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4. Glucagon-Like Peptide-1 Receptor Agonism Improves Nephrotoxic Serum Nephritis by Inhibiting T-Cell Proliferation

Author

Moschovaki Filippidou, Foteini, Kirsch, Alexander H., Thelen, Matthias, Kétszeri, Máté, Artinger, Katharina, Aringer, Ida, Schabhüttl, Corinna, Mooslechner, Agnes A., Frauscher, Bianca, Pollheimer, Marion, Niedrist, Tobias, Meinitzer, Andreas, Drucker, Daniel J., Pieber, Thomas R., Eller, Philipp, Rosenkranz, Alexander R., Heinemann, Akos, and Eller, Kathrin

Published
2020
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5. Targeting Calcitriol Metabolism in Acute Vitamin D Toxicity—A Comprehensive Review and Clinical Insight.

Author

Aberger, Simon, Schreiber, Nikolaus, Pilz, Stefan, Eller, Kathrin, Rosenkranz, Alexander R., and Kirsch, Alexander H.

Subjects
VITAMIN D, VITAMIN D metabolism, DIETARY supplements, CALCITRIOL
Abstract

High-dose vitamin D supplementation is common in the general population, but unsupervised high-dose supplementation in vitamin D-replete individuals poses a risk of severe toxicity. Susceptibility to vitamin D toxicity shows a significant inter-individual variability that may in part be explained by genetic predispositions (i.e., CYP24A1 polymorphism). The classic manifestation of vitamin D toxicity is hypercalcemia, which may be refractory to conventional therapy. Its causes include the endogenous overaction of 1α-hydroxylase, monogenic alterations affecting vitamin D metabolizing enzymes and exogenous vitamin D intoxication. In this manuscript, we include a literature review of potential pharmacological interventions targeting calcitriol metabolism to treat vitamin D intoxication and present a case of severe, exogenous vitamin D intoxication responding to systemic corticosteroids after the failure of conventional therapy. Systemic glucocorticoids alleviate acute hypercalcemia by inhibiting enteric calcium absorption and increasing the degradation of vitamin D metabolites but may cause adverse effects. Inhibitors of 1α-hydroxylase (keto/fluconazole) and inducers of CYP3A4 (rifampicin) may be considered steroid-sparing alternatives for the treatment of vitamin D intoxication. [ABSTRACT FROM AUTHOR]

Published
2024
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6. MicroRNA-142-3p improves vascular relaxation in uremia

Author

Kétszeri, Máté, Kirsch, Andrijana, Frauscher, Bianca, Moschovaki-Filippidou, Foteini, Mooslechner, Agnes A., Kirsch, Alexander H., Schabhuettl, Corinna, Aringer, Ida, Artinger, Katharina, Pregartner, Gudrun, Ekart, Robert, Breznik, Silva, Hojs, Radovan, Goessler, Walter, Schilcher, Irene, Müller, Helmut, Obermayer-Pietsch, Barbara, Frank, Saša, Rosenkranz, Alexander R., Eller, Philipp, and Eller, Kathrin

Published
2019
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8. Pre-Transplant Frequencies of FoxP3+CD25+ in CD3+CD8+ T Cells as Potential Predictors for CMV in CMV-Intermediate Risk Kidney Transplant Recipients.

Author

Mooslechner, Agnes A., Schuller, Max, Pfeifer, Verena, Klötzer, Konstantin A., Prietl, Barbara, Kirsch, Alexander H., Stiegler, Philipp, Sucher, Robert, Sourij, Harald, Rosenkranz, Alexander R., and Eller, Kathrin

Subjects
T cells, KIDNEY transplantation, MONONUCLEAR leukocytes, CYTOMEGALOVIRUS diseases
Abstract

Cytomegalovirus (CMV) infection detrimentally influences graft survival in kidney transplant recipients, with the risk primarily determined by recipient and donor serostatus. However, recipient CD8+ T cells play a crucial role in CMV control. The optimal preventive strategy (prophylaxis vs. pre-emptive treatment), particularly for seropositive (intermediate risk) recipients, remains uncertain. We investigated CD8+ T cell subpopulation dynamics and CMV occurrence (DNAemia ≥ 100 IU/mL) in 65 kidney transplant recipients, collecting peripheral blood mononuclear cells before (T1) and 1 year after transplantation (T2). Comparing the two timepoints, we found an increase in granulocyte, monocyte and CD3+CD8+ T cells numbers, while FoxP3+CD25+, LAG-3+ and PD-1+ frequencies were reduced at T2. CMV DNAemia occurred in 33 recipients (55.8%) during the first year. Intermediate risk patients were disproportionally affected by posttransplant CMV (N = 29/ 45, 64.4%). Intermediate risk recipients developing CMV after transplantation exhibited lower leukocyte, monocyte, and granulocyte counts and higher FoxP3+CD25+ frequencies in CD3+CD8+ T cells pre-transplantation compared to patients staying CMV negative. Pretransplant FoxP3+CD25+ in CD3+CD8+ T cells had the best discriminatory potential for CMV infection prediction within the first year after transplantation (AUC: 0.746). The FoxP3+CD25+ CD3+CD8+ T cell subset may aid in selecting intermediate risk kidney transplant recipients for CMV prophylaxis. [ABSTRACT FROM AUTHOR]

Published
2024

9. Extracorporeal Techniques in Kidney Failure.

Author

Meijers, Bjorn, Vega, Almudena, Juillard, Laurent, Kawanishi, Hideki, Kirsch, Alexander H., Maduell, Francisco, Massy, Ziad A., Mitra, Sandip, Vanholder, Raymond, Ronco, Claudio, and Cozzolino, Mario

Subjects
KIDNEY failure, CHRONIC kidney failure, OVERALL survival, MOLECULAR spectra
Abstract

During the last decades, various strategies have been optimized to enhance clearance of a variable spectrum of retained molecules to ensure hemodynamic tolerance to fluid removal and improve long-term survival in patients affected by kidney failure. Treatment effects are the result of the interaction of individual patient characteristics with device characteristics and treatment prescription. Historically, the nephrology community aimed to provide adequate treatment, along with the best possible quality of life and outcomes. In this article, we analyzed blood purification techniques that have been developed with their different characteristics. [ABSTRACT FROM AUTHOR]

Published
2024
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10. Differences in drug removal between standard high-flux and medium cut-off dialyzers in a case of severe vancomycin toxicity.

Author

Aberger, Simon, Kolland, Michael, Eller, Kathrin, Rosenkranz, Alexander R, and Kirsch, Alexander H

Subjects
DRUG monitoring, VANCOMYCIN, ACUTE kidney failure, ARTERIAL catheterization, NEPHROTOXICOLOGY, DRUG toxicity
Abstract

Vancomycin is a widely used glycopeptide antibiotic with the need for therapeutic drug monitoring to avoid renal toxicity. We report a case of severe vancomycin-associated anuric acute kidney injury managed with successful drug-removal by hemodialysis (HD) using different types of dialyzers. Medium cut-off (MCO) and high-flux dialyzers were effective in drug removal. Higher vancomycin elimination rate and lower plasma half-life were achieved with MCO dialyzer despite low-flow vascular access and intolerance to ultrafiltration. MCO dialyzers may be reasonable for drug removal in patients with intolerance of ultrafiltration, low-flow vascular access or impracticality of hemodiafiltration. Future studies should explore the use of MCO dialyzers in comparison with high-flux HD and hemodiafiltration in both the acute and chronic setting. [ABSTRACT FROM AUTHOR]

Published
2024
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11. Changes in cardiac troponins during hemodialysis depend on hemodialysis membrane and modality: a randomized crossover trial.

Author

Kolland, Michael, Amenitsch, Jascha, Schreiber, Nikolaus, Ginthör, Noemi, Schuller, Max, Riedl, Regina, Rainer, Peter P, Schneditz, Daniel, Niedrist, Tobias, Eller, Kathrin, Krietemeyer, Benedikt, Rosenkranz, Alexander R, and Kirsch, Alexander H

Subjects
CROSSOVER trials, CHEST pain, NON-ST elevated myocardial infarction, MYOCARDIAL infarction, BRAIN natriuretic factor, HEMODIALYSIS
Abstract

This article discusses the challenges of diagnosing acute coronary syndromes (ACS) in hemodialysis (HD) patients. The study aimed to explore the changes in cardiac troponin (cTn) levels during HD with different membranes and treatment modalities. The results showed significant differences in cTn changes depending on the type of membrane used. The data suggests that high-flux HD and MCO may be more effective in reducing troponin levels compared to low-flux HD and HDF. However, further research is needed to confirm these findings and establish a diagnostic algorithm for AMI in HD patients. [Extracted from the article]

Published
2024
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13. A Murine Model of Phosphate Nephropathy

Author

Eller, Philipp, Eller, Kathrin, Kirsch, Alexander H., Patsch, Josef J., Wolf, Anna M., Tagwerker, Andrea, Stanzl, Ursula, Kaindl, Reinhard, Kahlenberg, Volker, Mayer, Gert, Patsch, Josef R., and Rosenkranz, Alexander R.

Published
2011
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16. Improving adherence to immunosuppression after liver or kidney transplantation in individuals with impairments in personality functioning – A randomized controlled single center feasibility study.

Author

Wagner-Skacel, Jolana, Fink, Nadja, Kahn, Judith, Dalkner, Nina, Jauk, Emanuel, Bengesser, Susanne, Mairinger, Marco, Schüssler, Gerhard, Pieh, Christoph, Stadlbauer, Vanessa, Kirsch, Alexander H., Zitta, Sabine, Rosenkranz, Alexander R., Fickert, Peter, and Schemmer, Peter

Subjects
LIVER transplantation, KIDNEY transplantation, FEASIBILITY studies, IMMUNOSUPPRESSION, PERSONALITY, GROUP psychotherapy
Abstract

Introduction: Although adherence to immunosuppressive medication is the key factor for long-term graft survival today, 20–70% of transplant recipients are nonadherent to their immunosuppressive medication. Objective: A prospective, randomized, controlled single-center feasibility study was designed to evaluate the impact of a step guided multicomponent interprofessional intervention program for patients after kidney or liver transplantation on adherence to their immunosuppressive medication in daily clinical practice. Materials and methods: The intervention consisted of group therapy and daily training as well as individual sessions in a step guided approach. The primary endpoint of the study was adherence to immunosuppression as assessed with the “Basel Assessment of Adherence to Immunosuppressive Medications Scale” (BAASIS). The coefficient of variation (CV%) of Tacrolimus (TAC) through levels and the level of personality functioning was a secondary endpoint. We conducted six monthly follow-up visits. Results: Forty-one age- and sex-matched patients [19 females, 58.5 (SD = 10.56) years old, 22 kidney- and 19 liver transplantation] were randomized to the intervention- (N = 21) or control-group (N = 20). No differences between intervention- and control groups were found in the primary endpoint adherence and CV% of TAC. However, in further exploratory analyses, we observed that individuals with higher impairments in personality functioning showed higher CV% of TAC in the controls. The intervention might compensate personalityrelated susceptibility to poor adherence as evident in CV% of TAC. Discussion: The results of the feasibility study showed that this intervention program was highly accepted in the clinical setting. The Intervention group could compensate higher CV% of TAC after liver or kidney transplantation in individuals with lower levels of personality functioning and non-adherence. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Salivary potassium measured by genetically encoded potassium ion indicators as a surrogate for plasma potassium levels in hemodialysis patients—a proof-of-concept study.

Author

Deak, Andras T, Belić, Katarina, Meissl, Anna-Maria, Artinger, Katharina, Eller, Kathrin, Rechberger, Bernd, Niedrist, Tobias, Graier, Wolfgang F, Malli, Roland, Bischof, Helmut, Burgstaller, Sandra, Blass, Sandra, Avian, Alexander, Rosenkranz, Alexander R, and Kirsch, Alexander H

Subjects
HEMODIALYSIS patients, POTASSIUM ions, POTASSIUM, HYPERKALEMIA, SALIVA
Abstract

Background Hyperkalemia is a common complication in cardiorenal patients treated with agents interfering with renal potassium (K+) excretion. It frequently leads to discontinuation of potentially life-saving medication, which has increased the importance of K+ monitoring. Non-invasive means to detect hyperkalemia are currently unavailable, but would be of potential use for therapy guidance. The aim of the present study was to assess the analytical performance of genetically encoded potassium-ion indicators (GEPIIs) in measuring salivary [K+] ([K+]Saliva) and to determine whether changes of [K+]Saliva depict those of [K+]Plasma. Methods We conducted this proof-of-concept study: saliva samples from 20 healthy volunteers as well as plasma and saliva from 29 patients on hemodialysis (HD) before and after three consecutive HD treatments were collected. We compared [K+]Saliva as assessed by the gold standard ion-selective electrode (ISE) with GEPII measurements. Results The Bland–Altmann analysis showed a strong agreement (bias 0.71; 95% limits of agreement from –2.79 to 4.40) between GEPII and ISE. Before treatment, patients on HD showed significantly higher [K+]Saliva compared with healthy controls [median 37.7 (30.85; 48.46) vs 23.8 (21.63; 25.23) mmol/L; P  < .05]. [K+]Plasma in HD patients decreased significantly after dialysis. This was paralleled by a significant decrease in [K+]Saliva, and both parameters increased until the subsequent HD session. Despite similar kinetics, we found weak or no correlation between [K+]Plasma and [K+]Saliva. Conclusion GEPIIs have shown an excellent performance in determining [K+]Saliva. [K+]Plasma and [K+]Saliva exhibited similar kinetics. To determine whether saliva could be a suitable sample type to monitor [K+]Plasma, further testing in future studies are required. [ABSTRACT FROM AUTHOR]

Published
2023
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18. PATHOLOGY INFLAMMATION

Author

Rho, Elena, Artinger, Katharina, Kirsch, Alexander H., Schaubettl, Corinna, Aringer, Ida, Rosenkranz, Alexander R., Eller, Philipp, and Eller, Kathrin

Published
2014

19. PATHOLOGY INFLAMMATION

Author

Kirsch, Alexander H., Artinger, Katharina, Rho, Elena, Wolf, Anna M, Cornez, Isabelle, Eller, Philipp, Wolf, Dominik, Rosenkranz, Alexander R, and Eller, Kathrin

Published
2014

20. Low-Dose rIL-15 Protects from Nephrotoxic Serum Nephritis via CD8 + T Cells.

Author

Mooslechner, Agnes A., Schuller, Max, Artinger, Katharina, Kirsch, Alexander H., Schabhüttl, Corinna, Eller, Philipp, Rosenkranz, Alexander R., and Eller, Kathrin

Subjects
KNOCKOUT mice, NEPHRITIS, MYELOID cells, RENAL replacement therapy, CHRONIC kidney failure
Abstract

Rapid progressive glomerulonephritis (GN) often leads to end-stage kidney disease, driving the need for renal replacement therapy and posing a global health burden. Low-dose cytokine-based immunotherapies provide a new strategy to treat GN. IL-15 is a strong candidate for the therapy of immune-mediated kidney disease since it has proven to be tubular-protective before. Therefore, we set out to test the potential of low-dose rIL-15 treatment in a mouse model of nephrotoxic serum nephritis (NTS), mimicking immune complex-driven GN in humans. A single low-dose treatment with rIL-15 ameliorated NTS, reflected by reduced albuminuria, less tissue scarring, fewer myeloid cells in the kidney, and improved tubular epithelial cell survival. In addition, CD8+ T cells, a primary target of IL-15, showed altered gene expression and function corresponding with less cytotoxicity mediated by rIL-15. With the use of transgenic knock-out mice, antibody depletion, and adoptive cell transfer studies, we here show that the beneficial effects of rIL-15 treatment in NTS depended on CD8+ T cells, suggesting a pivotal role for them in the underlying mechanism. Our findings add to existing evidence of the association of IL-15 with kidney health and imply a potential for low-dose rIL-15 immunotherapies in GN. [ABSTRACT FROM AUTHOR]

Published
2022
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21. Alterations in the Kynurenine–Tryptophan Pathway and Lipid Dysregulation Are Preserved Features of COVID-19 in Hemodialysis.

Author

Schuller, Max, Oberhuber, Monika, Prietl, Barbara, Zügner, Elmar, Prugger, Eva-Maria, Magnes, Christoph, Kirsch, Alexander H., Schmaldienst, Sabine, Pieber, Thomas, Brodmann, Marianne, Rosenkranz, Alexander R., Eller, Philipp, and Eller, Kathrin

Subjects
COVID-19, CHRONIC kidney failure, BLOOD lipids, FREE fatty acids, PROGNOSIS
Abstract

Coronavirus disease 2019 (COVID-19)-induced metabolic alterations have been proposed as a source for prognostic biomarkers and may harbor potential for therapeutic exploitation. However, the metabolic impact of COVID-19 in hemodialysis (HD), a setting of profound a priori alterations, remains unstudied. To evaluate potential COVID-19 biomarkers in end-stage kidney disease (CKD G5), we analyzed the plasma metabolites in different COVID-19 stages in patients with or without HD. We recruited 18 and 9 asymptomatic and mild, 11 and 11 moderate, 2 and 13 severely affected, and 10 and 6 uninfected HD and non-HD patients, respectively. Plasma samples were taken at the time of diagnosis and/or upon admission to the hospital and analyzed by targeted metabolomics and cytokine/chemokine profiling. Targeted metabolomics confirmed stage-dependent alterations of the metabolome in non-HD patients with COVID-19, which were less pronounced in HD patients. Elevated kynurenine levels and lipid dysregulation, shown by an increase in circulating free fatty acids and a decrease in lysophospholipids, could distinguish patients with moderate COVID-19 from non-infected individuals in both groups. Kynurenine and lipid alterations were also associated with ICAM-1 and IL-15 levels in HD and non-HD patients. Our findings support the kynurenine pathway and plasma lipids as universal biomarkers of moderate and severe COVID-19 independent of kidney function. [ABSTRACT FROM AUTHOR]

Published
2022
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24. Chronic Inflammation Might Protect Hemodialysis Patients From Severe COVID-19.

Author

Prietl, Barbara, Odler, Balazs, Kirsch, Alexander H., Artinger, Katharina, Eigner, Manfred, Schmaldienst, Sabine, Pfeifer, Verena, Stanzer, Stefanie, Eberl, Anita, Raml, Reingard, Pieber, Thomas, Rosenkranz, Alexander R., Brodmann, Marianne, Eller, Philipp, and Eller, Kathrin

Subjects
HEMODIALYSIS patients, REGULATORY T cells, CORONAVIRUS diseases, COVID-19, IMMUNOLOGIC memory, T cells
Abstract

Hemodialysis patients (HD) are expected to have excess mortality in coronavirus disease 2019 (COVID-19). This was challenged by a recent study reporting HD patients to have comparable mortality and less ICU admissions when hospitalized with COVID-19. An altered immune system due to chronic inflammation might protect HD-patients from severe COVID-19. Therefore, we aimed to describe the peripheral blood immune phenotype in HD-patients and respective controls with COVID-19. Methods: Sixty-four patients (31 HD, 33 non-HD) with PCR-confirmed COVID-19 and 16 control patients (10 HD, 6 non-HD) were prospectively included. According to symptoms, COVID-19 patients were categorized as asymptomatic/mild, moderate or severe COVID-19 phenotypes. Cytokine profiling and immune phenotyping was performed. Results: Th1 and Th17 plasma cytokine levels were highly increased in HD patients without COVID-19 and were not significantly regulated during COVID-19. In non-HD COVID-19 patients these cytokines increased significantly with disease severity. While all patients with moderate or severe COVID-19 showed hallmarks of COVID-19 such as decreased CD3+, CD4+ and CD8+ and CD4+CD25hiFoxP3+ regulatory T cells, significantly increased CD38+CD8+ effector memory and CD38+CD8+ TEMRA T cells were detected in moderate/severe COVID-19 HD patients, which was not observed in non-HD patients with moderate or severe COVID-19. Furthermore, CD161+CD8+ T cells decreased significantly in non-HD COVID-19 patients dependent on disease severity, but not in HD patients. Dynamics of B cells and subtypes were comparable in HD and non-HD COVID-19 patients. Conclusions: HD patients might be protected from severe COVID-19 due to their chronic inflammatory state with increased CD38+CD8+ effector memory and TEMRA T cells as well as CD161+CD8+ T cells. [ABSTRACT FROM AUTHOR]

Published
2022
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25. At least 156 reasons to prioritize COVID-19 vaccination in patients receiving in-centre haemodialysis.

Author

Combe, Christian, Kirsch, Alexander H, Alfano, Gaetano, Luyckx, Valerie A, Shroff, Rukshana, Kanbay, Mehmet, van der Sande, Frank, Basile, Carlo, and ERA-EDTA, the EUDIAL Working Group of the

Subjects
*COVID-19 vaccines, *IMMUNIZATION of children, *HOME hemodialysis, *MEDICAL personnel, *COVID-19, *HEMODIALYSIS, *CLINICAL trials monitoring
Abstract

Patients receiving dialysis athome, whether peritonealdialysis or HD, have similar intrinsic risk, and are only less vulnerable than patients on ICHD because they do not travel frequently for care. The second question about prioritization of patients on ICHD for vaccination over other patient groups is more complex. In conclusion, it is clear that patients receiving ICHD are highly vulnerable to infection, severe disease and death from COVID-19, and are likely to respond to vaccination. [Extracted from the article]

Published
2021
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26. Decreased response to the mRNA anti-SARS-CoV-2 vaccine in hepatitis B vaccine non-responders and frail patients treated with peritoneal dialysis.

Author

Kolland, Michael, Riedl, Regina, Bachler, Bernhard, Ribitsch, Werner, Niedrist, Tobias, Meissl, Anna-Maria, Rosenkranz, Alexander R, and Kirsch, Alexander H

Subjects
HEPATITIS B, HEPATITIS B vaccines, PERITONEAL dialysis, SARS-CoV-2, HOME hemodialysis
Abstract

In a recent study on the response to COVID-19 vaccination in dialysis patients, there was a superior humoral response in patients treated with PD compared with HD [[7]]. Thus, while routine SARS-CoV-2 serology is as of yet not recommended after vaccination, the knowledge of which patients are more prone to show an insufficient response to the SARS-CoV-2 vaccination is likely to be clinically relevant. [Extracted from the article]

Published
2022
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27. Impact of cardiovascular risk stratification strategies in kidney transplantation over time.

Author

Deak, Andras T, Ionita, Francesca, Kirsch, Alexander H, Odler, Balazs, Rainer, Peter P, Kramar, Reinhard, Kubatzki, Michael P, Eberhard, Katharina, Berghold, Andrea, and Rosenkranz, Alexander R

Subjects
KIDNEY transplantation, CORONARY angiography, CORONARY disease, PEOPLE with diabetes, COMPUTED tomography
Abstract

Background Kidney transplant recipients exhibit a dramatically increased cardiovascular (CV) risk. In 2007, Austrian centres implemented a consensus of comprehensive CV screening programme prior to kidney transplantation (KT). The consensus placed a particular emphasis on screening for coronary artery disease (CAD) with cardiac computed tomography (CT) or coronary angiography (CAG) in patients with diabetes mellitus, known CAD or those having multiple conventional CV risk factors. Here, we investigate if this affected risk stratification and post-transplant CV outcomes. Methods In a retrospective chart review, we evaluated 551 KTs performed from 2003 to 2015 in our centre. Patients were categorized into three groups: KT before (2003–07), directly after (2008–11) and 5 years after (2012–15) implementation of the consensus. We analysed clinical characteristics, the rate of cardiac CTs and CAGs prior to KT as well as major adverse cardiac events (MACEs) during a 2-year follow-up after KT. Results The three study groups showed a homogeneous distribution of comorbidities and age. Significantly more cardiac CTs (13.6% versus 10.2% versus 44.8%; P = 0.002) and CAGs (39.6% versus 43.9% versus 56.2%; P = 0.003) were performed after the consensus. Coronary interventions were performed during 42 out of 260 CAGs (16.2%), the cumulative 2-year MACE incidence was 8.7%. Regarding MACE occurrence, no significant difference between the three groups was found. Conclusion CV risk stratification has become more rigorous and invasive after the implementation of the consensus; however, this was not associated with an improvement in CV outcome. [ABSTRACT FROM AUTHOR]

Published
2020
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28. Intradialytic kinetics of middle molecules during hemodialysis and hemodiafiltration.

Author

Leypoldt, John K, Storr, Markus, Agar, Baris U, Boschetti-de-Fierro, Adriana, Bernardo, Angelito A, Kirsch, Alexander H, Rosenkranz, Alexander R, Krieter, Detlef H, and Krause, Bernd

Subjects
HEMODIAFILTRATION, BLOOD volume, EXTRACELLULAR fluid, MYOGLOBIN, MOLECULAR weights
Abstract

Background The kinetics of β2-microglobulin during hemodialysis and hemodiafiltration is well described by a two-compartment model where clearance by the dialyzer is from a central compartment volume that approximates plasma volume and a total distribution volume that approximates extracellular fluid volume. The kinetics of middle molecules with molecular weights larger than β2-microglobulin have not been extensively studied. Methods Intradialytic plasma concentrations and overall dialyzer clearances of β2-microglobulin (11.8 kD), myoglobin (16.7 kD) and complement factor D (24.4 kD) were used to estimate three kinetic parameters from a two-compartment model, namely intercompartmental clearance, central compartment volume and total distribution volume, in hemodialysis patients; these data were collected during two clinical trials of medium cut-off dialyzers (with extended middle molecule removal) during hemodialysis and high-flux dialyzers during hemodialysis and hemodiafiltration. In the current exploratory analyses, the kinetic parameters from all dialyzers were combined. Overall dialyzer clearance was evaluated by total mass removed in the dialysate. Results In total, 345 sets of kinetic parameters from 35 patients were determined. Intercompartmental clearance and central compartment volume for myoglobin and complement factor D were smaller (P < 0.001) than those for β2-microglobulin. Independent of middle molecule, intercompartmental clearance and central compartment volume were associated with overall dialyzer clearance (P < 0.001), but total distribution volume was not (P = 0.083). Conclusions A two-compartment kinetic model can only describe intradialytic kinetics of middle molecules with molecular weights larger than β2-microglobulin if the central compartment is small and dependent on overall dialyzer clearance. [ABSTRACT FROM AUTHOR]

Published
2019
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29. Blockade of prostaglandin E2 receptor 4 ameliorates nephrotoxic serum nephritis.

Author

Aringer, Ida, Artinger, Katharina, Kirsch, Alexander H., Schabhüttl, Corinna, Jandl, Katharina, Bärnthaler, Thomas, Mooslechner, Agnes A., Herzog, Sereina A., Uhlig, Moritz, Kirsch, Andrijana, Frank, Saša, Banas, Miriam, Pollheimer, Marion, Eller, Philipp, Rosenkranz, Alexander R., Heinemann, Akos, and Eller, Kathrin

Abstract

Prostaglandin E2 (PGE2) signaling is known to modulate inflammation and vascular resistance. Receptors of PGE2 [E-type prostanoid receptors (EP)] might be an attractive pharmacological target in immune-mediated diseases such as glomerulonephritis. We hypothesized that selective EP4 antagonism improves nephrotoxic serum nephritis (NTS) by its anti-inflammatory properties. Mice were subjected to NTS and treated with the EP4 antagonist ONO AE3-208 (10 mg·kg body wt-1·day-1] or vehicle starting from disease initiation. In one set of experiments, treatment was started 4 days after NTS induction. Tubular epithelial cells were evaluated in vitro under starving conditions. EP4 antagonist treatment significantly improved the NTS phenotype without affecting blood pressure levels. Remarkably, the improved NTS phenotype was also observed when treatment was started 4 days after NTS induction. EP4 antagonism decreased tubular chemokine (C-X-C motif) ligand ( Cxcl) 1 and Cxcl-5 expression and thereby subsequently reduced interstitial neutrophil infiltration into the kidney. In vitro, tubular epithelial cells increasingly expressed Cxcl-5 mRNA and Cxcl-5 protein when treated with PGE2 or an EP4 agonist under starving conditions, which was blunted by EP4 antagonist treatment. Together, EP4 antagonism improves the NTS phenotype, probably by decreasing mainly Cxcl-5 production in tubular cells, thereby reducing renal neutrophil infiltration. [ABSTRACT FROM AUTHOR]

Published
2018
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30. Autophagy Protects From Uremic Vascular Media Calcification.

Author

Frauscher, Bianca, Kirsch, Alexander H., Schabhüttl, Corinna, Schweighofer, Kerstin, Kétszeri, Máté, Pollheimer, Marion, Dragun, Duska, Schröder, Katrin, Rosenkranz, Alexander R., Eller, Kathrin, and Eller, Philipp

Subjects
AUTOPHAGY, TREATMENT of chronic kidney failure, RAPAMYCIN
Abstract

Chronic kidney disease and diabetes mellitus are associated with extensive media calcification, which leads to increased cardiovascular morbidity and mortality. Here, we investigated the role of autophagy in the pathogenesis of uremic vascular media calcification. DBA/2 mice were fed with high-phosphate diet (HPD) in order to cause vascular calcification. DBA/2 mice on standard chow diet were used as control. In parallel, autophagy and its response to rapamycin, 3-methyladenine (3-MA), and bafilomycin were studied in an in vitro model using mouse vascular smooth muscle cells (MOVAS). DBA/2 mice on HPD developed severe vascular media calcification, which is mirrored in vitro by culturing MOVAS under calcifying conditions. Both, in vitro and in vivo, autophagy significantly increased in MOVAS under calcifying conditions and in aortas of HPD mice, respectively. Histologically, autophagy was located to the aortic Tunica media, but also vascular endothelial cells, and was found to continuously increase during HPD treatment. 3-MA as well as bafilomycin blocked autophagy in MOVAS and increased calcification. Vice versa, rapamycin treatment further increased autophagy and resulted in a significant decrease of vascular calcification in vitro and in vivo. Rapamycin reduced Runx2 transcription levels in aortas and MOVAS to control levels, whereas it increased a-smooth muscle actin and Sm22a transcription in MOVAS to control levels. Furthermore, rapamycin-treated HPD mice survived significantly longer compared to HPD controls. These findings indicate that autophagy is an endogenous response of vascular smooth muscle cells (VSMC) to protect from calcification in uremia. Induction of autophagy by rapamycin protects cells and mice from uremic media calcification possibly by inhibiting osteogenic transdifferentiation of VSMC. [ABSTRACT FROM AUTHOR]

Published
2018
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31. A New Murine Model of Chronic Kidney Disease-Mineral and Bone Disorder.

Author

Frauscher, Bianca, Artinger, Katharina, Kirsch, Alexander H., Aringer, Ida, Moschovaki-Filippidou, Foteini, Kétszeri, Máté, Schabhüttl, Corinna, Rainer, Peter P., Schmidt, Albrecht, Stojakovic, Tatjana, Fahrleitner-Pammer, Astrid, Rosenkranz, Alexander R., Eller, Philipp, and Eller, Kathrin

Subjects
CHRONIC kidney failure, CARDIOVASCULAR disease related mortality, BONE diseases, GLOMERULAR filtration rate, LABORATORY mice
Abstract

Chronic kidney disease (CKD) is associated with mineral and bone disorder (MBD), which is the main cause of the extensively increased cardiovascular mortality in the CKD population. We now aimed to establish a new murine experimental CKD-MBD model. Dilute brown non-Agouti (DBA/2) mice were fed with high-phosphate diet for 4 (HPD4) or 7 (HPD7) days, then with standard chow diet (SCD) and subsequently followed until day 84. They were compared to DBA/2 mice maintained on SCD during the whole study period. Both 4 and 7 days HPD-fed mice developed phosphate nephropathy with tubular atrophy, interstitial fibrosis, decreased glomerular filtration rate, and increased serum urea levels. The abdominal aorta of HPD-treated mice showed signs of media calcification. Histomorphometric analysis of HPD-treated mice showed decreased bone volume/tissue volume, low mineral apposition rate, and low bone formation rate as compared to SCD-fed mice, despite increased parathyroid hormone levels. Overall, the observed phenotype was more pronounced in the HPD7 group. In summary, we established a new, noninvasive, and therefore easy to perform reproducible CKD-MBD model, which showed media calcification, secondary hyperparathyroidism, and low-turnover bone disease. [ABSTRACT FROM AUTHOR]

Published
2017
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33. A patient with predominant interstitial nephritis as a renal manifestation of systemic lupus erythematosus.

Author

Odler, Balazs, Pollheimer, Marion J, Kirsch, Alexander H, Moazedi-Fuerst, Florentine, Rosenkranz, Alexander R, and Eller, Kathrin

Subjects
PROTEINURIA diagnosis, ADRENOCORTICAL hormones, BIOPSY, CREATININE, IMMUNOHISTOCHEMISTRY, KIDNEY diseases, INTERSTITIAL nephritis, PHOTOMETRY, SERODIAGNOSIS, SYSTEMIC lupus erythematosus, DISEASE complications, DISEASE risk factors, SYMPTOMS
Abstract

The article reports an exceptional case of lupus nephritis (LN) with predominant tubulointerstitial nephritis (TIN) without clinical features of classic LN that was successfully treated with a combination of high-dose corticosteroids, cyclophosphamide (CYC) and mycophenolate mofetil (MMF). Topics discussed include clinical guidelines for LN, finding on the kidney biopsy of the patient, and result of the immunohistochemical analysis of the tubulointerstitial inflammatory infiltrates.

Published
2020
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34. Manufacturing of a Secretoneurin Drug Delivery System with Self-Assembled Protamine Nanoparticles by Titration.

Author

Scheicher, Bernhard, Lorenzer, Cornelia, Gegenbauer, Katrin, Partlic, Julia, Andreae, Fritz, Kirsch, Alexander H., Rosenkranz, Alexander R., Werzer, Oliver, and Zimmer, Andreas

Subjects
PROTAMINES, DRUG delivery systems, DRUG factories, NANOMEDICINE, MOLECULAR self-assembly, VOLUMETRIC analysis, THERAPEUTICS
Abstract

Since therapeutic peptides and oligonucleotides are gathering interests as active pharmaceutical ingredients (APIs), nanoparticulate drug delivery systems are becoming of great importance. Thereby, the possibility to design drug delivery systems according to the therapeutic needs of APIs enhances clinical implementation. Over the last years, the focus of our group was laid on protamine-oligonucleotide-nanoparticles (so called proticles), however, the possibility to modify the size, zeta potential or loading efficiencies was limited. Therefore, at the present study we integrated a stepwise addition of protamine (titration) into the formation process of proticles loaded with the angiogenic neuropeptide secretoneurin (SN). A particle size around 130 nm was determined when proticles were assembled by the commonly used protamine addition at once. Through application of the protamine titration process it was possible to modify and adjust the particle size between approx. 120 and 1200 nm (dependent on mass ratio) without influencing the SN loading capacity. Dynamic light scattering pointed out that the difference in particle size was most probably the result of a secondary aggregation. Initially-formed particles of early stages in the titration process aggregated towards bigger assemblies. Atomic-force-microscopy images also revealed differences in morphology along with different particle size. In contrast, the SN loading was only influenced by the applied mass ratio, where a slight saturation effect was observable. Up to 65% of deployed SN could be imbedded into the proticle matrix. An in-vivo biodistribution study (i.m.) showed a retarded distribution of SN from the site of injection after the application of a SN-proticle formulation. Further, it was demonstrated that SN loaded proticles can be successfully freeze-dried and resuspended afterwards. To conclude, the integration of the protamine titration process offers new possibilities for the formulation of proticles in order to address key parameters of drug delivery systems as size, API loading or modified drug release. [ABSTRACT FROM AUTHOR]

Published
2016
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35. The Spleen Plays No Role in Nephrotoxic Serum Nephritis, but Constitutes a Place of Compensatory Haematopoiesis.

Author

Artinger, Katharina, Kirsch, Alexander H., Aringer, Ida, Schabhüttl, Corinna, Rosenkranz, Alexander R., Eller, Philipp, Rho, Elena, and Eller, Kathrin

Subjects
*SPLEEN physiology, *NEPHROTOXICOLOGY, *BLOOD serum analysis, *NEPHRITIS, *HEMATOPOIESIS, *IMMUNE response, *DIAGNOSIS
Abstract

Background: The spleen has been implicated in the pathogenesis of immune-complex glomerulonephritis by initiating and resolving adaptive immune responses. Thus, we aimed to evaluate the role of the spleen in experimental nephrotoxic serum nephritis (NTS). Methods: In order to accelerate the disease, animals were subjected to NTS by preimmunizing male C57BL/6J mice with rabbit IgG three days before injecting the rabbit anti-glomerular basement antiserum, or were immunized only. A group underwent splenectomy before NTS induction. Results: We observed enlargement of the spleen with a maximum at 14 days after NTS induction or immunization only. Splenectomized mice were found to develop albuminuria and renal histological changes comparable to sham-operated controls. Nevertheless, anaemia was aggravated in mice after splenectomy. During the course of NTS, we detected CD41+ megakaryocytes and Ter119+ erythroid precursor cells in the spleen of mice with NTS and of immunized mice. Ter119+Cxcr4+ cells and the binding partner Cxcl12 increased in the spleen, and decreased in the bone marrow. This was accompanied by a significant systemic increase of interferon-gamma in the serum. Conclusions: In summary, splenectomy does not influence the course of NTS per se, but is involved in concomitant anaemia. Extramedullary haematopoiesis in the spleen is probably facilitated through the migration of Cxcr4+ erythroid precursor cells from the bone marrow to the spleen via a Cxcl12 gradient and likely arises from the suppressive capacity of chronic inflammation on the bone marrow. [ABSTRACT FROM AUTHOR]

Published
2015
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37. Lipocalin-2 Expressed in Innate Immune Cells Is an Endogenous Inhibitor of Inflammation in Murine Nephrotoxic Serum Nephritis.

Author

Eller, Kathrin, Schroll, Andrea, Banas, Miriam, Kirsch, Alexander H., Huber, Julia M., Nairz, Manfred, Skvortsov, Sergej, Weiss, Günter, Rosenkranz, Alexander R., and Theurl, Igor

Subjects
LIPOCALIN-2, GENE expression, ACUTE kidney failure, IMMUNOLOGY, CYTOKINES, IMMUNE response, NEPHROLOGY, LABORATORY mice
Abstract

Lipocalin-2 (Lcn-2) is involved in divergent processes such as acute kidney injury or bacterial host defence. Our study was designed to evaluate the functional role of Lcn-2 in nephrotoxic serum nephritis (NTS). Since Lcn-2 is expressed in tubular epithelial cells as well as in cells of innate immunity such as macrophages and polymorphonuclear neutrophils (PMN), we induced NTS in wild-type (WT), Lcn-2 knock-out (KO) mice and WT/Lcn-2 KO chimeras. Mice lacking Lcn-2 exhibited more glomerular damage with increased proteinuria and interstitial leukocyte accumulation compared to WT mice. Chimeras able to express Lcn-2 in macrophages and PMN but not in epithelial cells were found to develop NTS comparable to wild-type controls. In contrast, chimeras expressing Lcn-2 in tubular epithelial cells with no expression in innate immune cells developed increased NTS due to decreased concerted apoptosis but increased necrosis and formation of damage-associated molecular patterns (DAMPs) such as high-mobility group box 1 (HMGB-1) in the kidney. In vivo blockade of HMGB-1, a toll-like receptor (TLR)-2 agonist, significantly reduced inflammation and NTS in Lcn-2 knock-out mice. In parallel, TLR-2 signalling was found to drive Lcn-2 transcription in vitro. Taken together, Lcn-2 expressed in innate immune cells is protective in NTS by inducing concerted apoptosis and inhibiting the formation of HMGB-1 thereby limiting cytokine production via TLR-2 signalling. In parallel, TLR-2 dependent transcription of Lcn-2 is an endogenous inhibitor of inflammation in NTS. [ABSTRACT FROM AUTHOR]

Published
2013
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