278 results on '"Rush A"'
Search Results
2. Risk Prediction for Delayed Allograft Function: Analysis of the Deterioration of Kidney Allograft Function (DeKAF) Study Data
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Matas, Arthur J., Helgeson, Erika, Fieberg, Ann, Leduc, Robert, Gaston, Robert S., Kasiske, Bertram L., Rush, David, Hunsicker, Lawrence, Cosio, Fernando, Grande, Joseph P., Cecka, J. Michael, Connett, John, and Mannon, Roslyn B.
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- 2022
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3. Late Graft Loss After Kidney Transplantation: Is “Death With Function” Really Death With a Functioning Allograft?
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Gaston, Robert S., Fieberg, Ann, Helgeson, Erika S., Eversull, Jason, Hunsicker, Lawrence, Kasiske, Bertram L., Leduc, Robert, Rush, David, and Matas, Arthur J.
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- 2020
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4. Anti-CD40 Antibodies do not Cause Thromboembolism as Demonstrated by in Vitro and in Vivo Studies
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Rubic-Schneider, Tina, Christen, Brigitte, Garcia, Deborah, Loll, Nathalie Runser, Erard, Esther, Flandre, Thierry, de Billy, Benjamin Cochin, Nock, Sebastien, Côté, Serge, Rush, James S, and Ulrich, Peter
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- 2018
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5. CD40 Inhibition with CFZ533 - A New, Fully Human, Non-Depleting, Fc Silent mAB - Improves Renal Allograft Function While Demonstrating Comparable Efficacy vs. Tacrolimus in De-Novo CNI-Free Kidney Transplant Recipients
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Nashan, B, Tedesco, H, van den Hoogen, MW, Berger, SP, Cibrik, D, Mulgaonkar, S, Leeser, D, Alloway, R, Patel, A, Pratschke, J, Sommerer, C, Wiseman, A, van Zuilen, A, Laessing, U, Rush, J, Haraldsson, B, and Witzke, O
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- 2018
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6. Urinary Metabolomics for Noninvasive Detection of Antibody-Mediated Rejection in Children After Kidney Transplantation
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Blydt-Hansen, Tom D., Sharma, Atul, Gibson, Ian W., Wishart, David S., Mandal, Rupasri, Ho, Julie, Nickerson, Peter, and Rush, David
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- 2017
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7. Late Graft Loss After Kidney Transplantation: Is 'Death With Function' Really Death With a Functioning Allograft?
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DeKAF Investigators, David N. Rush, Ann M. Fieberg, Arthur J. Matas, Jason Eversull, Erika S. Helgeson, Bertram L. Kasiske, Robert E Leduc, Lawrence G. Hunsicker, and Robert S. Gaston
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Adult ,Graft Rejection ,Male ,medicine.medical_specialty ,Biopsy ,medicine.medical_treatment ,Renal function ,Disease ,Kidney ,Kidney Function Tests ,Renal Dialysis ,Risk Factors ,Internal medicine ,Humans ,Transplantation, Homologous ,Medicine ,Prospective Studies ,Prospective cohort study ,Kidney transplantation ,Dialysis ,Aged ,Transplantation ,business.industry ,Graft Survival ,Middle Aged ,Allografts ,medicine.disease ,Kidney Transplantation ,United States ,Clinical trial ,medicine.anatomical_structure ,Kidney Failure, Chronic ,Female ,business ,Follow-Up Studies ,Glomerular Filtration Rate - Abstract
Background About half of late kidney allograft losses are attributed to death with function (DWF), a poorly characterized outcome. An ongoing question is whether DWF is a consequence of chronic allograft dysfunction. Using the prospective Long-term Deterioration of Kidney Allograft Function study database, we sought to better define the impact, phenotype, and clinical course of DWF in the current era. Methods Three thousand five hundred eighty-seven kidney recipients with functional grafts at 90 days post-transplant were followed prospectively for a median of 5.2 years. Results Characteristics at transplantation in those with DWF (N = 350, 9.8%) differed from those who otherwise lost their grafts (death-censored graft failure [DC-GF], N = 295, 8.2%) or maintained function (N = 2942, 82.0%); DWF patients were older, sicker, and had been on dialysis longer, with more preexisting cardiovascular disease, whereas DC-GF patients experienced more early rejection, more acute rejection after 90 days, and a clinically significant decrease in kidney function before graft failure. In contrast, the clinical course after transplantation in DWF patients did not differ before death from those who maintained function throughout. Conclusions DWF and DC-GF in kidney transplant recipients represent differing clinical phenotypes occurring in distinct patient populations. Reducing the impact of DWF requires better definition of causes and clinical course and then trials of therapies to improve outcomes. Composite endpoints in clinical trials that group DWF and DC-GF together may obscure important clinical findings.
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- 2019
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8. 311.3: A 5-Year Prospective, Randomized, Open-Label Study of Standard Versus Low-Dose Prolonged-Release Tacrolimus With Or Without ACEi/ARB in Kidney Transplantation
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Sandra M. Cockfield, Patricia M. Campbell, Marcelo Cantarovich, Azim Gangji, Ahmed Shoker, Anthony M. Jevnikar, Felix-Mauricio Monroy-Cuadros, Peter W. Nickerson, Michel R. Pâquet, G. V. Ramesh Prasad, Lynne Senécal, Jason J. Schwartz, Jean-Luc Wolff, and David Rush
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Transplantation - Published
- 2022
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9. Analysis of Biomarkers Within the Initial 2 Years Posttransplant and 5-Year Kidney Transplant Outcomes
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Nancy D. Bridges, Kenneth A. Newell, Madhav C. Menon, Girish N. Nadkarni, Jens Goebel, Barbara Murphy, Peter Nickerson, Emilio D. Poggio, Richard N. Formica, Yvonne Morrison, Geovani Faddoul, David N. Rush, Donald E. Hricik, and Peter S. Heeger
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Transplantation ,medicine.medical_specialty ,Surrogate endpoint ,business.industry ,030232 urology & nephrology ,Renal function ,Odds ratio ,030230 surgery ,medicine.disease ,Gastroenterology ,Article ,Organ transplantation ,03 medical and health sciences ,0302 clinical medicine ,Internal medicine ,Cohort ,medicine ,Biomarker (medicine) ,Prospective cohort study ,business ,Kidney disease - Abstract
Background An early posttransplant biomarker/surrogate marker for kidney allograft loss has the potential to guide targeted interventions. Previously published findings, including results from the Clinical Trials in Organ Transplantation (CTOT)-01 study, showed that elevated urinary chemokine CXCL9 levels and elevated frequencies of donor-reactive interferon gamma (IFNγ)-producing T cells by enzyme-linked immunosorbent spot (ELISPOT) assay associated with acute cellular rejection within the first year and with lower 1-year posttransplant estimated glomerular filtration rate (eGFR). How well these biomarkers correlate with late outcomes, including graft loss, is unclear. Methods In CTOT-17, we obtained 5-year outcomes in the CTOT-01 cohort and correlated them with (a) biomarker results and (b) changes in eGFR (Chronic Kidney Disease Epidemiology Collaboration formula) over the initial 2 years posttransplant using univariable analysis and multivariable logistic regression. Results Graft loss occurred in 14 (7.6%) of 184 subjects 2 to 5 years posttransplant. Neither IFNγ ELISPOTs nor urinary CXCL9 were informative. In contrast, a 40% or greater decline in eGFR from 6 months to 2 years posttransplant independently correlated with 13-fold odds of 5-year graft loss (adjusted odds ratio, 13.1; 95% confidence interval, 3.0-56.6), a result that was validated in the independent Genomics of Chronic Allograft Rejection cohort (n = 165; adjusted odds ratio, 11.2). Conclusions We conclude that although pretransplant and early posttransplant ELISPOT and chemokine measurements associate with outcomes within 2 years posttransplant, changes in eGFR between 3 or 6 months and 24 months are better surrogates for 5-year outcomes, including graft loss.
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- 2018
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10. Urinary Metabolomics for Noninvasive Detection of Antibody-Mediated Rejection in Children After Kidney Transplantation
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David S. Wishart, Peter Nickerson, David N. Rush, Ian W. Gibson, Atul Sharma, Tom Blydt-Hansen, Julie Ho, and Rupasri Mandal
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Graft Rejection ,Male ,medicine.medical_specialty ,Biopsy ,Urinary system ,030232 urology & nephrology ,Urology ,030230 surgery ,Kidney transplant ,Antibodies ,Mass Spectrometry ,03 medical and health sciences ,0302 clinical medicine ,Metabolomics ,medicine ,Humans ,Transplantation, Homologous ,Prospective Studies ,Child ,Prospective cohort study ,Kidney transplantation ,Transplantation ,medicine.diagnostic_test ,business.industry ,Reproducibility of Results ,medicine.disease ,Kidney Transplantation ,Tissue Donors ,Antibody mediated rejection ,Female ,business ,Biomarkers ,Follow-Up Studies - Abstract
Biomarkers are needed that identify patients with antibody-mediated rejection (AMR). The goal of this study was to evaluate the utility of urinary metabolomics for early noninvasive detection of AMR in pediatric kidney transplant recipients.Urine samples (n = 396) from a prospective, observational cohort of 59 renal transplant patients with surveillance or indication biopsies were assayed for 133 unique metabolites by quantitative mass spectrometry. Samples were classified according to Banff criteria for AMR and partial least squares discriminant analysis was used to identify associated changes in metabolite patterns by creating a composite index based on all 133 metabolites.Urine samples of patients with (n = 40) and without AMR (n = 278) were analyzed and a classifier for AMR was identified (area under receiver operating characteristic curve = 0.84; 95% confidence interval, 0.77-0.91; P = 0.006). Application of the classifier to "indeterminate" samples (samples that partially fulfilled Banff criteria for AMR; n = 65) yielded an AMR score of 0.19 ± 0.15, intermediate between scores for AMR and No AMR (0.28 ± 0.14 and 0.10 ± 0.13 respectively, P ≤ 0.001). The AMR score was associated with the presence of donor-specific antibodies, biopsy indication, Banff ct, t, ah and cg scores, and retained accuracy when applied to subclinical cases (creatinine,25% increase from baseline) or had minimal or no transplant glomerulopathy (Banff cg0-1). Exploratory classifiers that segregated samples based on concurrent T cell-mediated rejection (TCMR) identified overlapping metabolite signatures between AMR and TCMR, suggesting similar pathophysiology of tissue injury.These preliminary findings identify a urine metabolic classifier for AMR. Independent validation is needed to verify its utility for accurate, noninvasive AMR detection.
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- 2017
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11. Subclinical Antibody-Mediated Rejection
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David N. Rush, Maria-Angeles de Cos, Peter Nickerson, Piedad Ussetti, Emilio Rodrigo, Manuel Arias, Daniel Serón, Chris Wiebe, and Ignacio Herrero
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Graft Rejection ,Biopsy ,MEDLINE ,030230 surgery ,03 medical and health sciences ,0302 clinical medicine ,Text mining ,HLA Antigens ,Isoantibodies ,Predictive Value of Tests ,Risk Factors ,Immunity ,Animals ,Humans ,Medicine ,Asymptomatic Diseases ,Subclinical infection ,Transplantation ,medicine.diagnostic_test ,business.industry ,Graft Survival ,Organ Transplantation ,Immunity, Humoral ,Histocompatibility ,Treatment Outcome ,Predictive value of tests ,Immunology ,030211 gastroenterology & hepatology ,business ,Immunosuppressive Agents - Published
- 2017
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12. Subclinical Inflammation in Renal Transplantation
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Ian W. Gibson and David N. Rush
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Graft Rejection ,Pathology ,medicine.medical_specialty ,Time Factors ,medicine.medical_treatment ,Biopsy ,Inflammation ,030230 surgery ,Kidney ,Peripheral blood mononuclear cell ,Risk Assessment ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Risk Factors ,Parenchyma ,medicine ,Humans ,Subclinical infection ,Transplantation ,Creatinine ,Nephritis ,medicine.diagnostic_test ,business.industry ,Immunosuppression ,Kidney Transplantation ,Treatment Outcome ,chemistry ,Asymptomatic Diseases ,030211 gastroenterology & hepatology ,medicine.symptom ,business ,Immunosuppressive Agents - Abstract
The standardization of renal allograft pathology began in 1991 at the first Banff Conference held in Banff, Alberta, Canada. The first task of transplant pathologists, clinicians, and surgeons was to establish diagnostic criteria for T-cell-mediated rejection (TCMR). The histological threshold for this diagnosis was arbitrarily set at "i2t2": a mononuclear interstitial cell infiltrate present in at least 25% of normal parenchyma and >4 mononuclear cells within the tubular basement membrane of nonatrophic tubules. TCMR was usually found in dysfunctional grafts with an elevation in the serum creatinine; however, our group and others found this extent of inflammation in "routine" or "protocol" biopsies of normally functioning grafts: "subclinical" TCMR. The prevalence of TCMR is higher in the early months posttransplant and has decreased with the increased potency of current immunosuppressive agents. However, the pathogenicity of lesser degrees of inflammation under modern immunosuppression and the relation between ongoing inflammation and development of donor-specific antibody has renewed our interest in subclinical alloreactivity. Finally, the advances in our understanding of pretransplant risk assessment, and our increasing ability to monitor patients less invasively posttransplant, promises to usher in the era of precision medicine.
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- 2019
13. Optimization of Perioperative Conditions to Prevent Ischemic Cholangiopathy in Donation After Circulatory Death Donor Liver Transplantation
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Natalia I. Rush, Richard S. Mangus, Joseph Tector, Burcin Ekser, Matthew Wingler, Chandrashekhar A. Kubal, Jonathan A. Fridell, and Romil Saxena
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Adult ,Male ,Time Factors ,Biliary Tract Diseases ,medicine.medical_treatment ,Operative Time ,Ischemia ,Kaplan-Meier Estimate ,030230 surgery ,Liver transplantation ,Cold Ischemia Time ,Donor Selection ,Young Adult ,03 medical and health sciences ,0302 clinical medicine ,Fibrinolytic Agents ,Risk Factors ,Cause of Death ,Humans ,Medicine ,Warm Ischemia ,Aged ,Retrospective Studies ,Cause of death ,Transplantation ,Donor selection ,business.industry ,Cold Ischemia ,Graft Survival ,Perioperative ,Middle Aged ,medicine.disease ,Tissue Donors ,Liver Transplantation ,Treatment Outcome ,Tissue Plasminogen Activator ,Anesthesia ,Female ,030211 gastroenterology & hepatology ,Hepatectomy ,business ,Fibrinolytic agent - Abstract
BACKGROUND Donation after circulatory death (DCD) donor pool remains underutilized for liver transplantation (LT). We describe optimizing "modifiable risk factors," such as cold ischemia time (CIT) recipient warm ischemia time (WIT) and the use of thrombolytic flush at the time of procurement to minimize ischemic cholangiopathy (IC). METHODS From July 2011 (era II), to improve outcomes after DCD LT, measures were taken to minimize CIT, operative time and recipient WIT along with the use of tissue plasminogen activator (tPA) flush during DCD procurements. Thirty consecutive DCD LTs were performed prospectively in era II. Outcomes were compared with 61 historic controls (era I). Reperfusion biopsies were evaluated for the presence of necrosis and biliary epithelial damage. RESULTS Median CIT (4.9 [3.5-5.9] vs 6.4 [4.3-12]; P < 0.001), hepatectomy time (70 [42-120] vs 81 [58-207]; P = 0.02), and recipient WIT (16 [13-31] vs 24[15-40]; P < 0.001) were significantly shorter in era II. All patients in era II received tPA flushed liver grafts. None of the patients in era II developed IC (0% vs 18%; P = 0.013). There were fewer biliary complications in era II, and there was no increased risk of bleeding associated with the use of tPA. One-year graft survival was slightly better in era II (n = 24 patients with 1 year follow-up) (88% vs 80%; P = 0.14). CONCLUSIONS Optimizing peritransplant conditions, such as shortening ischemic times with the use of thrombolytic donor flush, may prevent IC after DCD LT. With this approach, the DCD donor pool may be expanded.
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- 2016
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14. Elevated Urinary Matrix Metalloproteinase-7 Detects Underlying Renal Allograft Inflammation and Injury
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Jennifer Bestland, Julie Ho, David N. Rush, Ian W. Gibson, Brett Hiebert, Peter Nickerson, Chris Wiebe, Ang Gao, Claudio Rigatto, Oleg V. Krokhin, Mihaela Antonovici, and John A. Wilkins
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Adult ,Male ,Proteomics ,Pathology ,medicine.medical_specialty ,Urinalysis ,Urinary system ,030232 urology & nephrology ,Enzyme-Linked Immunosorbent Assay ,Inflammation ,030230 surgery ,Matrix metalloproteinase ,03 medical and health sciences ,chemistry.chemical_compound ,0302 clinical medicine ,Predictive Value of Tests ,Tandem Mass Spectrometry ,medicine ,Humans ,CXCL10 ,Prospective Studies ,Transplantation ,Creatinine ,Nephritis ,medicine.diagnostic_test ,business.industry ,Acute kidney injury ,Reproducibility of Results ,Acute Kidney Injury ,Clinical Enzyme Tests ,Middle Aged ,respiratory system ,Allografts ,medicine.disease ,Kidney Transplantation ,Up-Regulation ,Chemokine CXCL10 ,Treatment Outcome ,chemistry ,Matrix Metalloproteinase 7 ,Female ,medicine.symptom ,business ,Biomarkers ,Chromatography, Liquid - Abstract
The urinary CXC chemokine ligand (CXCL)10 detects renal transplant inflammation noninvasively, but has limited sensitivity and specificity. In this study, we performed urinary proteomic analysis to identify novel biomarkers that may improve the diagnostic performance of urinary CXCL10 for detecting alloimmune inflammation in renal transplant patients.In preliminary studies, adult renal transplant patients with normal histology (n = 5), interstitial fibrosis and tubular atrophy (n = 6), subclinical (n = 6) and clinical rejection (n = 6), underwent in-depth urine protein compositional analysis with LC-MS/MS, and matrix metalloproteinase-7 (MMP7) were identified as a potential candidate for the diagnosis of renal allograft inflammation. Urine MMP7 performance was then studied in a larger, prospective adult renal transplant population (n = 148 urines from n = 133 patients) with matched surveillance/indication biopsies. The diagnostic performance of urinary MMP7 and CXCL10 in combination was next evaluated using concordance (C-) statistics, net reclassification improvement and integrated discrimination improvement indices, to determine whether it was better than CXCL10 alone.Urinary MMP7:creatinine (Cr) was lower in normal transplants compared to those with inflammation: glomerulonephritis (P = 0.009), viral nephropathies (P = 0.002), interstitial fibrosis and tubular atrophy and inflammation (P = 0.04), borderline (P = 0.08), subclinical (P = 0.01) and clinical rejection (P = 0.0006), and acute tubular necrosis (P0.0001). Urinary MMP7:Cr and CXCL10:Cr significantly distinguished noninflamed from inflamed biopsies (area under the curve, 0.74 and 0.70, respectively). The addition of urinary MMP7:Cr to CXCL10:Cr improved the diagnostic performance for subclinical and clinical inflammation/injury by integrated discrimination improvement (P = 0.002) and net reclassification improvement (P = 0.006) analyses.Urinary MMP7:Cr improves the overall diagnostic performance of urinary CXCL10:Cr for distinguishing normal histology from subclinical and clinical inflammation/injury, but not subclinical inflammation alone.
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- 2016
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15. Activity-based Protein Profiling Approaches for Transplantation
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Navarrete, Mario, primary, Wilkins, John A., additional, Lao, Ying, additional, Rush, David N., additional, Nickerson, Peter W., additional, and Ho, Julie, additional
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- 2019
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16. Subclinical Inflammation in Renal Transplantation
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Rush, David N., primary and Gibson, Ian W., additional
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- 2019
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17. Long-Term Changes in Bone Mineral Density in Kidney Transplant Recipients
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Anthony B. Hodsman, William D. Leslie, Kyla L. Naylor, Amit X. Garg, and David N. Rush
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Adult ,Male ,Quality Control ,medicine.medical_specialty ,Bone density ,Urology ,Renal function ,Standard score ,Kidney transplant ,Absorptiometry, Photon ,Bone Density ,Humans ,Medicine ,Longitudinal Studies ,Femoral neck ,Bone mineral ,Transplantation ,Femur Neck ,business.industry ,Manitoba ,Middle Aged ,Kidney Transplantation ,Transplant Recipients ,medicine.anatomical_structure ,Kidney Failure, Chronic ,Osteoporosis ,Female ,Lumbar spine ,business - Abstract
BACKGROUND Alterations in bone mineral metabolism occur when kidney function declines and often continue after transplantation. We investigated long-term changes in bone mineral density (BMD) among kidney transplant recipients undergoing routine clinical BMD monitoring and management. METHODS We identified adults receiving a kidney transplant in the province of Manitoba, Canada (1996-2011) who had greater than or equal to 2 posttransplant dual energy X-ray absorptiometry examinations. Bone mineral density was expressed as Z scores (standard deviation above/below sex-matched and age-matched reference data). The main outcome was the change in BMD. RESULTS A total of 326 kidney transplant recipients were included (mean age, 45 years; 61% men). Recipients were followed up for an average of 8.2 years (766 follow-up dual energy X-ray absorptiometry measurements). At baseline (first scan; median, 0.5 years after transplantation), bone density was slightly below average for age and sex (mean Z scores: lumbar spine, -0.4 ± 1.6; femoral neck, -0.7 ± 1.1; total hip, -0.7 ± 1.1). At the second scan (mean, 2.7 years after first scan), mean bone density Z scores have increased (lumbar spine, -0.2 ± 1.6; femoral neck, -0.6 ± 1; total hip, -0.6 ± 1.1; matched, P < 0.01 at all sites). The only factor associated with a significant BMD change at all sites was osteoporosis treatment (BMD increase). Even after restricting the analysis to recipients who had not received osteoporosis treatment, final mean bone density (mean, 8.2 years after first scan) was average for age and sex (lumbar spine, +0.7 ± 1.6; femoral neck, -0.1 ± 1.1; total hip, 0.0 ± 1.1). CONCLUSION With routine BMD monitoring and management, posttransplant bone density typically remains stable or improves with mean values that are average for age and sex.
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- 2014
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18. Effect of Time on Dialysis and Renal Transplantation on Endothelial Function
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Keren Mandelzweig, Manish M. Sood, Paul Komenda, Peter Nickerson, Joe Bueti, Brett Hiebert, David N. Rush, Claudio Rigatto, Yang Xu, and Navdeep Tangri
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Adult ,Male ,Time Factors ,Vascular cell adhesion molecule ,Endothelium ,medicine.medical_treatment ,Population ,Vascular Cell Adhesion Molecule-1 ,Translational study ,Inflammation ,Cohort Studies ,Endothelial activation ,Renal Dialysis ,Clinical and Translational Research ,medicine ,Humans ,Longitudinal Studies ,Endothelial dysfunction ,education ,Dialysis ,Retrospective Studies ,Transplantation ,education.field_of_study ,Cell adhesion molecule ,business.industry ,Middle Aged ,Cardiovascular disease ,medicine.disease ,Kidney Transplantation ,medicine.anatomical_structure ,Cardiovascular Diseases ,Immunology ,Kidney Failure, Chronic ,Female ,Endothelium, Vascular ,medicine.symptom ,business ,Biomarkers - Abstract
Background Soluble vascular cell adhesion molecule-1 (sVCAM-1) is a marker of endothelial injury and a potent predictor of cardiovascular mortality in patients with kidney failure on dialysis. The longitudinal effects of dialysis on endothelial dysfunction and in particular the effects of renal transplantation on markers of endothelial function including sVCAM-1 have not been well characterized. Methods We used the Transplant Manitoba registry and biobank to assemble a retrospective cohort of all patients receiving a first kidney transplant between January 1, 2000, and December 31, 2005 (n=186). One hundred seventy-four patients had at least two serum samples pretransplant and at least two samples posttransplant. In total, 1,004 serial samples (median 5/patient) were analyzed. Factors associated with sVCAM-1 were examined using mixed linear models. Results The sVCAM-1 levels increased progressively on dialysis (0.15 [0.10 to 0.20] ng/mL/day; P, Supplemental digital content is available in the article.
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- 2014
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19. Antibody-Mediated Rejection
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María J. Paniagua-Martín, María G. Crespo-Leiro, Ian W. Gibson, Elisabeth Schwaiger, Marcos López-Hoyos, Peter Nickerson, Daniel Serón, Georg A. Böhmig, Raquel Marzoa-Rivas, Eduardo Barge-Caballero, Joana Sellarés, Antonio Roman, David San Segundo, David N. Rush, Manuel Arias, Chris Wiebe, and Tom Blydt-Hansen
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Transplantation ,Text mining ,business.industry ,Antibody mediated rejection ,Medicine ,Computational biology ,business - Published
- 2014
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20. FRAX Predicts Fracture Risk in Kidney Transplant Recipients
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Anthony B. Hodsman, Amit X. Garg, William D. Leslie, Kyla L. Naylor, and David N. Rush
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Adult ,Male ,Fracture risk ,medicine.medical_specialty ,FRAX ,Population ,World Health Organization ,Risk Assessment ,Cohort Studies ,Bone Density ,Risk Factors ,Interquartile range ,Internal medicine ,Humans ,Medicine ,Renal Insufficiency ,education ,Probability ,Proportional Hazards Models ,Bone mineral ,Transplantation ,education.field_of_study ,business.industry ,Hazard ratio ,Area under the curve ,Manitoba ,Middle Aged ,Prognosis ,Kidney Transplantation ,Area Under Curve ,Calibration ,Cohort ,Female ,business ,Osteoporotic Fractures ,Follow-Up Studies - Abstract
Background The World Health Organization Fracture Risk Assessment Tool (FRAX) estimates the 10-year fracture probability. We assessed the prognostic value of FRAX in kidney transplant recipients, as its utility in recipients is unknown. Methods We considered 458 individuals (mean age 45 years, 64% men) who received a kidney transplant in the province of Manitoba, Canada at the time of their first bone mineral density (BMD) test posttransplant (mean 1.1 years posttransplant; transplant years 1996–2011). FRAX probabilities were calculated from baseline information (age, sex, clinical risk factors, with or without BMD). Recipients were followed a mean of 6.4 years (interquartile range 3.0–10.0 years) after cohort entry for an incident major osteoporotic fracture. Results In follow-up, 21 (4.6%) recipients experienced a major osteoporotic fracture. The observed 10-year major osteoporotic fracture risk of 6.3% (95% CI, 3.4–9.2%) was concordant with FRAX predictions (5.0% with BMD, 5.6% without BMD). Major osteoporotic fracture scores showed significant fracture prediction (hazard ratio per standard deviation, FRAX without BMD 1.66, 95% CI, 1.10–2.50; FRAX with BMD 1.64, 95% CI, 1.07–2.51). Area under the curve (AUC) for incident major osteoporotic fracture discrimination (AUC: FRAX with BMD 0.62, 95% CI, 0.50–0.74) was similar to the general population. Conclusions FRAX scores categorized most kidney transplant recipients as a low-risk fracture group, and the low observed fracture rates were consistent with the 10-year fracture predictions. FRAX showed modest fracture prediction and discrimination similar to the general population. Independent validation is needed before clinicians can routinely use FRAX in kidney transplant recipients.
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- 2014
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21. Analysis of Biomarkers Within the Initial 2 Years Posttransplant and 5-Year Kidney Transplant Outcomes
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Faddoul, Geovani, primary, Nadkarni, Girish N., additional, Bridges, Nancy D., additional, Goebel, Jens, additional, Hricik, Donald E., additional, Formica, Richard, additional, Menon, Madhav C., additional, Morrison, Yvonne, additional, Murphy, Barbara, additional, Newell, Kenneth, additional, Nickerson, Peter, additional, Poggio, Emilio D., additional, Rush, David, additional, and Heeger, Peter S., additional
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- 2018
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22. Increased Urinary CCL2
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David N. Rush, Julie Ho, Leroy Storsley, Ian W. Gibson, Chris Wiebe, Ang Gao, Martin Karpinski, Claudio Rigatto, and Peter Nickerson
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Adult ,Male ,medicine.medical_specialty ,Time Factors ,Urinary system ,Urology ,Delayed Graft Function ,Enzyme-Linked Immunosorbent Assay ,Kaplan-Meier Estimate ,Urine ,chemistry.chemical_compound ,Risk Factors ,Humans ,Medicine ,Prospective Studies ,Prospective cohort study ,Chemokine CCL2 ,Proportional Hazards Models ,Transplantation ,Creatinine ,Kidney ,business.industry ,Proportional hazards model ,Graft Survival ,Age Factors ,Manitoba ,Middle Aged ,Kidney Transplantation ,Up-Regulation ,Treatment Outcome ,medicine.anatomical_structure ,ROC Curve ,chemistry ,Multivariate Analysis ,Cohort ,Female ,business ,Biomarkers ,Cohort study - Abstract
BACKGROUND Early noninvasive markers that identify patients at risk of renal allograft loss may stratify patients for more intensive monitoring or therapy. CCL2 is a CCR2 receptor chemokine that is a chemoattractant protein for monocytes/macrophages, T cells, and natural killer cells. We have previously demonstrated in a multicenter cohort that urinary CCL2 at 6 months is an independent predictor for the development of IFTA at 24 months. The goal of this study was to determine if early urinary CCL2 is a predictor of graft loss in an independent patient cohort. METHODS A prospective, observational cohort study was conducted in the Transplant Manitoba Adult Kidney Program (n=231 patients) from 1997 to 2008. Six-month urinary CCL2 was measured by ELISA, corrected for urinary creatinine, and correlated with long-term graft outcomes. RESULTS Urine CCL2: Cr at 6 months was significantly associated with death-censored graft loss (HR, 2.42; 95% CI, 1.54-3.82, P
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- 2013
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23. Six-Month Urinary CCL2 and CXCL10 Levels Predict Long-term Renal Allograft Outcome
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Stefan Schaub, Peter Nickerson, David N. Rush, Chris Wiebe, Julie Ho, Ang Gao, Helmut Hopfer, and Patricia Hirt-Minkowski
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Adult ,Graft Rejection ,Male ,medicine.medical_specialty ,Time Factors ,medicine.medical_treatment ,Urinary system ,030232 urology & nephrology ,Urology ,Renal function ,Kaplan-Meier Estimate ,030230 surgery ,Urinalysis ,Disease-Free Survival ,03 medical and health sciences ,0302 clinical medicine ,Interquartile range ,Predictive Value of Tests ,Risk Factors ,medicine ,CXCL10 ,Humans ,Prospective Studies ,Chemokine CCL2 ,Proportional Hazards Models ,Transplantation ,Chi-Square Distribution ,business.industry ,Hazard ratio ,Graft Survival ,Reproducibility of Results ,Immunosuppression ,Middle Aged ,Allografts ,Kidney Transplantation ,Confidence interval ,Surgery ,Chemokine CXCL10 ,Treatment Outcome ,ROC Curve ,Area Under Curve ,Creatinine ,Cohort ,Multivariate Analysis ,Female ,business ,Biomarkers ,Switzerland ,Glomerular Filtration Rate - Abstract
BACKGROUND Early prognostic markers that identify high-risk patients could lead to increased surveillance, personalized immunosuppression, and improved long-term outcomes. The goal of this study was to validate 6-month urinary chemokine ligand 2 (CCL2) as a noninvasive predictor of long-term outcomes and compare it with 6-month urinary CXCL10. METHODS A prospective, observational renal transplant cohort (n = 185; minimum, 5-year follow-up) was evaluated. The primary composite outcome included 1 or more: allograft loss, renal function decline (>20% decrease estimated glomerular filtration rate between 6 months and last follow-up), and biopsy-proven rejection after 6 months. CCL2/CXCL10 are reported in relation to urine creatinine (ng/mmol). RESULTS Fifty-two patients (52/185, 28%) reached the primary outcome at a median 6.0 years, and their urinary CCL2:Cr was significantly higher compared with patients with stable allograft function (median [interquartile range], 38.6 ng/mmol [19.7-72.5] vs 25.9 ng/mmol [16.1-45.8], P = 0.009). Low urinary CCL2:Cr (≤70.0 ng/mmol) was associated with 88% 5-year event-free survival compared with 50% with high urinary CCL2:Cr (P < 0.0001). In a multivariate Cox-regression model, the only independent predictors of the primary outcome were high CCL2:Cr (hazard ratio [HR], 2.86; 95% confidence interval [95% CI], 1.33-5.73) and CXCL10:Cr (HR, 2.35; 95% CI, 1.23-4.88; both P = 0.009). Urinary CCL2:Cr/CXCL10:Cr area under the curves were 0.62 (P = 0.001)/0.63 (P = 0.03), respectively. Time-to-endpoint analysis according to combined high or low urinary chemokines demonstrates that endpoint-free survival depends on the overall early chemokine burden. CONCLUSIONS This study confirms that urinary CCL2:Cr is an independent predictor of long-term allograft outcomes. Urinary CCL2:Cr/CXCL10:Cr alone have similar prognostic performance, but when both are elevated, this suggests a worse prognosis. Therefore, urinary chemokines may be a useful tool for timely identification of high-risk patients.
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- 2016
24. Impact of Intestinal Motility, Mucosal Inflammation and Fecal Microflora on Transplant Intestine Function
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Burcin Ekser, Shekhar Kubal, Romil Saxena, Richard S. Mangus, Mark Tann, Benjamin Maccaby, Gao Xiang, Qunfeng Dong, Jonathan A. Fridell, Natalia I. Rush, Lin Huaiying, David R. Nelson, and Evelyn Toh
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Transplantation ,business.industry ,Immunology ,Mucosal inflammation ,Medicine ,business ,Feces ,Function (biology) ,Intestinal motility - Published
- 2017
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25. Single-Nucleotide Polymorphisms, Acute Rejection, and Severity of Tubulitis in Kidney Transplantation, Accounting for Center-to-Center Variation
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Ajay, Israni, Robert, Leduc, John, Holmes, Pamala A, Jacobson, Vishal, Lamba, Weihua, Guan, David, Schladt, Jinbo, Chen, Arthur J, Matas, William S, Oetting, and David, Rush
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Adult ,Graft Rejection ,Male ,Canada ,Time Factors ,Genotype ,Single-nucleotide polymorphism ,Accounting ,Polymorphism, Single Nucleotide ,Severity of Illness Index ,Article ,Genetic variation ,Severity of illness ,Humans ,SNP ,Medicine ,Kidney transplantation ,Proportional Hazards Models ,Transplantation ,business.industry ,Proportional hazards model ,Genetic Variation ,Middle Aged ,medicine.disease ,Kidney Transplantation ,United States ,Kidney Tubules ,Multivariate Analysis ,Cohort ,Kidney Failure, Chronic ,Female ,business ,Kidney disease - Abstract
Background. Acute rejection (AR) is associated with worse renal allograft outcomes. Therefore, this study investigated single-nucleotide polymorphisms (SNPs) to identify genetic variants associated with AR, accounting for center variation, in a multicenter, prospective, observation study. Methods. We enrolled patients from six transplant centers, five in the United States and one in Canada. A total of 2724 SNPs were genotyped. We accounted for center variation in AR rates by stratifying by transplant center and using novel knowledge discovery methods. Results. There was significant center variation in AR rates across the six transplant sites (P
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- 2010
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26. Long-Term Medical Outcomes Among Aboriginal Living Kidney Donors
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Julie Ho, Peter Nickerson, Leroy Storsley, Vuthana Suon, David N. Rush, Martin Karpinski, and Ann Young
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Male ,Parents ,medicine.medical_specialty ,Renal function ,chemistry.chemical_compound ,Diabetes mellitus ,Internal medicine ,Living Donors ,medicine ,Humans ,Kidney transplantation ,Ontario ,Transplantation ,Creatinine ,business.industry ,Siblings ,Body Weight ,Manitoba ,Retrospective cohort study ,Middle Aged ,medicine.disease ,Kidney Transplantation ,Surgery ,Proteinuria ,Treatment Outcome ,chemistry ,Indians, North American ,Female ,business ,Follow-Up Studies ,Cohort study ,Kidney disease - Abstract
BACKGROUND: It is unknown whether favorable long-term data on the safety of living kidney donation can be extrapolated to populations at higher risk of chronic kidney disease. Indigenous people (i.e., Aboriginals) have a high prevalence of risk factors for chronic kidney disease and Aboriginal living donor outcomes need to be defined. METHODS: We performed a retrospective cohort study of all 38 Aboriginal donors donating at our center since 1970 and 76 randomly selected white donor controls to determine the long-term rates of hypertension, diabetes, and renal function postdonation. RESULTS: Follow-up was obtained for 91% of both Aboriginal and white donors (mean follow-up approximately 14 years). Hypertension has been diagnosed more frequently among Aboriginal donors (Ab 42% vs. white 19%, P=0.02). Notably, all 11 Aboriginal donors more than 20 years postdonation have developed hypertension. Diabetes has also been diagnosed more frequently among Aboriginal donors (Ab 19% vs. white 2%, P=0.005), including 5 of 11 (45%) more than 20 years postdonation. Follow-up estimated glomerular filtration rate was higher in Aboriginal donors (Ab 77+/-17 vs. white 67+/-13 mL/min/1.73 m, P=0.002) but not significantly different in adjusted analyses. One Aboriginal donor developed end-stage renal disease 14 years postdonation. CONCLUSIONS: Aboriginal living kidney donors at our center have high rates of hypertension and diabetes on long-term follow-up, although renal function is preserved to date. This profile is similar to that of the general unselected Aboriginal population despite detailed medical evaluation before donation. These findings have important implications for donor counseling and may have implications for other high-risk donor populations.
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- 2010
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27. CD40 Inhibition with CFZ533-A New, Fully Human, Non-Depleting, Fc Silent mAB - Improves Renal Allograft Function While Demonstrating Comparable Efficacy vs. Tacrolimus in De-Novo CNI-Free Kidney Transplant Recipients
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B Haraldsson, Oliver Witzke, M. van den Hoogen, D Leeser, J Rush, Shamkant Mulgaonkar, Diane M. Cibrik, J Pratschke, U Laessing, A Patel, Bjoern Nashan, Claudia Sommerer, Stefan P Berger, Rita R. Alloway, A D van Zuilen, H. Tedesco, and Alexander C. Wiseman
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0301 basic medicine ,Transplantation ,medicine.medical_specialty ,CD40 ,biology ,business.industry ,medicine.drug_class ,Urology ,Monoclonal antibody ,Kidney transplant ,Tacrolimus ,03 medical and health sciences ,030104 developmental biology ,0302 clinical medicine ,030220 oncology & carcinogenesis ,Renal allograft ,biology.protein ,Medicine ,business ,Function (biology) - Published
- 2018
28. Anti-CD40 Antibodies do not Cause Thromboembolism as Demonstrated by in Vitro and in Vivo Studies
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Nathalie Runser Loll, Esther Erard, Deborah Garcia, James S. Rush, Thierry Flandre, Serge Côté, Peter Ulrich, Brigitte Christen, Benjamin Cochin de Billy, Tina Rubic-Schneider, and Sebastien Nock
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Transplantation ,biology ,business.industry ,In vivo ,biology.protein ,Medicine ,Anti cd40 ,Pharmacology ,Antibody ,business ,In vitro - Published
- 2018
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29. Factors Associated With Progression of Interstitial Fibrosis in Renal Transplant Patients Receiving Tacrolimus and Mycophenolate Mofetil
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Jean-Guy Lachance, David N. Rush, Ahmed Shoker, Sandra Cockfield, Anne Boucher, Dianne J. Arlen, Stephan Busque, Catherine Girardin, Peter Nickerson, Serdar Yilmaz, R. Jean Shapiro, Gregory A. Knoll, and David Landsberg
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Adult ,Graft Rejection ,Male ,medicine.medical_specialty ,Biopsy ,Urology ,Renal function ,Tacrolimus ,Mycophenolic acid ,HLA Antigens ,Prednisone ,Internal medicine ,Cadaver ,Living Donors ,medicine ,Humans ,Antibacterial agent ,Transplantation ,Kidney ,business.industry ,Middle Aged ,Mycophenolic Acid ,Fibrosis ,Kidney Transplantation ,Tissue Donors ,Calcineurin ,Endocrinology ,medicine.anatomical_structure ,Disease Progression ,Regression Analysis ,Female ,business ,Immunosuppressive Agents ,medicine.drug - Abstract
Background. We recently reported a randomized study in renal transplant patients (RTP) receiving tacrolimus, mycophenolate mofetil, and prednisone in which patients who had early protocol biopsies (PBx) derived no benefit compared with controls (no PBx) at 6 months, likely due to the low prevalence of subclinical rejection. We report on the follow-up of these patients to 24 months at which time a repeat PBx and tests of renal function were performed. Methods. Of the 240 RTP randomized, 22 were excluded for a protocol violation. Approximately 75% of the remaining 218 ( 111 PBx and 107 controls) completed the study. Results. At 24 months, graft function was excellent with a mean creatinine clearance of approximately 74 mL/min and negligible proteinuria; however, the prevalence of interstitial fibrosis and tubular atrophy (IF/TA)—ci + ct more than or equal to 2—increased from approximately 3% at baseline to up to 40% to 50%. By logistic regression analysis, the only independent positive correlate of IF/TA was transplantation with a deceased donor. However, by post hoc analysis, use of angiotensin-II-converting enzyme inhibitors or angiotensin II receptor blockers was negatively correlated with both the prevalence of IF/TA at 24 months and its progression between 6 and 24 months in RTP that had paired biopsies. Conclusions. A regimen of tacrolimus, mycophenolate mofetil, and prednisone results in excellent renal function at 24 months posttransplant but with a progressive increase in IF/TA. A potential inhibitory effect of angiotensin-II-converting enzyme inhibitor/angiotensin II receptor blockers on IF/TA is suggested that requires confirmation in a randomized study.
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- 2009
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30. Subclinical Antibody-Mediated Rejection
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Arias, Manuel, primary, Serón, Daniel, additional, Herrero, Ignacio, additional, Rush, David N., additional, Wiebe, Chris, additional, Nickerson, Peter W., additional, Ussetti, Piedad, additional, Rodrigo, Emilio, additional, and de Cos, Maria-Angeles, additional
- Published
- 2017
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31. Impact of Intestinal Motility, Mucosal Inflammation and Fecal Microflora on Transplant Intestine Function
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Kubal, Shekhar, primary, Mangus, Richard, additional, Huaiying, Lin, additional, Xiang, Gao, additional, Dong, Qunfeng, additional, Toh, Evelyn, additional, Rush, Natalia, additional, Saxena, Romil, additional, Tann, Mark, additional, Maccaby, Benjamin, additional, Ekser, Burcin, additional, Fridell, Jonathan, additional, and Nelson, David, additional
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- 2017
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32. Mucosal Macrophage Accumulation is an Early Event in Exfoliative Rejection of Intestinal Allografts
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Rush, Natalia, primary, Saxena, Romil, additional, Mangus, Richard, additional, Ekser, Burcin, additional, Fridell, Jonathan, additional, and Kubal, Shekhar, additional
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- 2017
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33. Detection of subclinical tubular injury after renal transplantation: comparison of urine protein analysis with allograft histopathology
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Michael J. Mihatsch, Michael Mayr, Axel Regeniter, Peter Nickerson, Gideon Hönger, David N. Rush, Jennifer Bestland, John A. Wilkins, Stefan Schaub, and Jürg Steiger
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Adult ,Graft Rejection ,Male ,Pathology ,medicine.medical_specialty ,Tubular atrophy ,Biopsy ,Urinary system ,030232 urology & nephrology ,030230 surgery ,Kidney ,Asymptomatic ,03 medical and health sciences ,0302 clinical medicine ,Lipocalin-2 ,Proto-Oncogene Proteins ,medicine ,Albuminuria ,Humans ,Transplantation, Homologous ,alpha-Macroglobulins ,Kidney transplantation ,Aged ,Subclinical infection ,Transplantation ,business.industry ,Hydrogen-Ion Concentration ,Middle Aged ,medicine.disease ,Kidney Transplantation ,Lipocalins ,3. Good health ,Retinol-Binding Proteins ,Kidney Tubules ,Tubular proteinuria ,Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization ,Female ,Kidney Diseases ,medicine.symptom ,beta 2-Microglobulin ,business ,Biomarkers ,Acute-Phase Proteins ,Kidney disease - Abstract
BACKGROUND Tubulointerstitial injury due to rejection leads to tubular atrophy (TA)/interstitial fibrosis (IF) followed by deterioration of allograft function. This study investigated whether urinary tubular injury biomarkers can detect subclinical tubulitis found in protocol biopsies allowing for a noninvasive screening procedure. METHODS Four rigidly defined groups (stable transplants with normal tubular histology [n=24], stable transplants with subclinical tubulitis [n=38], patients with clinical tubulitis Ia/Ib [n=18], and patients with other clinical tubular pathologies [n=20]) were compared for differences in urinary intact/cleaved beta2-microglobulin (i/cbeta2m), retinol-binding protein (RBP), neutrophil-gelatinase-associated lipocalin (NGAL), and alpha1-microglobulin (alpha1m). RESULTS Tubular proteinuria was present in 38% (RBP) to 79% (alpha1m) of patients in the stable transplant with normal tubular histology group. The stable transplant with subclinical tubulitis group had slightly higher levels of i/cbeta2m (P=0.11), RBP (P=0.17), alpha1m (P=0.09), and NGAL (P=0.06) than the stable transplant with normal tubular histology group with a substantial overlap. The clinical tubulitis Ia/Ib and the other clinical tubular pathology groups had significantly higher levels of RBP, NGAL, and alpha1m than stable transplants with normal tubular histology or stable transplants with subclinical tubulitis (P
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- 2007
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34. The Relative Importance of Cytokine Gene Polymorphisms in the Development of Early and Late Acute Rejection and Six-Month Renal Allograft Pathology
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Ian V. Hutchinson, Peter Nickerson, John Jeffery, Kathryn Tinckam, David N. Rush, Iga Dembinski, and Vera Pravica
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Adult ,Graft Rejection ,medicine.medical_specialty ,Pathology ,Time Factors ,Biopsy ,medicine.medical_treatment ,Donor Selection ,Random Allocation ,Odds Ratio ,Humans ,Transplantation, Homologous ,Medicine ,Kidney transplantation ,Subclinical infection ,Transplantation ,Polymorphism, Genetic ,business.industry ,Donor selection ,Anatomical pathology ,Immunosuppression ,Odds ratio ,medicine.disease ,Kidney Transplantation ,Logistic Models ,Phenotype ,Relative risk ,Cytokines ,business ,Follow-Up Studies - Abstract
BACKGROUND: Acute rejection episodes and 6-month protocol biopsy acute pathology are highly correlated with long-term outcomes in renal transplant recipients. Recurrent, vascular, and late rejections are particularly deleterious. METHODS: We determined the relative contribution of human leukocyte antigen matching, cytokine genotypes, delayed graft function (DGF), and baseline immunosuppression to the development of acute rejection and allograft pathology in 118 renal transplant recipients. RESULTS: Multivariate logistic regression modeling demonstrated that the adjusted odds ratio and 95% confidence interval for recurrent (> or =2) early rejections (0-3 months) increased linearly for high (H) > intermediate (I) > low (L) interferon-gamma (1.8; 1.1-3.2) and tumor necrosis factor (TNF)alpha (3.0; 1.3-6.9) genotype, whereas every 1 microg/L increase in the cyclosporine A level was protective (0.991; 0.984-0.999). The odds ratio for recurrent late rejections (4-6 months) increased for H > I > L TNFalpha (5.1; 1.8-14.7) genotype and DGF (7.1; 1.6-30.2), whereas H > I/L transforming growth factor-beta1 genotype decreased the relative risk (0.09: 0.02-0.49). Vascular rejection was only predicted by H > I > L TNFalpha phenotype (3.0; 1.2-7.9). The odds ratio for the 6-month Banff Acute Score (6A > or= 4) increased for H > I > L TNFalpha (2.7; 1.1-6.7) and interleukin-10 (3.4; 1.2-6.2) genotype, and DGF (3.4; 1.1-11.5). Treatment of early subclinical rejection decreased the relative risk (0.20; 0.07-0.62). CONCLUSIONS: High transforming growth factor-beta1 producer phenotype seems to be protective against acute inflammation, whereas H and I interferon-gamma, TNFalpha, and interleukin-10 producer genotypes correlate with adverse outcomes. Cytokine genotyping identifies individuals who may benefit from more intensive surveillance and treatment posttransplant.
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- 2005
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35. Epidemiology of Epstein-Barr Virus Chronic High Viral Load in Kidney Transplant Recipients
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Rampersad, Christie, Wiebe, Chris, Balshaw, Robert, Bullard, Jared, Cortes Villalobos, Armelle Perez, Trachtenberg, Aaron, Shaw, James, Karpinski, Martin, Goldberg, Aviva, Birk, Patricia, Pinsk, Maury, Rush, David N., Nickerson, Peter W., and Ho, Julie
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- 2024
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36. PRESERVATION OF HUMAN PANCREATIC ISLET IN VIVO FUNCTION AFTER 6-MONTH CULTURE IN SERUM-FREE MEDIA1
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A. Osama Gaber, Malak Kotb, Lillian W. Gaber, Agnes Lo, Benjamin T. Rush, Omaima M. Sabek, Abdel-Baset Halim, and Daniel W. Fraga
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Transplantation ,medicine.medical_specialty ,geography ,geography.geographical_feature_category ,Insulin ,medicine.medical_treatment ,Stimulation ,Nod ,Biology ,medicine.disease ,Islet ,In vitro ,Endocrinology ,In vivo ,Diabetes mellitus ,Internal medicine ,medicine - Abstract
Background. Culturing human islets in Memphis serum-free media (M-SFM) is associated with excellent postculture recovery, in vitro function, and in vivo survival. The authors investigate the possibility of preserving islet function for extended periods (6 months) in culture and describe the in vitro and in vivo functional outcomes associated with these extended culture times. Methods. Human islets isolated from three cadaveric donor organs were cultured in M-SFM for 1, 3, or 6 months before transplantation under the kidney capsule of nonobese diabetic (NOD)-severe combined immunodeficiency (SCID) mice. In vitro function was measured by static incubation at the time of transplantation. In vivo function was assessed by measuring human insulin and C-peptide production, and by the ability of 6-month cultured islets to cure streptozotocin-induced diabetes in this mouse model. Results. Islet recovery ratios after 1 month in culture ranged from 85% to 88% and declined to 28% to 53% after 6 months of culture (P
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- 2004
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37. Mucosal Macrophage Accumulation is an Early Event in Exfoliative Rejection of Intestinal Allografts
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Shekhar Kubal, Richard S. Mangus, Natalia I. Rush, Romil Saxena, Jonathan A. Fridell, and Burcin Ekser
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Transplantation ,business.industry ,Event (relativity) ,Immunology ,Medicine ,Macrophage ,business - Published
- 2017
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38. Elevated urinary CCL2: Cr at 6 months is associated with renal allograft interstitial fibrosis and inflammation at 24 months
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David N. Rush, Sabine Hombach-Klonisch, Peter Nickerson, Leroy Storsley, Claudio Rigatto, Julie Ho, Ang Gao, Martin Karpinski, Ian W. Gibson, and Chris Wiebe
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Adult ,Male ,medicine.medical_specialty ,Canada ,Time Factors ,Urinary system ,Biopsy ,Urology ,Inflammation ,CCL2 ,Fibrosis ,Risk Factors ,Odds Ratio ,Medicine ,Humans ,Prospective Studies ,Chemokine CCL2 ,Transplantation ,Chi-Square Distribution ,medicine.diagnostic_test ,business.industry ,Transplant glomerulopathy ,Histology ,Middle Aged ,medicine.disease ,Kidney Transplantation ,United States ,Up-Regulation ,Logistic Models ,Creatinine ,Immunology ,Cohort ,Chronic Disease ,Multivariate Analysis ,Linear Models ,Nephritis, Interstitial ,Female ,medicine.symptom ,business ,Biomarkers - Abstract
BACKGROUND We have demonstrated that 6-month urinary CCL2: Cr is a predictor of interstitial fibrosis and tubular atrophy (IFTA) on 24-month biopsy and death-censored graft loss. However, IFTA is no longer considered prognostically significant, whereas patients with graft loss frequently have interstitial fibrosis and inflammation (IF+i=ci>0+i>0). As early CCL2: Cr predicts late graft loss, the goal of this study was to determine if 6-month urinary CCL2: Cr was a predictor of IF+i at 24 months. METHODS Urinary CCL2 at 6 months was measured with ELISA and correlated with IF+i on 24-month surveillance biopsies from a prospective, multicenter adult renal transplant cohort (n=111). RESULTS Six-month urinary CCL2: Cr was significantly higher in IF+i and transplant glomerulopathy patients compared with normal histology at 24 months. By multivariate analysis, 6-month urinary CCL2: Cr was independently correlated with IF+i at 24 months (OR 2.78, 95% CI 1.38-6.12, AUC 0.695, P=0.003). Six-month urinary CCL2: Cr was also an independent correlate of 6-month IF+i (OR 1.99, 95% CI 1.03-4.18, AUC 0.63, P=0.04). Six-month urinary CCL2: Cr distinguished noninflamed renal tissue (normal, fibrosis) from IF+i with a sensitivity/specificity of 0.71/0.62 at a cutoff of 15 ng CCL2/mmol Cr (AUC 0.695, P=0.003, n=91). CONCLUSIONS Urinary CCL2: Cr may be useful for the noninvasive identification of patients with or at risk for IF+i. These patients may benefit from avoidance of drug minimization/withdrawal protocols and more intensive post-transplant surveillance. Furthermore, urinary CCL2: Cr may also identify individuals who may benefit from novel interventional trials targeting IF+i.
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- 2014
39. Six-Month Urinary CCL2 and CXCL10 Levels Predict Long-term Renal Allograft Outcome
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Hirt-Minkowski, Patricia, primary, Rush, David N., additional, Gao, Ang, additional, Hopfer, Helmut, additional, Wiebe, Chris, additional, Nickerson, Peter W., additional, Schaub, Stefan, additional, and Ho, Julie, additional
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- 2016
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40. Optimization of Perioperative Conditions to Prevent Ischemic Cholangiopathy in Donation After Circulatory Death Donor Liver Transplantation
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Kubal, Chandrashekhar, primary, Mangus, Richard, additional, Fridell, Jonathan, additional, Saxena, Romil, additional, Rush, Natalia, additional, Wingler, Matthew, additional, Ekser, Burcin, additional, and Tector, Joseph, additional
- Published
- 2016
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41. Elevated Urinary Matrix Metalloproteinase-7 Detects Underlying Renal Allograft Inflammation and Injury
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Ho, Julie, primary, Rush, David N., additional, Krokhin, Oleg, additional, Antonovici, Mihaela, additional, Gao, Ang, additional, Bestland, Jennifer, additional, Wiebe, Chris, additional, Hiebert, Brett, additional, Rigatto, Claudio, additional, Gibson, Ian W., additional, Wilkins, John A., additional, and Nickerson, Peter W., additional
- Published
- 2016
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42. IMMUNE-ACTIVATION GENE EXPRESSION IN CLINICALLY STABLE RENAL ALLOGRAFT BIOPSIES: MOLECULAR EVIDENCE FOR SUBCLINICAL REJECTION1,2
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John Jeffery, Rachel M. McKenna, David N. Rush, Paul C. Grimm, Mark L. Lipman, James Gough, and Yingnian Shen
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Transplantation ,Pathology ,medicine.medical_specialty ,medicine.medical_treatment ,Interleukin ,Biology ,Asymptomatic ,Fas ligand ,Granzyme B ,Cytokine ,Immune system ,Immunology ,medicine ,medicine.symptom ,Subclinical infection - Abstract
Background. A significant percentage of biopsies from stable, well-functioning renal allografts have histologic findings consistent with acute rejection or borderline rejection. The implication of this finding is not yet fully understood. We analyzed immune-activation gene transcripts in stable protocol biopsies to determine the extent of immunologic activity of graft-infiltrating cells in this setting. Histologic classification of the biopsies was based on the Banff criteria. To emphasize that the tissue samples were procured from grafts with no clinical evidence of impaired function, we interjected the term subclinical into the Banff terminology. This produced three histologic categories : normal, borderline subclinical rejection, and acute subclinical rejection. Methods. We used competitive template polymerase chain reaction techniques to quantify transcript amounts for the constant region of the T-cell receptor β chain; the cytokines, tumor necrosis factor a, interleukin (IL)-1β, transforming growth factor β, interferon γ, IL-2, IL-4, IL-10, and IL-15; and the cytotoxic T lymphocyte effector molecules, granzyme B, perforin, and Fas ligand. Results. We found that histologically normal biopsies were typically devoid of gene transcripts or had very low amounts. Conversely, biopsies with acute subclinical rejection by histologic examination had heightened amounts of transcripts for many of the genes assayed. Borderline subclinical rejection samples showed an intermediate amount of expression. Conclusions. These results demonstrate that histologic features of rejection are often accompanied by enhanced expression of pro-inflammatory gene transcripts, despite the absence of clinically overt graft dysfunction. As this state of subclinical rejection could prove detrimental to long-term graft function, a role for surveillance biopsies of stable grafts with intent to treat subclinical rejection should be considered.
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- 1998
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43. SAFETY AND TOLERABILITY OF CYCLOSPORINE AND CYCLOSPORINE MICROEMULSION DURING 18 MONTHS OF FOLLOW-UP IN STABLE RENAL TRANSPLANT RECIPIENTS
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John Jeffrey, Annette Tan, Raymond Dandavino, Rolf Loertscher, Edward Cole, Norman Muirhead, Paul Handa, David Landsberg, P. Halloran, Patrick S. Parfrey, Anne Boucher, L. C. Paul, Paul Keown, Pierre Daloze, Joseph Lawen, Jeffrey S. Zaltzman, David Russell, Lisa Hendricks, Ahmed Shoker, Calvin R. Stiller, David N. Rush, and Phillip Belitsky
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Transplantation ,medicine.medical_specialty ,Creatinine ,business.industry ,Urology ,Renal function ,Ciclosporin ,medicine.disease ,Nephrotoxicity ,Surgery ,chemistry.chemical_compound ,chemistry ,Tolerability ,medicine ,Adverse effect ,business ,medicine.drug ,Kidney disease - Abstract
Background. There has been concern that the increased drug exposure associated with treatment with cyclosporine microemulsion (CsA-ME) would lead to an increase in adverse events. Methods. The long-term safety and tolerability of conventional cyclosporine (CsA) and CsA-ME were compared in a randomized, multicenter, pharmacoepidemiologic study involving 1097 stable renal transplant patients after 18 months of follow-up. Results. No significant difference was seen in change in serum creatinine or calculated creatinine clearance between the two groups. Episodes of deterioration in renal function (change in serum creatinine ≥20%) were categorized with the following results for CsA-ME versus CsA, respectively: acute rejection, 4.5% vs. 4.5%; chronic rejection, 8% vs. 11%; CsA nephrotoxicity, 12% vs. 7% (P=0.008); transient changes, 17% vs. 12%; other causes, 4% vs. 6%. During the first 6 months of the study, a transient increase in the incidence of gastrointestinal and neurological adverse events was seen in the CsA-ME group compared with the CsA group. Up to 18 months, patients in the CsA group reported significantly fewer hearing and vestibular disorders, but more cardiovascular problems than those in the CsA-ME group (P=0.035). Conclusions. Tolerance to CsA and CsA-ME was similar. Renal function over 18 months was not adversely affected by the increased drug exposure with CsA-ME, although there was a transient increase in nephrotoxicity. The frequency of acute and chronic rejection did not change.
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- 1998
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44. A RANDOMIZED, PROSPECTIVE MULTICENTER PHARMACOEPIDEMIOLOGIC STUDY OF CYCLOSPORINE MICROEMULSION IN STABLE RENAL GRAFT RECIPIENTS1,2,3
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Edward S. Cole, Joseph Lawen, Jeffrey S. Zaltzman, Rolf Loertscher, Phillip Belitsky, Patrick S. Parfrey, David N. Rush, Anne Boucher, Paul Keown, Paul Handa, L. C. Paul, P. Halloran, Norman Muirhead, Calvin R. Stiller, David Russell, Ahmed Shoker, Raymond Dandavino, Pierre Daloze, John Jeffery, and David Landsberg
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Transplantation ,medicine.medical_specialty ,Creatinine ,business.industry ,Urology ,Renal function ,Ciclosporin ,Intestinal absorption ,law.invention ,Surgery ,chemistry.chemical_compound ,Randomized controlled trial ,Tolerability ,chemistry ,law ,medicine ,business ,Adverse effect ,medicine.drug - Abstract
Background. The safety, tolerability, and pharmacokinetics of conventional cyclosporine (ConCsA) and cyclosporine microemulsion (MeCsA) were compared under conditions of normal clinical practice in a prospective, randomized, concentration-controlled, pharmacoepidemiologic study. Methods. Between September 1994 and March 1995, 1097 stable renal transplant recipients in 14 Canadian centers were randomized 2:1 to treatment with MeCsA or ConCsA Patients were commenced on each study drug at a dose equal to their previous therapy with ConCsA, and the dose was adjusted to maintain predose whole blood cyclosporine concentrations within the therapeutic range established for each center. Prednisone and azathioprine were continued unless dose adjustment was required for clinical reasons. Results. The mean cyclosporine concentration was comparable in both treatment groups at all time points throughout the 6 months of follow-up. The mean dose of cyclosporine was 3.6 mg/kg/day in both treatment groups at entry to the study, and declined by 0.3% and by 2.8% in patients receiving ConCsA and MeCsA, respectively. The nature and severity of adverse events were similar in both treatment groups, but there was a transient increase in neurological and gastrointestinal complications in the group receiving MeCsA within the first month after conversion (P
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- 1996
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45. LOW FREQUENCY OF INFILTRATING CELLS INTENSELY EXPRESSING T CELL CYTOKINE mRNA IN HUMAN RENAL ALLOGRAFT REJECTION1,2
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Paul C. Grimm, John Jeffery, David N. Rush, Elzbieta Gospodarek, and Rachel M. McKenna
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Transplantation ,Pathology ,medicine.medical_specialty ,Kidney ,medicine.medical_treatment ,T cell ,Immunosuppression ,In situ hybridization ,Biology ,medicine.disease ,Reverse transcriptase ,medicine.anatomical_structure ,Cytokine ,Immunology ,medicine ,Infiltration (medical) - Abstract
Immunosuppressive drugs used in clinical transplantation block cytokine mRNA transcription in vitro, but clinical rejection episodes are common. An understanding of what cytokine message is transcribed would be helpful in determining what contributes to the success of immunosuppression and provide directions for further research aimed at targeting specific cytokines. Previous studies have examined cytokine mRNA in rejecting solid organ biopsies by the reverse transcriptase polymerase chain reaction (RT-PCR) with variable results. We used nonradioactive in situ hybridization with cytokine-specific riboprobes to determine the frequency of cells expressing cytokine mRNA in the allograft infiltrate. Kidney biopsies were obtained from patients receiving protocol biopsies and with clinical evidence of rejection. Fourteen biopsies with a pathologic diagnosis of rejection were studied. Eight showed no cytokine staining, 2 expressed U-2, and 3 expressed IL-4 and IFN-γ. The positive cells were present at a low frequency (mean 2, range 1-5 per 10 high-power fields). The proportion of kidney biopsies expressing detectable message for interleukin-2 (IL-2), interleukin-4 (IL-4), and interferon-γ (IFN-γ) by in situ hybridization were similar to those reported using RT-PCR. The novel finding is that these cytokines are expressed in a few strongly positive cells in the allograft infiltrate. The vast majority of infiltrating cells are negative. This suggests that either the biopsies were performed when cytokine message was not expressed at a high level or that in human allograft recipients the sustained expression of the cytokines IL-2, IL-4, and IFN-γ may not be necessary for graft rejection
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- 1995
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46. SEQUENTIAL PROTOCOL BIOPSIES IN RENAL TRANSPLANT PATIENTS
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John Jeffery, David N. Rush, and James Gough
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Transplantation ,Creatinine ,medicine.medical_specialty ,Kidney ,medicine.diagnostic_test ,business.industry ,Renal function ,medicine.disease ,Gastroenterology ,Surgery ,chemistry.chemical_compound ,medicine.anatomical_structure ,chemistry ,Prednisone ,Internal medicine ,Biopsy ,Medicine ,business ,Kidney transplantation ,Subclinical infection ,medicine.drug - Abstract
Twenty-five renal transplant patients on a triple immunosuppressive regimen of cyclosporine, azathioprine, and prednisone underwent protocol graft biopsies at 1, 2, 3, 6, and 12 months after transplant regardless of renal function. The histological diagnosis was made with the Banff schema. As reported previously, protocol biopsies revealed a high prevalence of subclinical rejection, as well as "borderline" inflammation, despite levels of CsA considered to be in the therapeutic range. Every biopsy was given a score for the severity of the histological changes (the Banff Score for Inflammatory Changes [BSI]), which permitted the generation of a cumulative BSI over the year of follow-up for each patient. At the end of 1 year, normal histology and excellent renal function (mean serum creatinine < 110 mumol/L) were seen only in transplant patients with the lowest cumulative BSI (P < 0.001). These results suggest that repeated inflammation in the renal allograft, even if subclinical, can lead to its dysfunction. Moreover, it would appear that, at least for the present, protocol biopsies may be required to assess adequately the effectiveness of current immunosuppressive therapies in renal transplant patients.
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- 1995
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47. Genetic and clinical determinants of early, acute calcineurin inhibitor-related nephrotoxicity: results from a kidney transplant consortium
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Pamala A, Jacobson, David, Schladt, Ajay, Israni, William S, Oetting, Yi Cheng, Lin, Robert, Leduc, Weihau, Guan, Vishal, Lamba, Arthur J, Matas, and David, Rush
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Adult ,Graft Rejection ,Male ,ATP Binding Cassette Transporter, Subfamily B ,Adolescent ,Genotype ,Calcineurin Inhibitors ,Biology ,Bioinformatics ,Kidney transplant ,Polymorphism, Single Nucleotide ,Tacrolimus ,Nephrotoxicity ,Acute nephrotoxicity ,Young Adult ,Postoperative Complications ,Risk Factors ,Cytochrome P-450 CYP3A ,Humans ,Genetic Predisposition to Disease ,ATP Binding Cassette Transporter, Subfamily B, Member 1 ,Prospective Studies ,Aged ,Proportional Hazards Models ,Aged, 80 and over ,Transplantation ,Middle Aged ,Kidney Transplantation ,Calcineurin ,Immunology ,Acute Disease ,Cyclosporine ,Female ,Kidney Diseases ,Complication ,Immunosuppressive Agents ,Follow-Up Studies - Abstract
Calcineurin inhibitor (CNI)-related acute nephrotoxicity is a common complication of transplantation. Clinical factors and elevated CNI levels are associated with nephrotoxicity; however, they do not fully explain the risk. Genetic factors may also predispose individuals to nephrotoxicity.We enrolled 945 kidney recipients into a multicenter, prospective study. DNA was genotyped for 2724 single-nucleotide polymorphisms (SNPs) using a customized chip. Cox models, unadjusted and adjusted for clinical factors, examined the association between SNPs and time to early CNI-related acute nephrotoxicity in the first 6 months posttransplant.Cyclosporine was associated with a 1.49 hazard (95% confidence interval, 1.04-2.14) of acute nephrotoxicity relative to tacrolimus. Acute nephrotoxicity occurred in 22.6% of cyclosporine and 19.8% of tacrolimus recipients. The median (interquartile range) daily dose and trough concentration at time of nephrotoxicity were 400 mg (400-500 mg) and 228 ng/mL (190-272 ng/mL) in the cyclosporine group, and 6 mg (4-8 mg) and 12.6 ng/mL (10.2-15.9 ng/mL) in the tacrolimus group, respectively. In single-SNP adjusted analysis, nine SNPs in the XPC, CYP2C9, PAX4, MTRR, and GAN genes were associated with cyclosporine nephrotoxicity. In a multi-SNP analysis, SNPs from the same genes remained significant after adjusting for the clinical factors, showing that the SNPs are jointly and independently predictive of cyclosporine nephrotoxicity. No SNPs were associated with tacrolimus nephrotoxicity.We identified SNPs that were potentially associated with early, acute cyclosporine-related nephrotoxicity. Identifying risk SNPs before transplantation provides an opportunity for personalization of immunosuppression by identifying those who may benefit from CNI-avoidance or minimization, or assist in selecting CNI type. These SNPs require independent validation.
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- 2012
48. HIGH SERUM LEVELS OF INTERLEUKIN-6 IN RENAL TRANSPLANT RECIPIENTS WITH MONOCLONAL GAMMOPATHIES
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Peter Nickerson, Denise Pochinco, Rachel M. McKenna, Jeffery, and D. Rush
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Transplantation ,Kidney ,biology ,business.industry ,Urinary system ,medicine.medical_treatment ,medicine.anatomical_structure ,Cytokine ,Renal transplant ,Immunopathology ,Monoclonal ,Immunology ,medicine ,biology.protein ,business ,Interleukin 6 - Published
- 1994
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49. INDUCTION IMMUNOSUPPRESSION WITH ANTILYMPHOCYTE GLOBULIN OR OKT3 IN CADAVER KIDNEY TRANSPLANTATION
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Donna Phelan, T. Mohanakumar, Samuel So, Martin D. Jendrisak, Tina M. Rush, Sheila M. Michalski, Douglas W. Hanto, and Christopher S. McCullough
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Adult ,Graft Rejection ,Male ,medicine.medical_specialty ,Adolescent ,medicine.medical_treatment ,Renal function ,chemical and pharmacologic phenomena ,Kidney ,Gastroenterology ,law.invention ,Randomized controlled trial ,law ,Prednisone ,Internal medicine ,Cadaver ,Immune Tolerance ,medicine ,Humans ,Surgical Wound Infection ,Prospective Studies ,Acute tubular necrosis ,Aged ,Antilymphocyte Serum ,Transplantation ,Chemotherapy ,business.industry ,Incidence (epidemiology) ,Graft Survival ,Middle Aged ,medicine.disease ,Kidney Transplantation ,Surgery ,medicine.anatomical_structure ,Antibody Formation ,Female ,business ,Muromonab-CD3 ,medicine.drug - Abstract
Improved cadaver kidney allograft survival rates, shorter duration of acute tubular necrosis, and a reduction in the incidence of rejection have been achieved using "quadruple sequential therapy"--AZA, prednisone, and antilymphocyte globulin (ALG) induction followed by the delayed addition of CsA. OKT3 has been shown to be effective in preventing and treating rejection, including steroid- and ALG-resistant rejection episodes. A single institution prospective randomized trial comparing ALG and OKT3 prophylaxis in first cadaver kidney allograft recipients was performed to assess their relative advantages and disadvantages. First cadaver kidney allograft recipients were prospectively randomized to receive 7 days of either ALG (n = 58) or OKT3 (n = 59) as part of a quadruple therapy protocol that included AZA, prednisone, and oral CsA. Patient characteristics, patient survival and causes of death, graft survival and causes of graft loss, incidence of and time to rejection and response to treatment, incidence of infections and their type, renal function, and antibody formation to ALG and OKT3 were examined. The 1-, 2-, and 3-year actuarial patient survival rates were 96% in the ALG group and 98% in the OKT3 group. The graft survival rates were 81.1%, 78.4%, and 78.4% in the ALG group and 84.1%, 78.7%, and 78.7% in the OKT3 group. In ALG-treated patients, 63% never had rejection, compared with 49% in the OKT3 patients (P = NS). In the ALG group 31% had a single rejection, 6% had 2 rejections, and none had 3 rejections, compared with 37%, 12%, and 2% in the OKT3 group. In the ALG group, 43% were steroid responsive compared with 65% in the OKT3 group (P = 0.08). There were 1.44 infections per patient in the ALG group compared with 0.76 in the OKT3 group (P = 0.0004). In the ALG group, 37% of patients developed CMV disease compared with 10% in the OKT3 group (P = 0.001). In donor-positive/recipient-negative patients, 8/10 (80%) in the ALG group developed CMV infection, of which 6 (75%) had severe or moderate CMV disease, compared with 2/15 (13%) patients in the OKT3 group (P = 0.002), of whom only one (6.7%) developed moderate disease. In donor-positive/recipient-positive patients, 8/23 (35%) in the ALG group developed CMV infection, of whom 5/8 (62.5%) developed severe or moderate disease compared with 1/21 (4.8%) in the OKT3 group (P = 0.02). Antibody formation to ALG and OKT3 occurred in 11% and 8% of patients, respectively.(ABSTRACT TRUNCATED AT 400 WORDS)
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- 1994
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50. Validation of urinary CXCL10 as a marker of borderline, subclinical, and clinical tubulitis
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William P. Stefura, Jennifer Bestland, Peter Nickerson, Kent T. HayGlass, David N. Rush, Martin Karpinski, Julie Ho, Ian W. Gibson, Ang Gao, and Leroy Storsley
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Adult ,Male ,medicine.medical_specialty ,Pathology ,Urinary system ,Urology ,Enzyme-Linked Immunosorbent Assay ,Urine ,chemistry.chemical_compound ,Fibrosis ,Biopsy ,Medicine ,Humans ,Subclinical infection ,Transplantation ,Creatinine ,Nephritis ,Receiver operating characteristic ,medicine.diagnostic_test ,business.industry ,Area under the curve ,Middle Aged ,medicine.disease ,Kidney Transplantation ,Chemokine CXCL10 ,Kidney Tubules ,Logistic Models ,chemistry ,Female ,Atrophy ,business ,Biomarkers - Abstract
Renal allograft injury secondary to subclinical and clinical tubulitis remains an important cause of allograft fibrosis and loss despite modern immunosuppression. The goal of this study was to validate the previously reported use of urinary CXCL10 (interferon-γ-induced protein of 10 kDa) as a noninvasive marker of tubulitis in an independent clinical cohort.Urine samples (n=102) from 91 patients with protocol or indication biopsies were assayed for urinary CXCL10 using ELISA. The groups analyzed were as follows: normal histology (n=22); interstitial fibrosis and tubular atrophy (IFTA) (n=20); IFTA and borderline tubulitis (n=13); borderline (n=13), subclinical (n=17); and clinical tubulitis (n=17) without IFTA.The ratio of urinary CXCL10 to creatinine (CXCL10: Cr) was found to distinguish borderline, subclinical and clinical tubulitis from normal histology, and IFTA. The area under the curve receiver operating characteristic curve to distinguish normal versus borderline and subclinical tubulitis was 0.845 (OR 1.407, P=0.0184); normal versus borderline, subclinical and clinical tubulitis was 0.835 (OR 1.400, P=0.0127). CXCL10: Cr demonstrated a sensitivity of 73.3% and specificity of 72.7% for normal versus borderline and subclinical tubulitis at a cut-off of 1.97 ng CXCL10/mmol Cr.This study validates urinary CXCL10 as a noninvasive, sensitive, and specific marker for tubulitis in an independent cohort. The straightforward urine processing is accessible to clinical laboratories. We propose that CXCL10 may be useful as a supplementary noninvasive screening test for tubulitis in renal transplant patients, with a level more than 1.97 ng CXCL10/mmol Cr being a threshold to consider biopsy.
- Published
- 2011
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