Your search keyword '"Martina Balleininger"' showing total 11 results

1. Cardiac‐specific succinate dehydrogenase deficiency in Barth syndrome

Author

Jan Dudek, I‐Fen Cheng, Arpita Chowdhury, Katharina Wozny, Martina Balleininger, Robert Reinhold, Silke Grunau, Sylvie Callegari, Karl Toischer, Ronald JA Wanders, Gerd Hasenfuß, Britta Brügger, Kaomei Guan, and Peter Rehling

Subjects

Barth syndrome, cardiolipin, mitochondria, respiratory chain, succinate dehydrogenase, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Barth syndrome (BTHS) is a cardiomyopathy caused by the loss of tafazzin, a mitochondrial acyltransferase involved in the maturation of the glycerophospholipid cardiolipin. It has remained enigmatic as to why a systemic loss of cardiolipin leads to cardiomyopathy. Using a genetic ablation of tafazzin function in the BTHS mouse model, we identified severe structural changes in respiratory chain supercomplexes at a pre‐onset stage of the disease. This reorganization of supercomplexes was specific to cardiac tissue and could be recapitulated in cardiomyocytes derived from BTHS patients. Moreover, our analyses demonstrate a cardiac‐specific loss of succinate dehydrogenase (SDH), an enzyme linking the respiratory chain with the tricarboxylic acid cycle. As a similar defect of SDH is apparent in patient cell‐derived cardiomyocytes, we conclude that these defects represent a molecular basis for the cardiac pathology in Barth syndrome.

Published

2015

2. Cardiolipin deficiency affects respiratory chain function and organization in an induced pluripotent stem cell model of Barth syndrome

Author

Ronald J.A. Wanders, Kaomei Guan, I-Fen Cheng, Jan Dudek, Frédéric M. Vaz, Martina Balleininger, Peter Rehling, Katrin Streckfuss-Bömeke, Daniela Hübscher, Milena Vukotic, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Subjects

Male, Cardiolipin, Barth syndrome, Cardiolipins, Induced Pluripotent Stem Cells, Tafazzin, Respiratory chain, Germ layer, Oxidative phosphorylation, Electron Transport, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, medicine, Animals, Humans, Induced pluripotent stem cell, 030304 developmental biology, chemistry.chemical_classification, Medicine(all), 0303 health sciences, Reactive oxygen species, biology, General Medicine, Cell Biology, Fibroblasts, medicine.disease, 3. Good health, Cell biology, chemistry, Biochemistry, Barth Syndrome, biology.protein, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Barth syndrome (BTHS) patients carrying mutations in tafazzin (TAZ1), which is involved in the final maturation of cardiolipin, present with dilated cardiomyopathy, skeletal myopathy, growth retardation and neutropenia. To study how mitochondrial function is impaired in BTHS patients, we generated induced pluripotent stem cells (iPSCs) to develop a novel and relevant human model system for BTHS. BTHS-iPSCs generated from dermal fibroblasts of three patients with different mutations in TAZ1 expressed pluripotency markers, and were able to differentiate into cells derived from all three germ layers both in vitro and in vivo. We used these cells to study the impact of tafazzin deficiency on mitochondria( oxidative phosphorylation. We found an impaired remodeling of cardiolipin, a dramatic decrease in basal oxygen consumption rate and in the maximal respiratory capacity in BTHS-iPSCs. Simultaneous measurement of extra-cellular acidification rate allowed us a thorough assessment of the metabolic deficiency in BTHS patients. Blue native gel analyses revealed that decreased respiration coincided with dramatic structural changes in respiratory chain supercomplexes leading to a massive increase in generation of reactive oxygen species. Our data demonstrate that BTHS-iPSCs are capable of modeling BTHS by recapitulating the disease phenotype and thus are important tools for studying the disease mechanism. (C) 2013 The Authors. Published by Elsevier B.V. All rights reserved.

Published

2013

3. Cardiac-specific succinate dehydrogenase deficiency in Barth syndrome

Author

I-Fen Cheng, Ronald Ja Wanders, Silke D. Grunau, Arpita Chowdhury, Robert Reinhold, Peter Rehling, Gerd Hasenfuß, Katharina Wozny, Martina Balleininger, Jan Dudek, Britta Brügger, Sylvie Callegari, Karl Toischer, Kaomei Guan, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Subjects

0301 basic medicine, medicine.medical_specialty, respiratory chain, Tafazzin, Cardiomyopathy, Respiratory chain, Mitochondrion, Cardiovascular System, Mice, 03 medical and health sciences, chemistry.chemical_compound, Internal medicine, medicine, Cardiolipin, Animals, Humans, Cells, Cultured, Research Articles, biology, Succinate dehydrogenase, Barth syndrome, succinate dehydrogenase, medicine.disease, cardiolipin, mitochondria, Citric acid cycle, Disease Models, Animal, Metabolism, 030104 developmental biology, Endocrinology, chemistry, Barth Syndrome, biology.protein, Molecular Medicine, Genetics, Gene Therapy & Genetic Disease, Research Article

Abstract

Barth syndrome (BTHS) is a cardiomyopathy caused by the loss of tafazzin, a mitochondrial acyltransferase involved in the maturation of the glycerophospholipid cardiolipin. It has remained enigmatic as to why a systemic loss of cardiolipin leads to cardiomyopathy. Using a genetic ablation of tafazzin function in the BTHS mouse model, we identified severe structural changes in respiratory chain supercomplexes at a pre-onset stage of the disease. This reorganization of supercomplexes was specific to cardiac tissue and could be recapitulated in cardiomyocytes derived from BTHS patients. Moreover, our analyses demonstrate a cardiac-specific loss of succinate dehydrogenase (SDH), an enzyme linking the respiratory chain with the tricarboxylic acid cycle. As a similar defect of SDH is apparent in patient cell-derived cardiomyocytes, we conclude that these defects represent a molecular basis for the cardiac pathology in Barth syndrome. peerReviewed

Published

2015

4. Aim24 stabilizes respiratory chain supercomplexes and is required for efficient respiration

Author

Markus Deckers, Katharina Römpler, Bettina Bareth, Jan Dudek, Milena Vukotic, Lisa Juris, and Martina Balleininger

Subjects

Supercomplex, Saccharomyces cerevisiae Proteins, Molecular Sequence Data, Biophysics, Respiratory chain, Saccharomyces cerevisiae, Biology, Mitochondrion, Biochemistry, Aim24, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Genetics, Cytochrome c oxidase, Amino Acid Sequence, Inner mitochondrial membrane, Molecular Biology, 030304 developmental biology, Membrane potential, 0303 health sciences, Protein Stability, Respiration, Cell Biology, Cell biology, Culture Media, Mitochondria, Transduction (biophysics), Mitochondrial respiratory chain, Metabolism, Membrane protein, Electron Transport Chain Complex Proteins, Mitochondrial Membranes, biology.protein, 030217 neurology & neurosurgery

Abstract

The mitochondrial respiratory chain is essential for the conversion of energy derived from the oxidation of metabolites into the membrane potential, which drives the synthesis of ATP. The electron transporting complexes bc1 complex and the cytochrome c oxidase assemble into large supercomplexes, allowing efficient energy transduction. Currently, we have only limited information about what determines the structure of the supercomplex. Here, we characterize Aim24 in baker’s yeast as a protein, which is integrated in the mitochondrial inner membrane and is required for the structural integrity of the supercomplex. Deletion of AIM24 strongly affects activity of the respiratory chain and induces a growth defect on non-fermentable medium. Our data indicate that Aim24 has a function in stabilizing the respiratory chain supercomplexes.

Published

2014

5. Characterization of Posttranslational Formylglycine Formation by Luminal Components of the Endoplasmic Reticulum

Author

Jens Fey, Ljudmila V. Borissenko, Martina Balleininger, Kurt von Figura, Thomas Dierks, and Bernhard Schmidt

Subjects

Time Factors, Detergents, Molecular Sequence Data, Glycine, Endoplasmic Reticulum, Biochemistry, Ribosome, Catalysis, 03 medical and health sciences, chemistry.chemical_compound, Dogs, 0302 clinical medicine, Microsomes, Animals, Amino Acid Sequence, Pancreas, Molecular Biology, 030304 developmental biology, 0303 health sciences, Alanine, Binding Sites, Dose-Response Relationship, Drug, biology, Sulfatase, Endoplasmic reticulum, Temperature, Active site, Intracellular Membranes, Cell Biology, Hydrogen-Ion Concentration, Protein O-Methyltransferase, Kinetics, Protein Transport, chemistry, Puromycin, Protein Biosynthesis, Microsomes, Liver, biology.protein, Microsome, Calcium, Cattle, Salts, Formylglycine-generating enzyme, Peptides, Protein Processing, Post-Translational, Ribosomes, 030217 neurology & neurosurgery, Cysteine

Abstract

C(alpha)-formylglycine is the key catalytic residue in the active site of sulfatases. In eukaryotes formylglycine is generated during or immediately after sulfatase translocation into the endoplasmic reticulum by oxidation of a specific cysteine residue. We established an in vitro assay that allowed us to measure formylglycine modification independent of protein translocation. The modifying enzyme was recovered in a microsomal detergent extract. As a substrate we used ribosome-associated nascent chain complexes comprising in vitro synthesized sulfatase fragments that were released from the ribosomes by puromycin. Formylglycine modification was highly efficient and did not require a signal sequence in the substrate polypeptide. Ribosome association helped to maintain the modification competence of nascent chains but only after their release efficient modification occurred. The modifying machinery consists of soluble components of the endoplasmic reticulum lumen, as shown by differential extraction of microsomes. The in vitro assay can be performed under kinetically controlled conditions. The activation energy for formylglycine formation is 61 kJ/mol, and the pH optimum is approximately 10. The activity is sensitive to the SH/SS equilibrium and is stimulated by Ca(2+). Formylglycine formation is efficiently inhibited by a synthetic sulfatase peptide representing the sequence directing formylglycine modification. The established assay system should make possible the biochemical identification of the modifying enzyme.

Published

2001

6. Mimicking a SURF1 allele reveals uncoupling of cytochrome c oxidase assembly from translational regulation in yeast

Author

Bettina Bareth, Peter Rehling, Martina Balleininger, Robert Reinhold, Mirjam Wissel, and David U. Mick

Subjects

Saccharomyces cerevisiae Proteins, Blotting, Western, Respiratory chain, Mutation, Missense, Oxidative phosphorylation, Saccharomyces cerevisiae, Mitochondrion, Cell Line, Electron Transport Complex IV, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Gene Expression Regulation, Fungal, Translational regulation, Genetics, Cytochrome c oxidase, Humans, Immunoprecipitation, SURF1, Cloning, Molecular, Molecular Biology, Genetics (clinical), 030304 developmental biology, 0303 health sciences, biology, Cytochrome b, Cytochrome c, Membrane Proteins, General Medicine, Sequence Analysis, DNA, Biochemistry, Amino Acid Substitution, biology.protein, Electrophoresis, Polyacrylamide Gel, Energy Metabolism, 030217 neurology & neurosurgery, Plasmids

Abstract

Defects in mitochondrial energy metabolism lead to severe human disorders, mainly affecting tissues especially dependent on oxidative phosphorylation, such as muscle and brain. Leigh Syndrome describes a severe encephalomyopathy in infancy, frequently caused by mutations in SURF1. SURF1, termed Shy1 in Saccharomyces cerevisiae, is a conserved assembly factor for the terminal enzyme of the respiratory chain, cytochrome c oxidase. Although the molecular function of SURF1/Shy1 is still enigmatic, loss of function leads to cytochrome c oxidase deficiency and reduced expression of the central subunit Cox1 in yeast. Here, we provide insights into the molecular mechanisms leading to disease through missense mutations in codons of the most conserved amino acids in SURF1. Mutations affecting G(124) do not compromise import of the SURF1 precursor protein but lead to fast turnover of the mature protein within the mitochondria. Interestingly, an Y(274)D exchange neither affects stability nor localization of the protein. Instead, SURF1(Y274D) accumulates in a 200 kDa cytochrome c oxidase assembly intermediate. Using yeast as a model, we demonstrate that the corresponding Shy1(Y344D) is able to overcome the stage where cytochrome c oxidase assembly links to the feedback regulation of mitochondrial Cox1 expression. However, Shy1(Y344D) impairs the assembly at later steps, most apparent at low temperature and exhibits a dominant-negative phenotype upon overexpression. Thus, exchanging the conserved tyrosine (Y(344)) with aspartate in yeast uncouples translational regulation of Cox1 from cytochrome c oxidase assembly and provides evidence for the dual functionality of Shy1.

Published

2011

7. Sulf loss influences N-, 2-O-, and 6-O-sulfation of multiple heparan sulfate proteoglycans and modulates fibroblast growth factor signaling

Author

Thomas Dierks, Marc-André Frese, Martina Balleininger, and William C. Lamanna

Subjects

Cell signaling, Perlecan, Biology, Fibroblast growth factor, Disaccharides, Biochemistry, Gene Expression Regulation, Enzymologic, Substrate Specificity, Extracellular matrix, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Sulfation, SULF1, Cell Line, Tumor, Animals, Humans, Molecular Biology, 030304 developmental biology, 0303 health sciences, Cell Biology, Heparan sulfate, Fibroblast Growth Factors, Wnt Proteins, Proteoglycan, chemistry, 030220 oncology & carcinogenesis, biology.protein, Sulfatases, Sulfotransferases, Heparan Sulfate Proteoglycans, Signal Transduction

Abstract

Sulf1 and Sulf2 are two heparan sulfate 6-O-endosulfatases that regulate the activity of multiple growth factors, such as fibroblast growth factor and Wnt, and are essential for mammalian development and survival. In this study, the mammalian Sulfs were functionally characterized using overexpressing cell lines, in vitro enzyme assays, and in vivo Sulf knock-out cell models. Analysis of subcellular Sulf localization revealed significant differences in enzyme secretion and detergent solubility between the human isoforms and their previously characterized quail orthologs. Further, the activity of the Sulfs toward their native heparan sulfate substrates was determined in vitro, demonstrating restricted specificity for S-domain-associated 6S disaccharides and an inability to modify transition zone-associated UA-GlcNAc( 6S). Analysis of heparan sulfate composition from different cell surface, shed, glycosylphosphatidylinositol- anchored and extracellular matrix proteoglycan fractions of Sulf knock-out cell lines established differential effects of Sulf1 and/or Sulf2 loss on nonsubstrate N-, 2-O-, and 6-O-sulfate groups. These findings indicate a dynamic influence of Sulf deficiency on the HS biosynthetic machinery. Real time PCR analysis substantiated differential expression of the Hs2st and Hs6st heparan sulfate sulfotransferase enzymes in the Sulf knock-out cell lines. Functionally, the changes in heparan sulfate sulfation resulting from Sulf loss were shown to elicit significant effects on fibroblast growth factor signaling. Taken together, this study implicates that the Sulfs are involved in a potential cellular feed-back mechanism, in which they edit the sulfation of multiple heparan sulfate proteoglycans, thereby regulating cellular signaling and modulating the expression of heparan sulfate biosynthetic enzymes.

Published

2008

8. Identification of novel lysosomal matrix proteins by proteome analysis

Author

Torben Lübke, Kurt von Figura, Bernhard Schmidt, Ellen Eckermann, Kudzai Mutenda, Katrin Kollmann, and Martina Balleininger

Subjects

Proteome, Mannose, Mannose 6-phosphate, Biology, Proteomics, Biochemistry, Chromatography, Affinity, Receptor, IGF Type 2, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Mice, Lysosome, medicine, Animals, Humans, Electrophoresis, Gel, Two-Dimensional, Molecular Biology, 030304 developmental biology, Gel electrophoresis, 0303 health sciences, Mannose 6-phosphate receptor, Mannosephosphates, 030302 biochemistry & molecular biology, Intracellular Signaling Peptides and Proteins, Proteins, Fibroblasts, Embryo, Mammalian, Endocytosis, medicine.anatomical_structure, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Lysosomal matrix

Abstract

The lysosomal matrix is estimated to contain about 50 different proteins. Most of the matrix proteins are acid hydrolases that depend on mannose 6-phosphate receptors (MPR) for targeting to lysosomes. Here, we describe a comprehensive proteome analysis of MPR-binding proteins from mouse. Mouse embryonic fibroblasts defective in both MPR (MPR 46-/- and MPR 300-/-) are known to secrete the lysosomal matrix proteins. Secretions of these cells were affinity purified using an affinity matrix derivatized with MPR46 and MPR300. In the protein fraction bound to the affinity matrix and eluted with mannose 6-phosphate, 34 known lysosomal matrix proteins, 4 candidate proteins of the lysosomal matrix and 4 non-lysosomal contaminants were identified by mass spectrometry after separation by two-dimensional gel electrophoresis or by multidimensional protein identification technology. For 3 of the candidate proteins, mammalian ependymin-related protein-2 (MERP-2), retinoid-inducible serine carboxypeptidase (RISC) and the hypothetical 66.3-kDa protein we could verify that C-terminally tagged forms bound in an M6P-dependent manner to an MPR-affinity matrix and were internalized via MPR-mediated endocytosis. Hence these 3 proteins are likely to represent hitherto unrecognized lysosomal matrix proteins.

Published

2005

9. Expression, localization, structural, and functional characterization of pFGE, the paralog of the C alpha-formylglycine-generating enzyme

Author

Bernhard Schmidt, Nicole Eiselt, Santosh Lakshmi Gande, Martina Balleininger, Malaiyalam Mariappan, Dirk Wenzel, Thomas Dierks, Kurt von Figura, and Andrea Preusser-Kunze

Subjects

Glycosylation, Time Factors, Endoplasmic Reticulum, Biochemistry, Mass Spectrometry, Oxidoreductases Acting on Sulfur Group Donors, Tissue Distribution, Trypsin, Fluorescent Antibody Technique, Indirect, Microscopy, Immunoelectron, Skin, chemistry.chemical_classification, Alanine, biology, Sulfatase, Recombinant Proteins, Cross-Linking Reagents, Formylglycine-generating enzyme, Sulfatases, DNA, Complementary, Blotting, Western, Molecular Sequence Data, Glycine, Transfection, Binding, Competitive, Catalysis, Cell Line, Multiple sulfatase deficiency, Two-Hybrid System Techniques, medicine, Humans, Immunoprecipitation, Codon, Molecular Biology, Binding Sites, Endoplasmic reticulum, Active site, Cell Biology, Fibroblasts, medicine.disease, bacterial infections and mycoses, Blotting, Northern, In vitro, Enzyme, Mannosyl-Glycoprotein Endo-beta-N-Acetylglucosaminidase, chemistry, biology.protein, Peptides, Protein Processing, Post-Translational, Cysteine

Abstract

pFGE is the paralog of the formylglycine-generating enzyme (FGE), which catalyzes the oxidation of a specific cysteine to C alpha-formylglycine, the catalytic residue in the active site of sulfatases. The enzymatic activity of sulfatases depends on this posttranslational modification, and the genetic defect of FGE causes multiple sulfatase deficiency. The structural and functional properties of pFGE were analyzed. The comparison with FGE demonstrates that both share a tissue-specific expression pattern and the localization in the lumen of the endoplasmic reticulum. Both are retained in the endoplasmic reticulum by a saturable mechanism. Limited proteolytic cleavage at similar sites indicates that both also share a similar three-dimensional structure. pFGE, however, is lacking the formylglycine-generating activity of FGE. Although overexpression of FGE stimulates the generation of catalytically active sulfatases, overexpression of pFGE has an inhibitory effect. In vitro pFGE interacts with sulfatase-derived peptides but not with FGE. The inhibitory effect of pFGE on the generation of active sulfatases may therefore be caused by a competition of pFGE and FGE for newly synthesized sulfatase polypeptides.

Published

2005

10. The iron sulfur protein AtsB is required for posttranslational formation of formylglycine in the Klebsiella sulfatase

Author

Claudia Miech, Thomas Dierks, Bernhard Schmidt, Kurt von Figura, Martina Balleininger, and Claudia Szameit

Subjects

Iron-Sulfur Proteins, Operon, Molecular Sequence Data, Glycine, Borohydrides, Transfection, medicine.disease_cause, 01 natural sciences, Biochemistry, Serine, Gene product, 03 medical and health sciences, Bacterial Proteins, Escherichia coli, medicine, Cloning, Molecular, Molecular Biology, 030304 developmental biology, 0303 health sciences, Alanine, 010405 organic chemistry, Chemistry, Sulfatase, Structural gene, Gene Expression Regulation, Bacterial, Cell Biology, Periplasmic space, Recombinant Proteins, 0104 chemical sciences, Klebsiella pneumoniae, Formylglycine-generating enzyme, Sulfatases, Protein Processing, Post-Translational

Abstract

The catalytic residue of eukaryotic and prokaryotic sulfatases is a alpha-formylglycine. In the sulfatase of Klebsiella pneumoniae the formylglycine is generated by posttranslational oxidation of serine 72. We cloned the atsBA operon of K. pneumoniae and found that the sulfatase was expressed in inactive form in Escherichia coli transformed with the structural gene (atsA). Coexpression of the atsB gene, however, led to production of high sulfatase activity, indicating that the atsB gene product plays a posttranslational role that is essential for the sulfatase to gain its catalytic activity. This was verified after purification of the sulfatase from the periplasm of the cells. Peptide analysis of the protein expressed in the presence of AtsB revealed that half of the polypeptides carried the formylglycine at position 72, while the remaining polypeptides carried the encoded serine. The inactive sulfatase expressed in the absence of AtsB carried exclusively serine 72, demonstrating that the atsB gene is required for formylglycine modification. This gene encodes a 395-amino acid residue iron sulfur protein that has a cytosolic localization and is supposed to directly or indirectly catalyze the oxidation of the serine to formylglycine.

Published

1999

11. Identification of novel lysosomal matrix proteins by proteome analysis.

Author

Katrin Kollmann, Kudzai E. Mutenda, Martina Balleininger, Ellen Eckermann, Kurt von Figura, Bernhard Schmidt, and Torben Lübke

Published

2005