Your search keyword '"Dietrich Feist"' showing total 6 results

1. Bile duct to portal space ratio and ductal plate remnants in liver disease of infants aged less than 1 year

Author

Herwart F. Otto, Consolato Sergi, Walter J. Hofmann, Dietrich Feist, Julia Benstz, and Walter Nützenadel

Subjects

medicine.medical_specialty, Pathology, Intrahepatic bile ducts, Kaplan-Meier Estimate, Biology, Gastroenterology, Pathology and Forensic Medicine, Liver disease, Cholestasis, Biliary atresia, Internal medicine, medicine, Humans, Bile duct, Liver Diseases, Keratin-7, Infant, Newborn, Infant, Prognosis, medicine.disease, Immunohistochemistry, Ductal Plate Malformation, Neonatal hepatitis, Portal System, Bile Ducts, Intrahepatic, medicine.anatomical_structure, Portal fibrosis

Abstract

To validate the bile duct to portal space ratio as an independent factor useful for the prognosis of neonatal liver disease.We assessed the maturation of the intrahepatic bile duct system (IBDS) in 87 consecutive infants aged less than 1 year undergoing non-subcapsular, adequate (at least six portal tracts), liver needle biopsies because of hepatomegaly and/or cholestasis. The maturation of the IBDS was evaluated by immunohistochemistry with an antibody directed to cytokeratin 7 (CK7), a biliary-type intermediate filament of the cytoskeleton, and a schema showing the IBDS remodelling. We used five categories to fit the different patterns of the IBDS remodelling using the ratio between the number of bile ducts and the number of portal tracts (BD/PT) and the presence of abnormal reaction patterns (marked intra-acinar pseudorosettes and/or periportal ductular proliferation): (A) abnormal reaction patterns with any BD/PT; (B) BD/PT = 0; (C) 0.1or = BD/PT0.5; (D) 0.5or = BD/PT0.9; and (E) BD/PT0.9 (B-E categories: no abnormal reaction patterns). Further, we evaluated cholestasis, portal fibrosis (PF), portal inflammation (PI), giant cell transformation (GCT), and extramedullary haematopoiesis (EMH).We identified A-E categories in 24, 14, 17, 8, and 24 biopsies, respectively. B and C categories were frequently observed in biliary atresia (BA), A category in neonatal hepatitis (NH), A-C categories in paucity of intrahepatic bile ducts (PIBD), and E category in 'other liver diseases' (OLD). Cholestasis, PI, GCT, and EMH were more frequent in A and C, while PF was variably seen in all categories. The lowest survival rate occurred in B (Kaplan-Meier estimator).(1) Biliary epithelial cell patterns recapitulate the primitive stages of the IBDS maturation; (2) abnormal reaction patterns occur mainly in NH, whilst BD/PT0.5 in BA; and (3) lack of intrahepatic bile ducts in infants aged less than 1 year is an adverse prognostic factor independent from aetiology of neonatal liver disease.

Published

2008

2. Autorinnen und Autoren

Author

Wiebke Ahrens, Michael A. Baumann, Rolf Behrens, Bernd H. Belohradsky, Hansjosef Böhles, Jürgen H. Brämswig, Ulrich Brandl, Rolf E. Brenner, Konrad Brockmeier, Rainer Büscher, Michael Diestelhorst, Gerd Dockter, Manfred Döpfner, Helmuth Günther Dörr, Hans Edmund Eckel, Peter Edelmann, Franz F. Eifinger, Udo H. Engelmann, Manigé Fartasch, Dietrich Feist, Gerhard Gaedicke, Manfred Gahr, Gerd Ganser, Alexander von Gontard, Klaus-Peter Grosse, Annette Grüters-Kieslich, Berthold P. Hauffa, Ulrich Heininger, Peter Herkenrath, Michael Hofbeck, Reinhard W. Holl, Alexander M. Holschneider, Bernd Hoppe, Hans-Iko Huppertz, Gabriele Jopp-Petzinna, Bärbel Kahl-Nieke, Klaus-Michael Keller, Martin Kirschstein, Günter Klaus, Lars Klinge, Berthold Koletzko, Sibylle Koletzko, Martin Konrad, Bernhard Korge, Christof Land, Heinz Lauffer, Gerd Lehmkuhl, Michael J. Lentze, Bernhard Lettgen, Christoph Licht, Esther Lowden, Johannes Luckhaus, Dietrich Michalk, Jan Müller-Berghaus, Dirk E. Müller-Wiefel, Emil G. Naumann, Gerhard Neuhäuser, Walter Nützenadel, Ekkehart Paditz, Carl-Joachim Partsch, Karl Paul, Frank Pillekamp, Uwe Querfeld, Michael B. Ranke, Wolfgang Rascher, Frank Riedel, Ernst Rietschel, Bernhard Roth, Walter Rüssmann, Jürgen Rütt, Ulrike Schauseil-Zipf, Eckhard Schönau, Elke Schubert, Bernd Schwahn, Lothar Schweigerer, Hannsjörg W. Seyberth, Thorsten Simon, Helmut Singer, Gernot H.G. Sinnecker, Stephan Sollberg, Wolfgang Sperl, Georg Mathias Sprinzl, Michael Streppel, Anton H. Sutor†, Michael A. Überall, Herbert E. Ulmer, Thomas Voit, Martin Wabitsch, Ulrich Wahn, Siegfried Waldegger, Martin Walger, Hasso von Wedel, Ulla-Christiane von Wedel, Michael Weiß, Gerhard Weißbach, Brigitte Widemann, Stefan Wirth, Joachim E. Zöller, and Torsten Zuberbier

Published

2011

3. Hepatomegalie

Author

Dietrich Feist and Stefan Wirth

Published

2011

4. Hepatomegalie

Author

Stefan Wirth and Dietrich Feist

Published

2005

5. Familial clustering of infantile cirrhosis in Northern Germany: A clue to the etiology of idiopathic copper toxicosis

Author

Hansjörg Schäfer, Hartmut Koch, Dietrich Feist, Rainer Krech, Thomas Müller, Jürgen Brämswig, Karl Ernst von Mühlendahl, Hans Feichtinger, W Müller, Hendrik Bosse, Burkhard Rodeck, Peter Welling, Heribert Lange, and Georg Haupt

Subjects

Liver Cirrhosis, Male, Pathology, medicine.medical_specialty, Pediatrics, Cirrhosis, Consanguinity, Indian childhood cirrhosis, Disease cluster, Genetic determinism, Germany, medicine, Genetic predisposition, Humans, Genetic Predisposition to Disease, Risk factor, Age of Onset, business.industry, Infant, Water, medicine.disease, Diet, Pedigree, Pediatrics, Perinatology and Child Health, Etiology, Female, business, Copper

Abstract

Two cases of infantile liver cirrhosis of unknown origin occurred in a circumscribed rural area of Northern Germany. Both children had increased dietary copper exposure. The search for additional cases of what appeared to be idiopathic copper toxicosis (ICT) revealed a cluster of affected infants in this region, raising questions about the relative importance of genetic and environmental factors that are considered to be etiologic. We gathered clinical and pathologic data concerning the patients, analyzed the pedigrees of affected families, and searched for possible environmental factors contributing to the pathologic process. We encountered 8 cases of infantile liver cirrhosis in 5 families in Emsland, a circumscribed and predominantly rural area of Northern Germany; ICT was definitely proven in 2 cases. Clinical presentation and liver pathology in 6 additional cases were consistent with the diagnosis of ICT. Pedigrees of affected families revealed complex relationships with occasional consanguinity of parents, suggesting autosomal recessive inheritance. The households were served by private wells with water of low pH flowing through copper pipes, suggesting the possibility of increased alimentary copper exposure. These findings support earlier conclusions that ICT develops when an infant with a genetic predisposition is exposed to a copper-enriched diet.

Published

1999

6. Fanconi-Bickel syndrome

Author

Friedrich Manz, Horst Bickel, Johannes Brodehl, Dietrich Feist, Karl Gellissen, Brigitte Gesch�ll-Bauer, Giulio Gilli, Erik Harms, Helmut Helwig, Walter N�tzenadel, and R�diger Waldherr

Subjects

Nephrology, Adult, Male, medicine.medical_specialty, Adolescent, Renal function, Late onset, Carbohydrate metabolism, Short stature, Renal tubular dysfunction, Internal medicine, Medicine, Humans, Child, Kidney, business.industry, Glucose transporter, Infant, Syndrome, Fanconi Syndrome, Glycogen Storage Disease, Endocrinology, medicine.anatomical_structure, Pediatrics, Perinatology and Child Health, Female, medicine.symptom, business

Abstract

Clinical, biochemical, functional and morphological data are presented in nine infants, children and adults, with Fanconi-Bickel syndrome. Long-term follow-up studies show severe growth retardation, partly compensated for by late onset of puberty. Glomerular filtration rate is normal or slightly decreased. Renal tubular dysfunction is characterized by a specific pattern of impaired proximal tubular transport mechanisms, with marked impairment of glucose transport. The utilization of glucose and galactose is defective, whereas fructose metabolism seems to be normal. Glycogenosis of the liver may be an epiphenomenon. Glycogen accumulation in the kidney is limited to the proximal tubule, with maximal levels in the straight part. The Fanconi-Bickel syndrome is a defined clinical entity which is distinguished from other inherited metabolic diseases by complex defects of renal tubular transport and other forms of glycogenosis.

Published

1987