, Koster-Kamphuis, L. (Linda), Lilien, M. (Marc), Raes, A.K. (Ann), Groothoff, J. (Jaap), Schoenmaker, N.J. (Nikki), Tromp, W.F. (Wilma), Lee, J.H. (Johanna) van der, Adams, B. (Brigitte), Bouts, A.H. (Antonia), Collard, L. (Laure), Cransberg, K. (Karlien), Damme-Lombaerts, R. (Rita) van, Godefroid, N. (Nathalie), Hoeck, K. (Koen) van, Koster-Kamphuis, L. (Linda), Lilien, M. (Marc), Raes, A.K. (Ann), and Groothoff, J. (Jaap)

Abstract

Background In Belgium and the Netherlands, up to 40% of the children on dialysis are children with immigrant parents of non-Western European origin (non-Western). Concerns exist regarding whether these non-Western patients receive the same quality of care as children with parents of Western European origin (Western). We compared initial dialysis, post-initial treatment, and outcomes between non-Western and Western patients on dialysis. Methods All children <19 years old on chronic dialysis in the Netherlands and Belgium between September 2007 and May 2011 were included in the study. Non-Western patients were defined as children of whom one or both parents were born in non-Western countries. Results Seventy-nine of the 179 included patients (44%) were non-Western children. Compared to Western patients, non-Western patients more often were treated with hemodi-alysis (HD) instead of peritoneal dialysis (PD) as first dialysis mode (52 vs. 37%, p=0.046). Before renal transplantation, non-Western patients were on dialysis for a median (range) of 30 (5-99) months, vs. 15 (0-66) months in Western patients (p=0.007). Renal osteodystrophy was diagnosed in 34% of non-Western vs. 18% ofWestern patients (p=0.028). The incidence rate ratio [95% confidence interval] for acute peritonitis was 2.44 [1.43-4.17] (p=0.032) for non-Western compared to Western patients. Conclusions There are important disparities between children on chronic dialysis with parents from Western European origin and those from non-Western European origin in the choice of modality, duration, and outcomes of dialysis therapy.

Published
2012
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37. Fewer pre-emptive renal transplantations and more rejections in immigrant children compared to native Dutch and Belgian children.

Author

Tromp, W.F., Cransberg, K., Lee, J.H., Bouts, A.H.M., Collard, L., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K.J. Van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Ranguelov, N., Groothoff, J.W., Tromp, W.F., Cransberg, K., Lee, J.H., Bouts, A.H.M., Collard, L., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K.J. Van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Ranguelov, N., and Groothoff, J.W.

Abstract

01 juni 2012, Item does not contain fulltext, BACKGROUND: In the Netherlands and Belgium, an increasing number of children who have end-stage renal disease (ESRD) are of non-Western origin. We analysed renal transplantation practices and outcome for immigrant ESRD children as compared to native children in both countries. METHODS: All Dutch and Belgian children aged <19 years who received their first renal transplantation between 1 September 2007 and 1 January 2011 were included. Therapy characteristics and outcomes were registered prospectively on a 3-monthly basis. Immigrants were defined as children of whom one or both parents had been born outside Western European countries. Multivariable Cox regression analysis was used to quantify the hazard ratio for acute rejection. RESULTS: One hundred and nineteen first renal transplant recipients were included, of which 41 (34%) were immigrants. Median [range] follow-up time of transplantation was 18 [2-28] months. Compared to native children, immigrants had pre-emptive transplantations (15 versus 32%, P = 0.040) and transplantations with a kidney from a living donor less often (24 versus 59%, P < 0.001). Survival analysis in 96 children with at least 3 months of follow-up showed an increased risk for acute rejection in immigrants adjusted for donor source, duration of dialysis and number of HLA mismatches on the DR locus [hazard ratio (95% confidence interval) 2.5 (1.1-5.9)]. CONCLUSIONS: Immigrant children receive fewer pre-emptive and living donor transplantations compared to native children. After transplantation, immigrant children are at higher risk for acute rejection irrespective of the mode of transplantation.

Published
2012

38. Lessons learned from efforts to improve the quality of care in children with end-stage renal disease in the Netherlands and Belgium.

Author

Tromp, W.F., Lee, J.H., Offringa, M., Bouts, A.H.M., Collard, L., Cransberg, K., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K. van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., Groothoff, J.W., Tromp, W.F., Lee, J.H., Offringa, M., Bouts, A.H.M., Collard, L., Cransberg, K., Damme-Lombaerts, R. van, Godefroid, N., Hoeck, K. van, Koster-Kamphuis, L., Lilien, M.R., Raes, A., and Groothoff, J.W.

Abstract

1 december 2011, Item does not contain fulltext

Published
2011

39. Schimke immunoosseous dysplasia: Defining skeletal features

Author

Hunter, K.B. (Kshamta), Lücke, T. (Thomas), Spranger, J. (Jürgen), Smithson, S.F. (Sarah), Alpay, H. (Harika), André, J.-L. (Jean-Luc), Asakura, Y. (Yumi), Bogdanovic, R. (Radovan), Bonneau, D. (Dominique), Cairns, R. (Robyn), Cransberg, K. (Karlien), Fründ, S. (Stefan), Fryssira, H. (Helen), Goodman, D. (David), Helmke, K. (Knut), Hinkelmann, B. (Barbara), Lama, G. (Guiliana), Lamfers, P. (Petra), Loirat, C. (Chantal), Majore, S. (Silvia), Mayfield, C. (Christy), Pontz, B.F. (Betram), Rusu, C. (Christina), Saraiva, J.M. (Jorge), Schmidt, B. (Beate), Schoemaker, L. (Lawrence), Sigaudy, S. (Sabine), Stajic, N. (Natasa), Taha, D. (Doris), Boerkoel, C.F. (Cornelius), Hunter, K.B. (Kshamta), Lücke, T. (Thomas), Spranger, J. (Jürgen), Smithson, S.F. (Sarah), Alpay, H. (Harika), André, J.-L. (Jean-Luc), Asakura, Y. (Yumi), Bogdanovic, R. (Radovan), Bonneau, D. (Dominique), Cairns, R. (Robyn), Cransberg, K. (Karlien), Fründ, S. (Stefan), Fryssira, H. (Helen), Goodman, D. (David), Helmke, K. (Knut), Hinkelmann, B. (Barbara), Lama, G. (Guiliana), Lamfers, P. (Petra), Loirat, C. (Chantal), Majore, S. (Silvia), Mayfield, C. (Christy), Pontz, B.F. (Betram), Rusu, C. (Christina), Saraiva, J.M. (Jorge), Schmidt, B. (Beate), Schoemaker, L. (Lawrence), Sigaudy, S. (Sabine), Stajic, N. (Natasa), Taha, D. (Doris), and Boerkoel, C.F. (Cornelius)

Abstract

Schimke immunoosseous dysplasia (SIOD) is an autosomal recessive multisystem disorder characterized by prominent spondyloepiphyseal dysplasia, T cell deficiency, and focal segmental glomerulosclerosis. Biallelic mutations in swi/snf-related, matrix-associated, actin-dependent regulator of chromatin, subfamily a-like 1 (SMARCAL1) are the only identified cause of SIOD, but approximately half of patients referred for molecular studies do not have detectable mutations in SMARCAL1. We hypothesized that skeletal features distinguish between those with or without SMARCAL1 mutations. Therefore, we analyzed the skeletal radiographs of 22 patients with and 11 without detectable SMARCAL1 mutations. We found that patients with SMARCAL1 mutations have a spondyloepiphyseal dysplasia (SED) essentially limited to the spine, pelvis, capital femoral epiphyses, and possibly the sella turcica, whereas the hands and other long bones are basically normal. Additionally, we found that several of the adolescent and young adult patients developed osteoporosis and coxarthrosis. Of the 11 patients without detectable SMARCAL1 mutations, seven had a SED indistinguishable from patients with SMARCAL1 mutations. We conclude therefore that SED is a feature of patients with SMARCAL1 mutations and that skeletal features do not distinguish who of those with SED have SMARCAL1 mutations.

Published
2010
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40. Diagnostic value of urinary dysmorphic erythrocytes in clinical practice

Author

Crop, M.J. (Meindert), Rijke, Y.B. (Yolanda) de, Verhagen, P.C.M.S. (Paul), Cransberg, K. (Karlien), Zietse, R. (Bob), Crop, M.J. (Meindert), Rijke, Y.B. (Yolanda) de, Verhagen, P.C.M.S. (Paul), Cransberg, K. (Karlien), and Zietse, R. (Bob)

Abstract

Background: In clinical practice, discriminating between glomerular and nonglomerular causes of hematuria is often difficult. Dysmorphic red blood cells (dRBC) in the urinary sediment are claimed to be effective, but the cutoff points in the literature vary. This follow-up study aimed to determine the diagnostic value of dRBC. Methods: We investigated 134 hematuria patients in the departments of nephrology and urology. To diagnose the origin of hematuria, urological and/or nephrological examination was performed and the %dRBC identified by microscopy. Follow-up was performed after 3.5 years. Results: The cause of hematuria was proven in 68 patients (35% glomerular; 65% nonglomerular). Patients with glomerular disease had significantly more albuminuria and dRBC than patients with nonglomerular disease, but the %dRBC ranged from 1 to 50% and no optimal cutoff could be identified. Logistic regression analysis showed that %dRBC had a predicted probability to diagnose glomerular disease of 77.9% (area under the curve, AUC, 0.85). When %dRBC was combined with other risk factors such as serum creatinine, sex, age, dipstick erythrocyte or proteinuria score and number of casts, the predictive probability increased to 90.6% (AUC 0.97). Follow-up of the included patients showed no benefit of dRBC to identify patients at risk for glomerular disease. Conclusions: The diagnostic value of routinely collected urinary dRBC to diagnose glomerular disease in patients presenting with hematuria is modest. However, including dRBC with other variables, such as age and erythrocyte score on dipstick testing may increase the sensitivity, but needs to be confirmed in another, preferably larger, population. Copyright

Published
2010
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41. Haemofiltration in newborns treated with extracorporeal membrane oxygenation: A case-comparison study

Author

Blijdorp, K. (Karin), Cransberg, K. (Karlien), Wildschut, E.D. (Enno), Gischler, S.J. (Saskia), Houmes, R.J.M. (Robert Jan), Wolff, E.D. (Eric), Tibboel, D. (Dick), Blijdorp, K. (Karin), Cransberg, K. (Karlien), Wildschut, E.D. (Enno), Gischler, S.J. (Saskia), Houmes, R.J.M. (Robert Jan), Wolff, E.D. (Eric), and Tibboel, D. (Dick)

Abstract

Introduction: Extracorporeal membrane oxygenation is a supportive cardiopulmonary bypass technique for patients with acute reversible cardiovascular or respiratory failure. Favourable effects of haemofiltration during cardiopulmonary bypass instigated the use of this technique in infants on extracorporeal membrane oxygenation. The current study aimed at comparing clinical outcomes of newborns on extracorporeal membrane oxygenation with and without continuous haemofiltration. Methods: Demographic data of newborns treated with haemofiltration during extracorporeal membrane oxygenation were compared with those of patients treated without haemofiltration in a retrospective 1:3 case-comparison study. Primary outcome parameters were time on extracorporeal membrane oxygenation, time until extubation after decannulation, mortality and potential cost reduction. Secondary outcome parameters were total and mean fluid balance, urine output in mL/kg/day, dose of vasopressors, blood products and fluid bolus infusions, serum creatinin, urea and albumin levels. Results: Fifteen patients with haemofi

Published
2009
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42. Pulmonary complaints and lung function after pediatric kidney transplantation.

Author

Cransberg, K., Pijnenburg, M.A.M., Lunstroot, M., Lilien, M., Cornelissen, E.A.M., Davin, J.C., Hoeck, K. van, Merkus, P.J.F.M., Nauta, J., Cransberg, K., Pijnenburg, M.A.M., Lunstroot, M., Lilien, M., Cornelissen, E.A.M., Davin, J.C., Hoeck, K. van, Merkus, P.J.F.M., and Nauta, J.

Abstract

Item does not contain fulltext, Recently four of 38 children with a kidney transplant were diagnosed with bronchiectasis. The aim of the current study was to identify patients with increased risk for pulmonary damage. In this cross-sectional observational study, children with a functioning kidney graft in the Netherlands and Antwerp, Belgium, were screened with the use of a symptom checklist and spirometry. Maximum score for upper airway complaints was 21 (normal: <8), for lower airway complaints 28 (<10). Results of FVC, FEV(1) and MEF(25) were expressed as percentage predicted for height and sex. One hundred and thirty-five patients completed the interview (122) and/or spirometry (103); 91 did both. Lower airways symptoms were above acceptable levels in 18 (14%) patients. Forty-nine patients (48%) had an abnormal lung function test: in 12 concerning FVC%, in 11 FEV(1)%, in 24 MEF(25)% and in 36 FEV(1)/FVC. Of correlations between symptomatology or spirometry data, and clinical parameters, only that between GFR and MEF(25)% was statistically significant. Children with a kidney transplant are at increased risk for obstructive lung disease. We recommend to monitor lung function during the follow-up after renal transplantation.

Published
2008

43. Recovery of graft function in pediatric kidney transplantation is not affected by delayed introduction of cyclosporine.

Author

Cransberg, K., Bouts, A.H.M., Cornelissen, E.A.M., Lilien, M.R., Hoeck, K. van, Hop, W.C.J., Nauta, J., Cransberg, K., Bouts, A.H.M., Cornelissen, E.A.M., Lilien, M.R., Hoeck, K. van, Hop, W.C.J., and Nauta, J.

Abstract

Contains fulltext : 71230.pdf (publisher's version ) (Closed access), BACKGROUND: Delayed graft function and acute rejections adversely affect the long-term survival of kidney transplantation. To decrease the incidences of these phenomena, we changed the initial immunosuppressive protocol in pediatric kidney transplantation in The Netherlands. METHODS: We compared a cohort (n=123) treated with basiliximab and delayed onset cyclosporine (CsA) with the preceding cohort (n=110) in which CsA was started already preoperatively. Both cohorts were treated with mycophenolate mofetil and corticosteroids as well. All consecutive transplantations were included. RESULTS: The incidence of delayed graft function did not significantly differ between the cohorts (10% and 13%, in basiliximab and control group). Significantly fewer patients in the basiliximab group had acute rejection episodes (20% vs. 36% in control group, P=0.007). The mean estimated glomerular filtration rate at 1 year and graft survival at 2 years posttransplant did not differ between groups (62 vs. 64 mL/min 1.73 m2, and 89% vs. 92%, respectively). CONCLUSION: Postponed onset of CsA in triple immunosuppressive therapy (corticosteroids, CsA, and mycophenolate mofetil) with addition of basiliximab did not reduce the incidence of delayed graft function in pediatric kidney transplantation. Yet, fewer acute rejections were noted. Long-term favorable effects could not be detected in this study.

Published
2008

44. Topotecan distribution in an anephric infant with therapy resistant bilateral Wilms tumor with a novel germline WT1 gene mutation

Author

Lugtenberg, R.T. (Rieneke), Cransberg, K. (Karlien), Loos, W.J. (Walter), Wagner, A. (Anja), Alders, M. (Mariëlle), Heuvel-Eibrink, M.M. (Marry) van den, Lugtenberg, R.T. (Rieneke), Cransberg, K. (Karlien), Loos, W.J. (Walter), Wagner, A. (Anja), Alders, M. (Mariëlle), and Heuvel-Eibrink, M.M. (Marry) van den

Abstract

The therapeutic strategy for bilateral Wilms tumor (WT) remains a challenge. Especially in cases with chemotherapy resistant disease, bilateral nephrectomy is sometimes inevitable. For optimal cure rates stage V WT patients benefit from adjuvant treatment; however, there are limited data available on chemotherapy pharmacokinetics in anephric children. In this report, we describe a 10-month old girl with bilateral Wilms tumor and a novel germline WT1 gene mutation. This patient hardly showed any response on preoperative chemotherapy, and ultimately, underwent sequential bilateral tumor-nephrectomy. Subsequently, during peritoneal dialysis, she received topotecan as adjuvant chemotherapy based on plasma levels, indicating that this is a reasonable option as adjuvant treatment in therapy-resistant Wilms tumor patients after bilateral nephrectomy. This case showed a novel germline WT1 gene mutation of which the correlation with resistant phenotype has to be confirmed in larger cohorts of WT patients.

Published
2008
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45. Pediatric Kidney Transplantation in the Netherlands collaborative studies

Author

Cransberg, K. (Karlien) and Cransberg, K. (Karlien)

Abstract

The first successful kidney transplantation dates back to the year 1954. A healthy adult donated a kidney to his identical twin brother with life-threatening kidney disease. No immunosuppressive medication was used. The recipient lived for nine more years, got married, had children, and had a job to his liking.1 This event raised the hopes of all patients with end stage kidney disease. It took another five years before the first kidney transplantation in a child succeeded, with a kidney donated by his identical twin.2 Transplantation is the ultimate modality of renal replacement therapy for end stage renal failure in children. It replaces most of the lost functions of the native kidneys, in contrast to any form of dialysis. Transplantation may restore kidney function within normal ranges, whereas with dialysis no more than 10% of normal clearance is reached. Moreover, dialysis is associated with high morbidity and even mortality. Chronic dialysis in children is therefore not considered as a permanent solution, but as a bridge to transplantation. In the Netherlands kidney transplantation in children is an accepted and feasible option since 1973. In our country the procedure is thought to be feasible in children with a minimum age of 3 years, or a minimum body weight of 12 kg. Either a pediatric or a vascular surgeon performs the transplantation, in some centers together with a pediatric urologist. The grafted kidney is usually placed in the iliac fossa; in case of a small child receiving an adult kidney, the abdomen may be the graft site. The renal blood vessels are anastomosed with the recipient’s external or commune iliac vessels, or, in case of intra-abdominal placement, with the aorta and inferior caval vein. The donor ureter is implanted in the recipient’s bladder. In most centers a temporary intraureteral splint is placed to enable the urine to drain without resistance from the transplanted kidney.

Published
2008

46. Children of non-Western origin with end-stage renal disease in the Netherlands, Belgium and a part of Germany have impaired health-related quality of life compared with Western children

Author

Schoenmaker, N. J., primary, Haverman, L., additional, Tromp, W. F., additional, van der Lee, J. H., additional, Offringa, M., additional, Adams, B., additional, Bouts, A. H. M., additional, Collard, L., additional, Cransberg, K., additional, van Dyck, M., additional, Godefroid, N., additional, van Hoeck, K., additional, Koster-Kamphuis, L., additional, Lilien, M. R., additional, Raes, A., additional, Taylan, C., additional, Grootenhuis, M. A., additional, and Groothoff, J. W., additional

Published
2013
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47. Transplantation: clinical studies - A

Author

Yildirim, T., primary, Yilmaz, R., additional, Altindal, M., additional, Turkmen, E., additional, Arici, M., additional, Altun, B., additional, Erdem, Y., additional, Guliyev, O., additional, Erkmen Uyar, M., additional, Tutal, E., additional, Bal, Z., additional, Sezer, S., additional, Bal, U., additional, Say n, B., additional, Erdemir, B., additional, O'Rourke-Potowki, A., additional, Gauge, N., additional, Penny, H., additional, Cronin, A., additional, Frame, S., additional, Goldsmith, D. J., additional, Yagan, J. A., additional, Chandraker, A., additional, Velickovic Radovanovic, R. M., additional, Catic Djordjevic, A., additional, Mitic, B., additional, Stefanovic, N., additional, Cvetkovic, T., additional, Serpieri, N., additional, Grosjean, F., additional, Sileno, G., additional, Torreggiani, M., additional, Esposito, V., additional, Mangione, F., additional, Abelli, M., additional, Castoldi, F., additional, Catucci, D., additional, Esposito, C., additional, Dal Canton, A., additional, Vatazin, A. V., additional, Zulkarnaev, A. B., additional, Borst, C., additional, Liu, Y., additional, Thoning, J., additional, Tepel, M., additional, Libetta, C., additional, Margiotta, E., additional, Borettaz, I., additional, Canevari, M., additional, Martinelli, C., additional, Lainu, E., additional, Meloni, F., additional, Sepe, V., additional, Miguel Costa, R., additional, Vasquez Martul, E., additional, Reboredo, J., additional, Rivera, C., additional, Simonato, F., additional, Tognarelli, G., additional, Daidola, G., additional, Gallo, E., additional, Burdese, M., additional, Cantaluppi, V., additional, Biancone, L., additional, Segoloni, G. P., additional, Priora, M., additional, Messina, M., additional, Tamagnone, M., additional, Linsalata, A., additional, Lavacca, A., additional, Segoloni, G., additional, Zuidema, W., additional, Erdman, R., additional, van de Wetering, J., additional, Dor, F., additional, Roodnat, J., additional, Massey, E., additional, Timmerman, L., additional, IJzermans, J., additional, Weimar, W., additional, Sibley-Allen, C., additional, Hilton, R., additional, Moghul, M., additional, Burnapp, L., additional, Blake, G., additional, Koo, T. Y., additional, Park, J.-S., additional, Park, H. C., additional, Kim, G.-H., additional, Lee, C. H., additional, Oh, I. H., additional, Kang, C. M., additional, Hwang, J. K., additional, Park, S. C., additional, Choi, B. S., additional, Chun, H. J., additional, Kim, J. I., additional, Yang, C. W., additional, Moon, I. S., additional, Van Laecke, S., additional, Van Biesen, W., additional, Nagler, E. V., additional, Taes, Y., additional, Peeters, P., additional, Vanholder, R., additional, Pruthi, R., additional, Ravanan, R., additional, Casula, A., additional, Harber, M., additional, Roderick, P., additional, Fogarty, D., additional, Cho, A., additional, Shin, J.-h., additional, Jang, H. R., additional, Lee, J. E., additional, Huh, W., additional, Kim, D. J. K., additional, Oh, H. Y., additional, Kim, Y.-G., additional, Sancho Calabuig, A., additional, Gavela Martinez, E., additional, Kanter Berga, J., additional, Beltran Catalan, S., additional, Avila Bernabeu, A. I., additional, Pallardo Mateu, L. M., additional, Gonzalez, E., additional, Polanco, N., additional, Molina, M., additional, Gutierrez, E., additional, Garcia Puente, L., additional, Sevillano, A., additional, Morales, E., additional, Praga, M., additional, Andres, A., additional, Banasik, M., additional, Boratynska, M., additional, Koscielska-Kasprzak, K., additional, Bartoszek, D., additional, Myszka, M., additional, Zmonarski, S., additional, Nowakowska, B., additional, Wawrzyniak, E., additional, Halon, A., additional, Chudoba, P., additional, Klinger, M., additional, Rojas-Rivera, J., additional, Morales, J. M., additional, Egido, J., additional, Kopecky, C. M., additional, Haidinger, M., additional, Kaltenecker, C., additional, Antlanger, M., additional, Marsche, G., additional, Holzer, M., additional, Kovarik, J., additional, Werzowa, J., additional, Hecking, M., additional, Saemann, M. D., additional, Kim, J. M., additional, Koh, E. S., additional, Chung, B. H., additional, Kim, Y. S., additional, Krajewska, M., additional, Mazanowska, O., additional, Kaminska, D., additional, Zabinska, M., additional, Malkiewicz, B., additional, Patrzalek, D., additional, Sulowicz, J., additional, Szostek, S., additional, Wojas-Pelc, A., additional, Ignacak, E., additional, Sulowicz, W., additional, Bellizzi, V., additional, Calella, P., additional, Cupisti, A., additional, Capitanini, A., additional, D'Alessandro, C., additional, Giannese, D., additional, Camocardi, A., additional, Conte, G., additional, Barsotti, M., additional, Bilancio, G., additional, Luciani, R., additional, Locsey, L., additional, Seres, I., additional, Kovacs, D., additional, Asztalos, L., additional, Paragh, G., additional, Wohlfahrtova, M., additional, Balaz, P., additional, Rokosny, S., additional, Wohlfahrt, P., additional, Bartonova, A., additional, Viklicky, O., additional, Kers, J., additional, Geskus, R. B., additional, Meijer, L. J., additional, Bemelman, F., additional, ten Berge, I. J. M., additional, Florquin, S., additional, Hwang, J.-C., additional, Jiang, M.-Y., additional, Lu, Y.-H., additional, Weng, S.-F., additional, Testa, A., additional, Porto, G., additional, Sanguedolce, M., additional, Spoto, B., additional, Parlongo, R., additional, Pisano, A., additional, Enia, G., additional, Tripepi, G., additional, Zoccali, C., additional, Mamode, N., additional, Lennerling, A., additional, Citterio, F., additional, Van Assche, K., additional, Sterckx, S., additional, Frunza, M., additional, Jung, H., additional, Pascalev, A., additional, Johnson, R., additional, Loven, C., additional, Soleymanian, T., additional, Keyvani, H., additional, Jazayeri, S. M., additional, Fazeli, Z., additional, Ghamari, S., additional, Mahabadi, M., additional, Chegeni, V., additional, Najafi, I., additional, Ganji, M. R., additional, Meys, K. M. E., additional, Groothoff, J. W., additional, Jager, K., additional, Schaefer, F., additional, Tonshoff, B., additional, Mota, C., additional, Cransberg, K., additional, van Stralen, K., additional, Gurluler, E., additional, Gures, N., additional, Alim, A., additional, Gurkan, A., additional, Cakir, U., additional, Berber, I., additional, Caluwe, R., additional, Nagler, E., additional, Van Vlem, B., additional, Betkowska-Prokop, A., additional, Kuzniewski, M., additional, Krzanowski, M., additional, Masson, I., additional, Flamant, M., additional, Maillard, N., additional, Cavalier, E., additional, Moranne, O., additional, Alamartine, E., additional, Mariat, C., additional, Delanaye, P., additional, Canas Sole, L. L., additional, Iglesias Alvarez, E., additional, Pastor, M. C. M. C., additional, Moreno Flores, F. F., additional, Abujder, V. V., additional, Graterol, F. F., additional, Bonet Sol, J. J., additional, Lauzurica Valdemoros, R. R., additional, Yoshikawa, M., additional, Kitamura, K., additional, Nakai, K., additional, Goto, S., additional, Fujii, H., additional, Ishimura, T., additional, Takeda, M., additional, Fujisawa, M., additional, Nishi, S., additional, Prasad, N., additional, Gurjer, D., additional, Bhadauria, D., additional, Gupta, A., additional, Sharma, R., additional, Kaul, A., additional, Cybulla, M., additional, West, M., additional, Nicholls, K., additional, Torras, J., additional, Sunder-Plassmann, G., additional, Feriozzi, S., additional, Lo, S., additional, Wong, P. Y. H., additional, Ip, D., additional, Wong, C. K., additional, Chow, V. C. C., additional, Mo, S. K. L., additional, Molnar, M., additional, Ujszaszi, A., additional, Czira, M. E., additional, Novak, M., additional, Mucsi, I., additional, Cruzado, J. M., additional, Coelho, S., additional, Porta, N., additional, Bestard, O., additional, Melilli, E., additional, Taco, O., additional, Rivas, I., additional, Grinyo, J., additional, Pouteau, L.-M., additional, N'Guyen, J.-M., additional, Hami, A., additional, Hourmant, M., additional, Ghahramani, N., additional, Karparvar, Z., additional, Shadrou, S., additional, Ghahramani, M., additional, Fauvel, J. P., additional, Hadj-Aissa, A., additional, Buron, F., additional, Morelon, E., additional, Ducher, M., additional, Heine, C., additional, Glander, P., additional, Neumayer, H.-H., additional, Budde, K., additional, Liefeldt, L., additional, Montero, N., additional, Webster, A. C., additional, Royuela, A., additional, Zamora, J., additional, Crespo, M., additional, Pascual, J., additional, Adema, A. Y., additional, van Dorp, W. T. H., additional, Mallat, M. J. K., additional, de Fijter, H. W., additional, Hong, Y. A., additional, Park, C. W., additional, Kim, Y.-S., additional, Suleymanlar, G., additional, Uzundurukan, Z., additional, Kapuagas , A., additional, Sencan, I., additional, Akdag, R., additional, Torio, A., additional, Mas, V., additional, Perez-Saez, M. J., additional, Mir, M., additional, Faura, A., additional, Montes-Ares, O., additional, Checa, M. D., additional, Sawinski, D., additional, Trofe-Clark, J., additional, Sparkes, T., additional, Patel, P., additional, Goral, S., additional, Bloom, R., additional, Kim, H. J., additional, Park, S. J., additional, Kim, T. H., additional, Kim, Y. W., additional, Kim, Y. H., additional, Kang, S. W., additional, Abdel Halim, M., additional, Gheith, O., additional, Al-Otaibi, T., additional, Mosaad, A., additional, Awadeen, W., additional, Said, T., additional, Nair, P., additional, and Nampoory, M. R. N., additional

Published
2013
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48. Maintenance immunosuppression with mycophenolate mofetil and corticosteroids in pediatric kidney transplantation: temporary benefit but not without risk.

Author

Cransberg, K., Cornelissen, M., Lilien, M., Hoeck, K. van, Davin, J.C., Nauta, J., Cransberg, K., Cornelissen, M., Lilien, M., Hoeck, K. van, Davin, J.C., and Nauta, J.

Abstract

Contains fulltext : 52819.pdf (publisher's version ) (Closed access), BACKGROUND: Aiming at reducing cyclosporine toxicity, we investigated safety and efficacy of mycophenolate mofetil (MMF) as an immunosuppressive drug in pediatric kidney transplantation compared with cyclosporine (CsA), both in combination with corticosteroids. METHODS: One year after kidney transplantation, children on triple immunosuppression, having experienced no more than one, steroid-sensitive, acute rejection episode, were randomized to withdrawal of either CsA or MMF and were followed for 2 yr. RESULTS: In each group, two patients had an acute rejection episode during withdrawal. Treatment failure occurred in 3 of 21 MMF and 5 of 23 CsA patients. Final analysis was for 18 patients in either group. A larger than 10 mL/min 1.73 m decrease in glomerular filtration rate was observed in more patients on CsA than on MMF (73% vs. 29%, P=0.019). No differences in blood pressure or nightly decrease of blood pressure were noted. Hypercholesterolism improved in the MMF (-16%), but not the CsA group (+5%, P<0.05), over the first, but not over both study years. Differences in triglycerid levels between groups were not shown. At study end, MMF patients tended to have lower hemoglobin levels than patients on CsA. Two MMF patients experienced a first acute rejection episode during the second study year, resulting in chronic transplant glomerulopathy with graft loss in one and deterioration of kidney function in the other. CONCLUSION: In pediatric kidney transplantation, maintenance immunosuppression with MMF together with corticosteroids has short-term benefits for kidney function and lipid pattern compared with CsA but is not without risk of complications.

Published
2007

49. Four cases of hemolytic uremic syndrome - source contaminated swimming water?

Author

Cransberg, K., Kerkhof, I. van den, Banffer, J., Stijnen, P.J.J., Wernars, K., Kar, N.C.A.J. van de, Nauta, J., and Wolff, E.D.

Subjects
Epidemiologie en pathogenese van het hemolytisch uremisch syndroom, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), Epidemiology and pathogenesis of the hemolytic uremic syndrome
Abstract

Contains fulltext : 23916___.PDF (Publisher’s version ) (Open Access)

Published
1996

50. Etiology and epidemiology of end-stage renal disease in Dutch children 1987-2001.

Author

Miklovicova, D., Cornelissen, M., Cransberg, K., Groothoff, J.W., Dedik, L., Schroder, C.H., Miklovicova, D., Cornelissen, M., Cransberg, K., Groothoff, J.W., Dedik, L., and Schroder, C.H.

Abstract

Contains fulltext : 47449.pdf (publisher's version ) (Closed access), In this retrospective study 351 children (<16.0 years) with end-stage renal disease (ESRD) accepted for renal replacement therapy (RRT) in the four Dutch pediatric centers were analyzed for the period 1987-2001. The data were compared with a previous study performed in 1979-1986. Eighty patients were of non-Dutch origin. An annual ESRD incidence of 5.8 patients per million of the child population (p.m.c.p.) was calculated, without significant changes with time. The final prevalence in Dutch children under 15 years of ESRD was 38.7 p.m.c.p. The most frequent primary renal disease leading to ESRD was urethral valves, with a significant increase vs. the previous observation period (14% vs. 6%). The distribution of primary renal diseases was similar in patients of non-Dutch origin and in Dutch patients. Peritoneal dialysis was the most frequent dialysis procedure initially applied (62% vs. 26% in the earlier observation period). Thirteen percent of all first transplantations (n=278) were pre-emptive and 19% from living donors. Five-year graft survival after a living-donor and a cadaver graft was 80% and 73%, respectively. Overall patient survival after 10 years on RRT was 94%.

Published
2005

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