Your search keyword '"Hilgers, Karl F."' showing total 9 results

1. Spot urinary sodium in CKD patients: correlation with 24h-excretion and evaluation of commonly used prediction equations

Author

Kurzhagen, Johanna T., Titze, Stephanie, Büschges-Seraphin, Beatrix, Schiffer, Mario, Schneider, Markus P., Eckardt, Kai-Uwe, and Hilgers, Karl F.

Published

2024

2. Sex differences in the development of vascular and renal lesions in mice with a simultaneous deficiency of Apoe and the integrin chain Itga8.

Author

Marek, Ines, Canu, Maurizio, Cordasic, Nada, Rauh, Manfred, Volkert, Gudrun, Fahlbusch, Fabian B., Rascher, Wolfgang, Hilgers, Karl F., Hartner, Andrea, and Menendez-Castro, Carlos

Subjects

ATHEROSCLEROSIS, KIDNEY injuries

Abstract

Background: Apoe-deficient (Apoe-/-) mice develop progressive atherosclerotic lesions with age but no severe renal pathology in the absence of additional challenges. We recently described accelerated atherosclerosis as well as marked renal injury in Apoe-/- mice deficient in the mesenchymal integrin chain Itga8 (Itga8-/-). Here, we used this Apoe-/-, Itga8-/- mouse model to investigate the sex differences in the development of atherosclerosis and concomitant renal injury. We hypothesized that aging female mice are protected from vascular and renal damage in this mouse model. Methods: Apoe-/- mice were backcrossed with Itga8-/- mice. Mice were kept on a normal diet. At the age of 12 months, the aortae and kidneys of male and female Apoe-/- Itga8+/+ mice or Apoe-/- Itga8-/- mice were studied. En face preparations of the aorta were stained with Sudan IV (lipid deposition) or von Kossa (calcification). In kidney tissue, immunostaining for collagen IV, CD3, F4/80, and PCNA and real-time PCR analyses for Il6, Vegfa, Col1a1 (collagen I), and Ssp1 (secreted phosphoprotein 1, synonym osteopontin) as well as ER stress markers were performed. Results: When compared to male mice, Apoe-/- Itga8+/+ female mice had a lower body weight, equal serum cholesterol levels, and lower triglyceride levels. However, female mice had increased aortic lipid deposition and more aortic calcifications than males. Male Apoe-/- mice with the additional deficiency of Itga8 developed increased serum urea, glomerulosclerosis, renal immune cell infiltration, and reduced glomerular cell proliferation. In females of the same genotype, these renal changes were less pronounced and were accompanied by lower expression of interleukin-6 and collagen I, while osteopontin expression was higher and markers of ER stress were not different. Conclusions: In this model of atherosclerosis, the female sex is a risk factor to develop more severe atherosclerotic lesions, even though serum fat levels are higher in males. In contrast, female mice are protected from renal damage, which is accompanied by attenuated inflammation and matrix deposition. Thus, sex affects vascular and renal injury in a differential manner. [ABSTRACT FROM AUTHOR]

Published

2017

3. BK viremia and polyomavirus nephropathy in 352 kidney transplants; risk factors and potential role of mTOR inhibition.

Author

Jacobi, Johannes, Prignitz, Antonina, Büttner, Maike, Korn, Klaus, Weidemann, Alexander, Hilgers, Karl F., Heller, Katharina, Velden, Joachim, Knöll, Antje, Wullich, Bernd, May, Christoph, Eckardt, Kai-Uwe, and Amann, Kerstin U.

Subjects

IMMUNODEFICIENCY, IMMUNOREGULATION, IMMUNOSUPPRESSION, KIDNEY diseases, CYCLOSPORINE

Abstract

Background: Polyomavirus BK nephropathy (PyVAN) remains an important cause of early graft dysfunction and graft loss in kidney transplantation. Methods: In this retrospective, single centre cohort study we studied the incidence and outcome of BK viral infection in 352 patients transplanted in 2008-2011. Results: During follow-up viral replication was detected in 48 patients (13.6%); 22 patients (6.2%) had biopsy proven PyVAN. In multivariate logistic regression analyses risk factors for BK-viremia were lack of enrolment into randomized controlled trials (RCTs), biopsy proven acute rejections, cytomegaly virus (CMV) serostatus of both donor and recipient and previous transplantation. In patients without PyVAN reduction or switch of immunosuppression was associated with rapid viral clearance and stable graft function. In contrast, in most patients with PyVAN graft function deteriorated and 5 patients prematurely lost their allograft. Switch of immunosuppression to a low dose cyclosporine plus mTOR inhibitor based regimen in patients with PyVAN was safe, well tolerated and tended to be associated with a better short-term outcome in terms of graft function compared to reduction of existing immunosuppression alone. Conclusions: With the lack of licensed anti-polyoma viral drugs reduction or conversion of immunosuppression remains the mainstay of therapy in patients with PyVAN. The combination of low dose cyclosporine plus mTOR inhibition appears to be safe and warrants further investigation. [ABSTRACT FROM AUTHOR]

Published

2013

4. A complex microdeletion 17q12 phenotype in a patient with recurrent de novo membranous nephropathy.

Author

Hinkes, Bernward, Hilgers, Karl F., Bolz, Hanno J., Goppelt-Struebe, Margarete, Amann, Kerstin, Nagl, Sandra, Bergmann, Carsten, Rascher, Wolfgang, Eckardt, Kai-Uwe, and Jacobi, Johannes

Subjects

DELETION mutation, MAYER-Rokitansky-Kuster-Hauser syndrome, CHROMOSOMES, KIDNEY diseases, PHENOTYPES

Abstract

Background: Microdeletions on chromosome 17q12 cause of diverse spectrum of disorders and have only recently been identified as a rare cause of Mayer-Rokitansky-Kuester-Hauser-Syndrome (MRKH), which is characterized by uterus aplasia ± partial/complete vaginal aplasia in females with a regular karyotype. For the first time we report about a patient with a 17q12 microdeletion who is affected by MRKH in combination with a vascular and soft tissue disorder. Repeatedly she suffered from kidney transplant failure caused by consuming membranous nephropathy. Case presentation: A 38-year-old female patient had been diagnosed with right kidney aplasia, left kidney dysplasia and significantly impaired renal function during infancy. Aged 16 she had to start hemodialysis. Three years later she received her first kidney transplant. Only then she was diagnosed with MRKH. The kidney transplant was lost due to consuming nephrotic syndrome caused by de novo membranous nephropathy, as was a second kidney transplant years later. In addition, a hyperelasticity syndrome affects the patient with congenital joint laxity, kyphoscoliosis, bilateral hip dysplasia, persistent hypermobility of both elbows, knees and hips. Her clinical picture resembles a combination of traits of a hypermobile and a vascular form of Ehlers-Danlos-Syndrome, but no mutations in the COL3A1 gene was underlying. Instead, array-based comparative genomic hybridisation (CGH) detected a heterozygous 1.43 Mb deletion on chromosome 17q12 encompassing the two renal developmental genes HNF1β and LHX1. Conclusions: Deletions of HNF1β have recently drawn significant attention in pediatric nephrology as an important cause of prenatally hyperechogenic kidneys, renal aplasia and renal hypodysplasia. In contrast, membranous nephropathy represents an often-unaccounted cause of nephrotic syndrome in the adult population. A causative connection between theses two conditions has never been postulated, but is suggestive enough in this case to hypothesize it. [ABSTRACT FROM AUTHOR]

Published

2012

5. Severe metabolic alkalosis and recurrent acute on Chronic kidney injury in a patient with Crohn's disease.

Author

Jacobi, Johannes, Schnellhardt, Susanne, Opgenoorth, Mirian, Amann, Kerstin U., Küttner, Axel, Schmid, Axel, Eckardt, Kai-Uwe, and Hilgers, Karl F.

Subjects

ALKALOSIS, CHRONIC kidney failure, CROHN'S disease, ACIDOSIS, HOMEOSTASIS, PATIENTS

Abstract

Background: Diarrhea is common in patients with Crohn's disease and may be accompanied by acid base disorders, most commonly metabolic acidosis due to intestinal loss of bicarbonate. Case Presentation: Here, we present a case of severe metabolic alkalosis in a young patient suffering from M. Crohn. The patient had undergone multiple resections of the intestine and suffered from chronic kidney disease. He was now referred to our clinic for recurrent acute kidney injury, the nature of which was pre-renal due to profound volume depletion. Renal failure was associated with marked hypochloremic metabolic alkalosis which only responded to high volume repletion and high dose blockade of gastric hypersecretion. Intestinal failure with stomal fluid losses of up to 5.7 litres per day required port implantation to commence parenteral nutrition. Fluid and electrolyte replacement rapidly improved renal function and acid base homeostasis. Conclusions: This case highlights the important role of gastrointestinal function to maintain acid base status in patients with Crohn's disease. [ABSTRACT FROM AUTHOR]

Published

2010

6. Lack of a8 integrin leads to morphological changes in renal mesangial cells, but not in vascular smooth muscle cells.

Author

Marek, Ines, Volkert, Gudrun, Jahn, Angelika, Fahlbusch, Fabian, Zürn, Christina, Özcan, Zehra, Goppelt-Struebe, Margarete, Hilgers, Karl F., Rascher, Wolfgang, and Hartner, Andrea

Subjects

SMOOTH muscle, MUSCLE cells, RENAL artery, INTEGRINS, MICE

Abstract

Background: Extracellular matrix receptors of the integrin family are known to regulate cell adhesion, shape and functions. The α8 integrin chain is expressed in glomerular mesangial cells and in vascular smooth muscle cells. Mice deficient for α8 integrin have structural alterations in glomeruli but not in renal arteries. For this reason we hypothesized that mesangial cells and vascular smooth muscle cells differ in their respective capacity to compensate for the lack of α8 integrin. Results: Wild type and α8 integrin-deficient mesangial cells varied markedly in cell morphology and expression or localization of cytoskeletal molecules. In α8 integrin-deficient mesangial cells α-smooth muscle actin and CTGF were downregulated. In contrast, there were no comparable differences between α8 integrin-deficient and wild type vascular smooth muscle cells. Expression patterns of integrins were altered in α8 integrin-deficient mesangial cells compared to wild type mesangial cells, displaying a prominent overexpression of α2 and α6 integrins, while expression patterns of the these integrins were not different between wild type and α8 integrin-deficient vascular smooth muscle cells, respectively. Cell proliferation was augmented in α8 integrin-deficient mesangial cells, but not in vascular smooth muscle cells, compared to wild type cells. Conclusions: Our findings suggest that α8 integrin deficiency has differential effects in mesangial cells and vascular smooth muscle cells. While the phenotype of vascular smooth muscle cells lacking α8 integrin is not altered, mesangial cells lacking α8 integrin differ considerably from wild type mesangial cells which might be a consequence of compensatory changes in the expression patterns of other integrins. This could result in glomerular changes in α8 integrin-deficient mice, while the vasculature is not affected in these mice. [ABSTRACT FROM AUTHOR]

Published

2010

7. Effects of diabetes and hypertension on macrophage infiltration and matrix expansion in the rat kidney.

Author

Hartner, Andrea, Veelken, Roland, Wittmann, Michael, Cordasic, Nada, and Hilgers, Karl F.

Subjects

DIABETES, ENDOCRINE diseases, HYPERTENSION, ANIMAL models in research, STREPTOZOTOCIN

Abstract

Background: In experimental models of diabetes mellitus, aggravation of renal injury by concomitant hypertension has been described. Inflammatory mechanisms contribute to renal damage in both diseases. We investigated whether hypertension and diabetes mellitus act synergistically to induce macrophage infiltration and matrix expansion in the kidney. Methods: Insulin-dependent diabetes mellitus was induced by streptozotocin injections to hypertensive mRen2-transgenic rats (TGR) and normotensive Sprague-Dawley control rats. Quantitative immunohistochemical examination of kidney tissue sections was used to measure macrophage infiltration and matrix expansion. The expression of MCP-1, Osteopontin, RANTES, ICAM-1 and VCAM-1 was evaluated by real-time RT-PCR. The localization of MCP-1 was studied by immunohistochemistry. Results: Macrophage infiltration was present in the kidney of normotensive diabetic rats. Hypertensive rats exhibited a more marked infiltration of macrophages, regardless of whether diabetes was present or not. Gene expression of ICAM-1, VCAM-1 and RANTES was unaltered whereas Osteopontin and MCP-1 were induced by hypertension. Immunoreactive MCP-1 was slightly increased in diabetic rat kidney podocytes, and more markedly increased in hypertensive animals. Glomerular matrix accumulation was induced by diabetes and hypertension to a similar degree, and was highest in hypertensive, diabetic animals. Conclusion: Diabetes mellitus caused a mild, and angiotensin-dependent hypertension a more marked infiltration of macrophages in the kidney. Combination of both diseases led to additive effects on matrix expansion but not on inflammation. Hypertension appears to be a much stronger stimulus for inflammation of the kidney than STZ diabetes, at least in mRen2-transgenic rats. [ABSTRACT FROM AUTHOR]

Published

2005

8. From red to white urine: a patient's nightmare with a rather benign outcome.

Author

Knier B, Büschges-Seraphin B, Hilgers KF, Amann KU, Uder M, Eckardt KU, and Jacobi J

Subjects

Female, Humans, Middle Aged, Treatment Outcome, Urine, Urologic Diseases diagnosis, Urologic Diseases urine, Chyle metabolism, Hematuria diagnosis, Hematuria urine

Abstract

Background: Chyluria is a medical condition with presence of chyle in the urine. The disease is most prevalent in endemic regions of Africa and the Indian subcontinent where it is mostly caused by parasitic infections, particularly lymphatic filariasis due to wucheria bancrofti. Non-parasitic chyluria, however, is a very rare finding., Case Presentation: We report the case of a 48 year old woman who developed a lymphorenal fistula with chyluria following ureterrenoscopy with biopsies taken for urological work-up of persistent macrohematuria. Renal biopsy confirmed the diagnosis of benign familial hematuria due to thin basement nephropathy, a condition frequently associated with episodes of macrohematuria., Conclusions: This case highlights a rare case of non-parasitic chyluria as a complication of urological work-up for macrohematuria of benign nature.

Published

2012

9. Acute syphilitic chorioretinitis after a missed primary diagnosis: a case report.

Author

Handtrack C, Knorr H, Amann KU, Schoerner C, Hilgers KF, and Geissdörfer W

Abstract

Introduction: Syphilis is well known as an infectious disease which can present with a large variety of symptoms. Clinical diagnosis can be difficult and may be complicated in modern medicine by immunosuppressive treatment and possible side effects of medication., Case Presentation: We describe a rare case of placoid chorioretinitis due to Treponema pallidum which developed after the primary symptom of proteinuria was not recognized as a rare manifestation of syphilis. Diagnosis of syphilitic chorioretinitis and/or endophthalmitis was made by broad range amplification of the bacterial 16S ribosomal RNA gene obtained from vitreous after diagnostic vitrectomy., Conclusion: This case shows that clinicians should be alert in patients with proteinuria and chorioretinitis as they can represent rare manifestations of syphilis. Syphilis should be in the differential diagnosis of any unknown symptom and in the presumed side effects of medication.

Published

2008