Your search keyword '"Tanja Wittkampf"' showing total 7 results

1. An Unusual Severe Vascular Case of Pseudoxanthoma Elasticum Presenting as Generalized Arterial Calcification of Infancy

Author

Nicolas Chassaing, G. Le Boulanger, Frank Rutsch, C. Labrèze, A. Croué, Ludovic Martin, Leon J. Schurgers, Tanja Wittkampf, Biochemie, and RS: CARIM School for Cardiovascular Diseases

Subjects

Adult, Male, Candidate gene, Pathology, medicine.medical_specialty, Genotype, ABCC6, generalized arterial calcification of infancy, Generalized arterial calcification, genetic heterogeneity, Calcinosis, Matrix gla protein, mineralization inhibitors, Genetics, medicine, Humans, Pyrophosphatases, pseudoxanthoma elasticum, Genetics (clinical), ENPP1, biology, Genetic heterogeneity, business.industry, Phosphoric Diester Hydrolases, Infant, Anatomy, Arteries, medicine.disease, Pseudoxanthoma elasticum, Immunohistochemistry, Pedigree, idiopathic arterial calcification of infancy, Mutation, biology.protein, Female, Multidrug Resistance-Associated Proteins, business, Calcification

Abstract

Pseudoxanthoma elasticum (PXE) is an autosomal recessive disease affecting tissues rich in elastic fibers such as the skin, retina, and cardiovascular system. Mutations in the ABCC6 gene are known to be causative in most patients. Generalized arterial calcification of infancy (GACI) is characterized by extensive hydroxyapatite deposits in the internal elastic laminae in large and medium-sized arteries, leading to arterial stenoses and early and severe myocardial ischemia. GACI has been found to be primarily caused by mutations in the ENPP1 gene. We report two brothers born to unrelated parents. The elder developed uncomplicated PXE in adolescence and harbored mutations in the ABCC6 gene. The younger child died of a condition strikingly reminiscent of GACI at 15 months of age. This case of GACI was independent of mutations in the ENPP1 gene but was probably related to ABCC6 mutations. We demonstrate that matrix Gla protein and fetuin-A, involved in PXE, are also expressed in this case of GACI. These proteins could act as local and systemic inhibitors to limit the extension of mineralization. This report emphasizes concurrently that ABCC6 may be a relevant candidate gene in some cases of GACI with no mutations in the ENPP1 gene, and that GACI may be an atypical and severe end of the vascular phenotype spectrum of PXE.

Published

2010

2. Functional Consequences of Mitochondrial DNA Deletions in Human Skin Fibroblasts

Author

Peter Schroeder, Jean Krutmann, Bianca Schuermann, Marc Majora, Tanja Wittkampf, Ekkehard Wilichowski, Susanne Franke, Maren Schneider, Susanne Grether-Beck, and Françoise Bernerd

Subjects

musculoskeletal diseases, 0303 health sciences, Mitochondrial DNA, integumentary system, medicine.diagnostic_test, DNA damage, Lysyl oxidase, Human skin, Mitochondrion, Biology, medicine.disease_cause, Molecular biology, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Western blot, 030220 oncology & carcinogenesis, medicine, Fibroblast, Oxidative stress, 030304 developmental biology

Abstract

Deletions within the mitochondrial DNA (mtDNA) are thought to contribute to extrinsic skin aging. To study the translation of mtDNA deletions into functional and structural changes in the skin, we seeded human skin fibroblasts into collagen gels to generate dermal equivalents. These cells were either derived from Kearns-Sayre syndrome (KSS) patients, who constitutively carry large amounts of the UV-inducible mitochondrial common deletion, or normal human volunteers. We found that KSS fibroblasts, in comparison with normal human fibroblasts, contracted the gels faster and more strongly, an effect that was dependent on reactive oxygen species. Gene expression and Western blot analysis revealed significant upregulation of lysyl oxidase (LOX) in KSS fibroblasts. Treatment with the specific LOX inhibitor β-aminopropionitrile decreased the contraction difference between KSS and normal human fibroblast equivalents. Also, addition of the antioxidant N-tert-butyl-α-phenylnitrone reduced the contraction difference by inhibiting collagen gel contraction in KSS fibroblasts, and both β-aminopropionitrile and N-tert-butyl-α-phenylnitrone diminished LOX activity. These data suggest a causal relationship between mtDNA deletions, reactive oxygen species production, and increased LOX activity that leads to increased contraction of collagen gels. Accordingly, increased LOX expression was also observed in vivo in photoaged human and mouse skin. Therefore, mtDNA deletions in human fibroblasts may lead to functional and structural alterations of the skin.

Published

2009

3. Generalized arterial calcification of infancy and pseudoxanthoma elasticum can be caused by mutations in either ENPP1 or ABCC6

Author

Justin H Davies, Geneviève Baujat, Samuel J. Garber, Stephen G. Kahler, Olivier Roche, Smail Hadj-Rabia, Jacqueline Stella, Martine Le Merrer, Rashmi Chikarmane, Karen J. Loechner, Wendy E. Smith, Loreto Martorell, Tatevik Shahinyan, Marie-Frederique Tazarourte-Pinturier, Robert Terkeltaub, Elizabeth Wraige, Tanja Wittkampf, Charu Deshpande, Wolfgang Höhne, Lourdes Loidi, Yvonne Nitschke, Ilse Feenstra, Frank Rutsch, Beat Steinmann, Ludovic Martin, Ulrike Botschen, Guest G, K Lambot, Nicolas Chassaing, Marcel du Moulin, Mignon McCulloch, University of Zurich, and Rutsch, Frank

Subjects

Male, Proband, Pathology, medicine.medical_specialty, 2716 Genetics (clinical), Molecular Sequence Data, ABCC6, 610 Medicine & health, Biology, Article, Generalized arterial calcification, Genomic disorders and inherited multi-system disorders [IGMD 3], 03 medical and health sciences, Ectopic calcification, 0302 clinical medicine, Genotype-phenotype distinction, 1311 Genetics, Surveys and Questionnaires, Genotype, medicine, Genetics, Humans, Genetics(clinical), Pseudoxanthoma Elasticum, Pyrophosphatases, Child, Vascular Calcification, Genetics (clinical), Retrospective Studies, 030304 developmental biology, 0303 health sciences, Base Sequence, Phosphoric Diester Hydrolases, Infant, Pseudoxanthoma elasticum, medicine.disease, 3. Good health, 10036 Medical Clinic, Child, Preschool, 030220 oncology & carcinogenesis, Mutation, biology.protein, Angioid Streaks, Female, Multidrug Resistance-Associated Proteins, Calcification

Abstract

Item does not contain fulltext Spontaneous pathologic arterial calcifications in childhood can occur in generalized arterial calcification of infancy (GACI) or in pseudoxanthoma elasticum (PXE). GACI is associated with biallelic mutations in ENPP1 in the majority of cases, whereas mutations in ABCC6 are known to cause PXE. However, the genetic basis in subsets of both disease phenotypes remains elusive. We hypothesized that GACI and PXE are in a closely related spectrum of disease. We used a standardized questionnaire to retrospectively evaluate the phenotype of 92 probands with a clinical history of GACI. We obtained the ENPP1 genotype by conventional sequencing. In those patients with less than two disease-causing ENPP1 mutations, we sequenced ABCC6. We observed that three GACI patients who carried biallelic ENPP1 mutations developed typical signs of PXE between 5 and 8 years of age; these signs included angioid streaks and pseudoxanthomatous skin lesions. In 28 patients, no disease-causing ENPP1 mutation was found. In 14 of these patients, we detected pathogenic ABCC6 mutations (biallelic mutations in eight patients, monoallelic mutations in six patients). Thus, ABCC6 mutations account for a significant subset of GACI patients, and ENPP1 mutations can also be associated with PXE lesions in school-aged children. Based on the considerable overlap of genotype and phenotype of GACI and PXE, both entities appear to reflect two ends of a clinical spectrum of ectopic calcification and other organ pathologies, rather than two distinct disorders. ABCC6 and ENPP1 mutations might lead to alterations of the same physiological pathways in tissues beyond the artery.

Published

2012

4. Hypophosphatemia, hyperphosphaturia, and bisphosphonate treatment are associated with survival beyond infancy in generalized arterial calcification of infancy

Author

Rudolf-Josef Fischer, Nico Ruf, John Gregory, Bettina Lorenz-Depierieux, Peter Nürnberg, Zulf Mughal, Tanja Wittkampf, Tim M. Strom, Petra Böyer, Frank Rutsch, Yvonne Nitschke, Chantal Loirat, Dirk Schnabel, Justin H Davies, Gabriele Weissen-Plenz, Robert Terkeltaub, Van Reempts, Patrick, et al., and GACI Study Group

Subjects

Male, medicine.medical_specialty, Pathology, Heterozygote, RJ, Hypophosphatemia, RJ101, Gastroenterology, Generalized arterial calcification, Article, Cohort Studies, Calcinosis, Internal medicine, Genetics, medicine, Humans, Pyrophosphatases, Genetics (clinical), Survival analysis, Alleles, Hypophosphatemia, Familial, Ultrasonography, Diphosphonates, business.industry, Phosphoric Diester Hydrolases, Homozygote, Angiography, Infant, Newborn, Infant, Arteries, medicine.disease, R1, Hyperphosphaturia, Infant newborn, Survival Analysis, Mutation, Female, Human medicine, Cardiology and Cardiovascular Medicine, business, Bisphosphonate treatment

Abstract

Background—Generalized arterial calcification of infancy has been reported to be frequently lethal, and the efficiency of any therapy, including bisphosphonates, is unknown. A phosphate-poor diet markedly increases survival of NPP1 null mice, a model of generalized arterial calcification of infancy.Methods and Results—We performed a multicenter genetic study and retrospective observational analysis of 55 subjects affected by generalized arterial calcification of infancy to identify prognostic factors. Nineteen (34%) patients survived the critical period of infancy. In all 8 surviving patients tested, hypophosphatemia due to reduced renal tubular phosphate reabsorption developed during childhood. Eleven of 17 (65%) patients treated with bisphosphonates survived. Of 26 patients who survived their first day of life and were not treated with bisphosphonates only 8 (31%) patients survived beyond infancy. Forty different homozygous or compound heterozygous mutations, including 16 novel mutations inENPP1, were found in 41 (75%) of the 55 patients. Twenty-nine (71%) of these 41 patients died in infancy (median, 30 days). Seven of the 14 (50%) patients withoutENPP1mutations died in infancy (median, 9 days). When present on both alleles, the mutation p.P305T was associated with death in infancy in all 5 cases; otherwise, no clear genotype-phenotype correlation was seen.Conclusion—ENPP1coding region mutations are associated with generalized arterial calcification of infancy in ≈75% of subjects. Except for the p.P305T mutation, which was universally lethal when present on both alleles, the identifiedENPP1mutations per se have no discernable effect on survival. However, survival seems to be associated with hypophosphatemia linked with hyperphosphaturia and also with bisphosphonate treatment.

Published

2009

5. A novel mutation in LMBRD1 causes the cblF defect of vitamin B(12) metabolism in a Turkish patient

Author

Terttu Suormala, Frank Rutsch, Brian Fowler, Tanja Wittkampf, Julia B. Hennermann, Martin Stucki, Ayse Gül Malerczyk-Aktas, Peter Nürnberg, Mohammad R. Toliat, and Susann Gailus

Subjects

Lysosomal transport, Male, medicine.medical_specialty, Nucleocytoplasmic Transport Proteins, Turkey, Methylmalonic acid, medicine.disease_cause, Cobalamin, 5-Methyltetrahydrofolate-Homocysteine S-Methyltransferase, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Mutase, Internal medicine, Genetics, medicine, Humans, Cyanocobalamin, Methionine synthase, Homocysteine, Genetics (clinical), Alleles, 030304 developmental biology, 0303 health sciences, Mutation, biology, Methylmalonyl-CoA Mutase, Fibroblasts, 3. Good health, B vitamins, Vitamin B 12, Endocrinology, chemistry, biology.protein, Female, Lysosomes, 030217 neurology & neurosurgery, Methylmalonic Acid

Abstract

In the cblF defect of vitamin B(12) (cobalamin) metabolism, cobalamin is trapped in lysosomes. Consequently, cobalamin coenzyme synthesis is blocked, and cofactors for methionine synthase and methylmalonyl-coenzyme A (CoA) mutase are deficient. We recently identified LMBRD1 as the causative gene located on chromosome 6q13 and showed that 18 out of 24 alleles in unrelated patients carried the deletion c.1056delG (p.L352fsX18) (Rutsch et al. (Nat Genet 41:234-239, 2009). LMBRD1 encodes the lysosomal membrane protein LMBD1, which presumably facilitates lysosomal cobalamin export. Our patient is the second child of consanguineous Turkish parents. He presented on the second day of life with cerebral seizures due to intraventricular hemorrhage. Plasma homocysteine and urinary methylmalonic acid levels were elevated, and serum cobalamin level was decreased. Synthesis of both cobalamin coenzymes was deficient in cultured skin fibroblasts. The cblF defect was confirmed by somatic complementation analysis. Sequencing of LMBRD1 revealed the novel deletion c.1405delG (p.D469fsX38) on both alleles. Real-time polymerase chain reaction (PCR) revealed reduced messenger RNA (mRNA) levels in patient fibroblasts compared with controls. Transfection of patient fibroblasts with the LMBD1 wild-type complement DNA (cDNA) rescued coenzyme synthesis and function, confirming this new deletion as an additional cause of the cblF defect. This case adds to the spectrum of clinical presentations and mutations of this rare disorder of lysosomal transport.

Published

2009

6. Identification of a putative lysosomal cobalamin exporter altered in the cblF defect of vitamin B12 metabolism

Author

Corinne Sagné, Horst Robenek, Azita Sharifi, Thorsten Marquardt, Mohammad R. Toliat, Martin Stucki, Tanja Wittkampf, Christian Becker, Peter Nürnberg, Frank Rutsch, Terttu Suormala, David S. Rosenblatt, Wolfgang Höhne, Matthias R. Baumgartner, Insa Buers, Brian Fowler, Susann Gailus, Isabelle R. Miousse, Gudrun Nürnberg, Bruno Gasnier, Department of General Pediatrics, Münster University Children Hospital, Biologie cellulaire et moléculaire de la sécrétion (BCMS), Centre National de la Recherche Scientifique (CNRS), University of Zurich, and Rutsch, F

Subjects

Male, Nucleocytoplasmic Transport Proteins, MESH: Vitamin B 12 Deficiency, MESH: Membrane Transport Proteins, chemistry.chemical_compound, 0302 clinical medicine, MESH: Child, MESH: Proteins, Tissue Distribution, Cyanocobalamin, Child, chemistry.chemical_classification, 0303 health sciences, MESH: Nucleocytoplasmic Transport Proteins, Chromosome Mapping, Amino acid, Vitamin B 12, MESH: Hyperhomocysteinemia, Biochemistry, MESH: Transcobalamins, Chromosomes, Human, Pair 6, Female, Chromosome Deletion, MESH: Chromosomes, Human, Pair 6, MESH: Lysosome-Associated Membrane Glycoproteins, MESH: Chromosome Deletion, MESH: Methylmalonic Acid, Hyperhomocysteinemia, 610 Medicine & health, Biology, Cobalamin, Frameshift mutation, 03 medical and health sciences, 1311 Genetics, MESH: Polymorphism, Genetic, Genetics, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Vitamin B12, MESH: Tissue Distribution, 030304 developmental biology, Transcobalamins, MESH: Humans, Polymorphism, Genetic, Methionine, Lysosome-Associated Membrane Glycoproteins, Membrane Transport Proteins, Proteins, Vitamin B 12 Deficiency, Metabolism, MESH: Male, MESH: Hela Cells, B vitamins, MESH: Vitamin B 12, chemistry, 10036 Medical Clinic, MESH: Chromosome Mapping, MESH: Female, 030217 neurology & neurosurgery, HeLa Cells, Methylmalonic Acid

Abstract

International audience; Vitamin B(12) (cobalamin) is essential in animals for metabolism of branched chain amino acids and odd chain fatty acids, and for remethylation of homocysteine to methionine. In the cblF inborn error of vitamin B(12) metabolism, free vitamin accumulates in lysosomes, thus hindering its conversion to cofactors. Using homozygosity mapping in 12 unrelated cblF individuals and microcell-mediated chromosome transfer, we identified a candidate gene on chromosome 6q13, LMBRD1, encoding LMBD1, a lysosomal membrane protein with homology to lipocalin membrane receptor LIMR. We identified five different frameshift mutations in LMBRD1 resulting in loss of LMBD1 function, with 18 of the 24 disease chromosomes carrying the same mutation embedded in a common 1.34-Mb haplotype. Transfection of fibroblasts of individuals with cblF with wild-type LMBD1 rescued cobalamin coenzyme synthesis and function. This work identifies LMBRD1 as the gene underlying the cblF defect of cobalamin metabolism and suggests that LMBD1 is a lysosomal membrane exporter for cobalamin.

Published

2009

7. 118. Identification of a novel lysosomal membrane protein mutated in the Cbl F defect of vitamin B12 metabolism

Author

Tanja Wittkampf, Peter Nuernberg, Susann Gailus, Bruno Gasnier, Horst Robenek, Thorsten Marquardt, Isabelle Racine-Miousse, David S. Rosenblatt, Terttu Suormala, Frank Rutsch, Corinne Sagné, Brian Fowler, and Wolfgang Hoehne

Subjects

Lysosomal membrane, Vesicle-associated membrane protein 8, Endocrinology, Biochemistry, Chemistry, Endocrinology, Diabetes and Metabolism, Genetics, Identification (biology), Metabolism, Vitamin B12, Molecular Biology, Cell biology

Published

2009