Your search keyword '"Gal, Andreas"' showing total 94 results

1. Founder effect of Fabry disease due to p.F113L mutation: Clinical profile of a late-onset phenotype.

Author

Azevedo O, Gal A, Faria R, Gaspar P, Miltenberger-Miltenyi G, Gago MF, Dias F, Martins A, Rodrigues J, Reimão P, Pereira O, Simões S, Lopes E, Guimarães MJ, Sousa N, and Cunha D

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Cardiomyopathy, Hypertrophic complications, Cohort Studies, Female, Humans, Late Onset Disorders, Male, Middle Aged, Portugal, Young Adult, Fabry Disease genetics, Founder Effect, Mutation, Phenotype, alpha-Galactosidase genetics

Abstract

Background: Knowledge on clinical profiles of late-onset phenotypes of Fabry disease (FD) is essential to better define their natural history. Our study aims to demonstrate a founder effect of FD due to the GLA gene mutation c.337T>C (p.F113L) in the Portuguese region of Guimarães; and to characterize the clinical profile of this late-onset phenotype in a large cohort of genetically related adult patients, living in the same region., Methods and Results: FD screening was performed in 150 adult patients with hypertrophic cardiomyopathy (HCM) and found 25 Fabry patients (16.6%). The p.F113L mutation was found in 21 of them, leading to a genealogy study and haplotype analysis of the p.F113L patients. Genealogy research revealed a 12-generation family tree with a common ancestor to p.F113L patients, suggesting a founder effect that was supported by haplotype findings. Pedigree analysis was performed and 120 consecutive p.F113L patients underwent a predefined diagnostic evaluation of FD multiorgan involvement. This late-onset phenotype was characterized by common and/or potentially severe cardiac manifestations (left ventricular hypertrophy 40.8%, atrial fibrillation 5%, non-sustained ventricular tachycardia 12.5%, atrioventricular block 18.3%, bifascicular block 13.4%). Extracardiac manifestations included albuminuria>30 mg/24 h 36.1%, chronic kidney disease≥G3 7.6%, brain white matter lesions 54.4%, stroke 3.3%, sensorineural deafness 44.5%, cornea verticillata 13.9%. Plasma lyso-GB3 was undetectable in females, regardless of clinical manifestations., Conclusion: A founder effect of FD due to p.F113L mutation was documented by genealogy and genetics in a Portuguese region. In this late-onset phenotype, although cardiac manifestations carry the highest prognostic impact, extracardiac involvement is common., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

2. A novel stop mutation (p.(Gln22*)) of DAX1 (NR0B1) results in late-onset X-linked adrenal hypoplasia congenita.

Author

Gerards J, Ritter MM, Kaminsky E, Gal A, Hoeppner W, and Quinkler M

Abstract

DAX1 (NR0B1) is an orphan nuclear receptor, which plays an important role in development and function of the adrenal glands and gonads. Mutations in DAX1 cause X-linked adrenal hypoplasia congenita (X-linked AHC), which is characterized by adrenal insufficiency (AI) and hypogonadotropic hypogonadism (HHG). Affected boys present with adrenal failure usually in childhood and, later in life, with delayed puberty. However, patients with a late-onset form of X-linked AHC have also been described in the past years. We report a male patient who presented with symptoms of an adrenal crisis at the age of 38 years and was later diagnosed with HHG. Family history was positive with several male relatives diagnosed with AI and compatible with the assumed X-chromosomal inheritance of the trait. Direct sequencing of DAX1 of the patient revealed a hemizygous cytosine-to-thymine substitution at nucleotide 64 in exon 1, which creates a novel nonsense mutation (p.(Gln22*)). In order to compare the clinical presentation of the patient to that of other patients with X-linked AHC, we searched the electronic database MEDLINE (PubMed) and found reports of nine other cases with delayed onset of X-linked AHC. In certain cases, genotype-phenotype correlation could be assumed., Learning Points: X-linked AHC is a rare disease characterized by primary AI and hypogonadotropic hypogonadism (HHG). The full-blown clinical picture is seen usually only in males with a typical onset in childhood.Patients with a late-onset form of X-linked AHC have also been described recently. Being aware of this late-onset form might help to reach an early diagnosis and prevent life-threatening adrenal crises.Adult men with primary AI of unknown etiology should be investigated for HHG. Detecting a DAX1 mutation may confirm the clinical diagnosis of late-onset X-linked AHC.In relatives of patients with genetically confirmed X-linked AHC, targeted mutation analysis may help to identify family members at risk and asymptomatic carriers, and discuss conscious family planning.

Published

2017

3. Clinical utility gene card for: Fabry disease - update 2016.

Author

Gal A, Beck M, Höppner W, and Germain DP

Subjects

Fabry Disease diagnosis, Fabry Disease epidemiology, Genetic Testing standards, Humans, Fabry Disease genetics, Genetic Testing methods, alpha-Galactosidase genetics

Published

2017

4. Mutational analysis of the GLA gene in Mexican families with Fabry disease.

Author

Gutiérrez-Amavizca BE, Gal A, Ortíz-Orozco R, Orth U, Prado Montes De Oca E, Gutiérrez-Amavizca JP, and Figuera LE

Subjects

DNA Mutational Analysis, Fabry Disease diagnosis, Female, Genotype, Humans, Male, Mexico, Microsatellite Repeats, Pedigree, Phenotype, Fabry Disease genetics, Mutation, alpha-Galactosidase genetics

Abstract

Fabry disease (FD) is a lysosomal storage disorder, which develops due to a deficiency in the hydrolytic enzyme, α-galactosidase A (α-Gal A). Alpha-Gal A hydrolyzes glycosphingolipid globotriaosylceramide (Gb3), and an α-Gal A deficiency leads to Gb3 accumulation in tissues and cells in the body. This pathology is likely to involve multiple systems, but it is generally considered to affect primarily vascular endothelium. In this study, we investigated mutations in the GLA gene, which encodes α-Gal A, in Mexican families with FD. We included seven probands with FD that carried known mutations. We analysed pedigrees of the probands, and performed molecular screening in 65 relatives with the potential of carrying a GLA mutation. Five mutations (P40S, IVS4 +4 , G328V, R363H, R404del) were detected in seven unrelated Mexican families with the classic FD phenotype. Of the 65 relatives examined, 42 (64.6%) had a GLA gene mutation. In summary, among seven Mexican probands with FD, 65 relatives were at risk of carrying a known GLA mutation, and molecular screening identified 42 individuals with the mutation. Thus, our findings showed that it is important to perform molecular analysis in families with FD to detect mutations and to provide accurate diagnoses for individuals that could be affected.

Published

2017

5. EGFRvIII does not affect radiosensitivity with or without gefitinib treatment in glioblastoma cells.

Author

Struve N, Riedel M, Schulte A, Rieckmann T, Grob TJ, Gal A, Rothkamm K, Lamszus K, Petersen C, Dikomey E, and Kriegs M

Subjects

Antineoplastic Agents therapeutic use, Brain Neoplasms metabolism, Cell Cycle, Cell Line, Tumor, Cell Proliferation, Cell Separation, Cell Survival, DNA Breaks, Double-Stranded, DNA Repair, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Flow Cytometry, Gefitinib, Glioblastoma metabolism, Humans, Microscopy, Fluorescence, Radiation Tolerance, Signal Transduction, X-Rays, Brain Neoplasms drug therapy, Brain Neoplasms radiotherapy, ErbB Receptors metabolism, Gene Expression Regulation, Neoplastic, Glioblastoma drug therapy, Glioblastoma radiotherapy, Quinazolines therapeutic use

Abstract

Background: Glioblastomas (GBM) are often characterized by an elevated expression of the epidermal growth factor receptor variant III (EGFRvIII). We used GBM cell lines with native EGFRvIII expression to determine whether this EGFR variant affects radiosensitivity with or without EGFR targeting., Methods: Experiments were performed with GBM cell lines lacking (LN229, U87MG, U251, CAS-1) or endogenously expressing EGFRvIII (BS153, DKMG). The two latter cell lines were also used to establish sublines with a low (-) or a high proportion (+) of cells expressing EGFRvIII. EGFR signaling and the cell cycle were analyzed using Western blot and flow cytometry; cell survival was assessed by colony forming assay and double-strand break repair capacity by immunofluorescence., Results: DKMG and BS153 parental cells with heterogeneous EGFRvIII expression were clearly more radiosensitive compared to other GBM cell lines without EGFRvIII expression. However, no significant difference was observed in cell proliferation, clonogenicity or radiosensitivity between the EGFRvIII- and + sublines derived from DKMG and BS153 parental cells. Expression of EGFRvIII was associated with decreased DSB repair capacity for BS153 but not for DKMG cells. The effects of EGFR targeting by gefitinib alone or in combination with irradiation were also found not to depend on EGFRvIII expression. Gefitinib was only observed to influence the proliferation of EGFRvIII- BS153 cells., Conclusion: The data indicate that EGFRvIII does not alter radiosensitivity with or without anti-EGFR treatment.

Published

2015

6. Radiosensitization of NSCLC cells by EGFR inhibition is the result of an enhanced p53-dependent G1 arrest.

Author

Kriegs M, Gurtner K, Can Y, Brammer I, Rieckmann T, Oertel R, Wysocki M, Dorniok F, Gal A, Grob TJ, Laban S, Kasten-Pisula U, Petersen C, Baumann M, Krause M, and Dikomey E

Subjects

Animals, Antibodies, Monoclonal, Humanized pharmacology, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung radiotherapy, Cell Division, Cell Line, Tumor, Cetuximab, Erlotinib Hydrochloride, G1 Phase Cell Cycle Checkpoints radiation effects, Humans, Lung Neoplasms drug therapy, Lung Neoplasms radiotherapy, Mice, Mice, Nude, Quinazolines pharmacology, RNA, Small Interfering genetics, Radiation Tolerance genetics, Signal Transduction drug effects, Signal Transduction radiation effects, Xenograft Model Antitumor Assays, Carcinoma, Non-Small-Cell Lung pathology, ErbB Receptors antagonists & inhibitors, G1 Phase Cell Cycle Checkpoints drug effects, Lung Neoplasms pathology, Tumor Suppressor Protein p53 metabolism

Abstract

Purpose: How EGF receptor (EGFR) inhibition induces cellular radiosensitization and with that increase in tumor control is still a matter of discussion. Since EGFR predominantly regulates cell cycle and proliferation, we studied whether a G1-arrest caused by EGFR inhibition may contribute to these effects., Materials and Methods: We analyzed human non-small cell lung cancer (NSCLC) cell lines either wild type (wt) or mutated in p53 (A549, H460, vs. H1299, H3122) and HCT116 cells (p21 wt and negative). EGFR was inhibited by BIBX1382BS, erlotinib or cetuximab; p21 was knocked down by siRNA. Functional endpoints analyzed were cell signaling, proliferation, G1-arrest, cell survival as well as tumor control using an A549 tumor model., Results: When combined with IR, EGFR inhibition enhances the radiation-induced permanent G1 arrest, though solely in cells with intact p53/p21 signaling. This increase in G1-arrest was always associated with enhanced cellular radiosensitivity. Strikingly, this effect was abrogated when cells were re-stimulated, suggesting the initiation of dormancy. In line with this, only a small non-significant increase in tumor control was observed for A549 tumors treated with fractionated RT and EGFR inhibition., Conclusion: For NSCLC cells increase in radiosensitivity by EGFR inhibition results from enhanced G1-arrest. However, this effect does not lead to improved tumor control because cells can be released from this arrest by re-stimulation., (Copyright © 2015 Elsevier Ireland Ltd. All rights reserved.)

Published

2015

7. Ocular signs correlate well with disease severity and genotype in Fabry disease.

Author

Pitz S, Kalkum G, Arash L, Karabul N, Sodi A, Larroque S, Beck M, and Gal A

Subjects

Adolescent, Adult, Child, Fabry Disease pathology, Female, Humans, Male, Middle Aged, Mutation, Missense, Severity of Illness Index, Cornea pathology, Fabry Disease genetics, Genotype

Abstract

Ocular signs in Fabry disease have generally been regarded to be primarily of diagnostic value. We explored whether ocular findings, alone or in particular in combination with the α-galactosidase A gene mutation, have predictive value for disease severity. Data from the Fabry Outcome Survey (FOS), a large, global database sponsored by Shire, were selected for adult patients who had undergone ophthalmological examination. Three ocular signs were assessed: cornea verticillata, tortuous conjunctival and/or retinal vessels, and cataract. Fabry disease severity was measured using FOS Mainz Severity Score Index and modifications thereof. Ophthalmological data were available for 1203 (699 female, 504 male) adult patients with eye findings characteristic of Fabry disease in 55.1%. Cornea verticillata had a similar distribution in women (51.1%) and men (50.8%), whereas tortuous vessels and Fabry cataract were somewhat more frequent in men than in women. Patients with cornea verticillata, selected as the principal ocular sign for this study, had more severe disease (median score, 20.0) versus those without ocular signs (11.0; P<0.001). This finding could be confirmed by applying age adjusted severity scores. Moreover, the prevalence of cornea verticillata was significantly higher in patients with null (male, 76.9%; female, 64.5%) and missense (male, 79.2%; female, 67.4%) mutations versus mild missense (male, 17.1%; female, 23.1%) and the p.N215S (male, 15.0%; female, 15.6%) mutations (P<0.01). Our analyses show a correlation between the prevalence of ocular changes in Fabry disease and disease severity. Consequently, information on ocular findings and α-galactosidase A gene mutation may help assess the risk for more severe Fabry disease. These observed findings are of notable clinical importance, as Fabry disease is characterized by high clinical course variability and only weak genotype-phenotype correlation at the individual patient level. Further confirmatory studies are needed.

Published

2015

8. OSBPL2 encodes a protein of inner and outer hair cell stereocilia and is mutated in autosomal dominant hearing loss (DFNA67).

Author

Thoenes M, Zimmermann U, Ebermann I, Ptok M, Lewis MA, Thiele H, Morlot S, Hess MM, Gal A, Eisenberger T, Bergmann C, Nürnberg G, Nürnberg P, Steel KP, Knipper M, and Bolz HJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Animals, Child, Preschool, Female, Gene Expression Regulation, Genetic Linkage, Humans, Infant, Male, Mice, MicroRNAs genetics, MicroRNAs metabolism, Middle Aged, Pedigree, RNA, Messenger genetics, RNA, Messenger metabolism, Receptors, Steroid genetics, Young Adult, Deafness genetics, Hair Cells, Auditory metabolism, Receptors, Steroid metabolism, Stereocilia metabolism

Abstract

Background: Early-onset hearing loss is mostly of genetic origin. The complexity of the hearing process is reflected by its extensive genetic heterogeneity, with probably many causative genes remaining to be identified. Here, we aimed at identifying the genetic basis for autosomal dominant non-syndromic hearing loss (ADNSHL) in a large German family., Methods: A panel of 66 known deafness genes was analyzed for mutations by next-generation sequencing (NGS) in the index patient. We then conducted genome-wide linkage analysis, and whole-exome sequencing was carried out with samples of two patients. Expression of Osbpl2 in the mouse cochlea was determined by immunohistochemistry. Because Osbpl2 has been proposed as a target of miR-96, we investigated homozygous Mir96 mutant mice for its upregulation., Results: Onset of hearing loss in the investigated ADNSHL family is in childhood, initially affecting the high frequencies and progressing to profound deafness in adulthood. However, there is considerable intrafamilial variability. We mapped a novel ADNSHL locus, DFNA67, to chromosome 20q13.2-q13.33, and subsequently identified a co-segregating heterozygous frameshift mutation, c.141&#95;142delTG (p.Arg50Alafs*103), in OSBPL2, encoding a protein known to interact with the DFNA1 protein, DIAPH1. In mice, Osbpl2 was prominently expressed in stereocilia of cochlear outer and inner hair cells. We found no significant Osbpl2 upregulation at the mRNA level in homozygous Mir96 mutant mice., Conclusion: The function of OSBPL2 in the hearing process remains to be determined. Our study and the recent description of another frameshift mutation in a Chinese ADNSHL family identify OSBPL2 as a novel gene for progressive deafness.

Published

2015

9. Dried blood spots allow targeted screening to diagnose mucopolysaccharidosis and mucolipidosis.

Author

Cobos PN, Steglich C, Santer R, Lukacs Z, and Gal A

Abstract

Background: As patients with different types of mucopolysaccharidosis (MPS) and mucolipidosis (ML) may present with overlapping clinical features - including coarse face, hepatosplenomegaly, bone dysplasia and claw-hand deformities, collectively also called 'MPS-like phenotype', enzymatic and/or molecular genetic analyses are indispensable for accurate diagnosis and applying specific therapy. In this prospective study, we screened patients with symptoms compatible with MPS for MPS I, II (males) and VI., Methods: Dried blood spots/specimens (DBS) were collected from 200 patients with an MPS-like phenotype and analysed for activities of α-iduronidase (IDUA), iduronate-2-sulphatase (IDS), and arylsulphatase B (ARSB), the enzymes deficient in mucopolysaccharidosis (MPS) type I, II and VI, respectively. For the samples with pathologic enzyme activity, mutational analysis was carried out using the same DBS., Results: Based on enzymatic analysis of 200 DBS samples, a total of 45 (22.5%) showed low activity; 17 for MPS I (8.5%), 11 for MPS II (5.5%) and 9 for MPS VI (4.5%). Enzyme activities were suggestive for ML II/III in 8 (4.0%) cases. For 41 (91.1%) samples, DNA could be extracted from the filter paper. Mutations were identified in 11 (64.7%), 11 (100%), 9 (100%) and 5 (62.5%) patients putatively diagnosed biochemically with MPS I, II, VI, and ML II/III, respectively., Conclusions: DBS enzymatic analysis can be used to diagnose MPS/ML. Initial results should be confirmed by a second enzyme assay and/or by molecular genetic testing. Given the advantages of DBS over other sample types in terms of ease of collection, storage and transportation, DBS are particularly useful for screening patients with an MPS-like phenotype in regions lacking specialised laboratories. In order to ascertain the diagnosis in a large number of cases, patients should be assessed in parallel for at least MPS I, II and VI.

Published

2015

10. Identification of a PRPF4 loss-of-function variant that abrogates U4/U6.U5 tri-snRNP integration and is associated with retinitis pigmentosa.

Author

Linder B, Hirmer A, Gal A, Rüther K, Bolz HJ, Winkler C, Laggerbauer B, and Fischer U

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Western, Embryo, Nonmammalian metabolism, Gangliosides metabolism, Gene Components, HEK293 Cells, Humans, Molecular Sequence Data, Nuclear Proteins metabolism, Pedigree, Ribonucleoprotein, U4-U6 Small Nuclear metabolism, Sequence Analysis, DNA, Spliceosomes metabolism, Zebrafish, Mutation, Missense genetics, Retinitis Pigmentosa genetics, Ribonucleoprotein, U4-U6 Small Nuclear genetics, Spliceosomes genetics

Abstract

Pre-mRNA splicing by the spliceosome is an essential step in the maturation of nearly all human mRNAs. Mutations in six spliceosomal proteins, PRPF3, PRPF4, PRPF6, PRPF8, PRPF31 and SNRNP200, cause retinitis pigmentosa (RP), a disease characterized by progressive photoreceptor degeneration. All splicing factors linked to RP are constituents of the U4/U6.U5 tri-snRNP subunit of the spliceosome, suggesting that the compromised function of this particle may lead to RP. Here, we report the identification of the p.R192H variant of the tri-snRNP factor PRPF4 in a patient with RP. The mutation affects a highly conserved arginine residue that is crucial for PRPF4 function. Introduction of a corresponding mutation into the zebrafish homolog of PRPF4 resulted in a complete loss of function in vivo. A series of biochemical experiments suggested that p.R192H disrupts the binding interface between PRPF4 and its interactor PRPF3. This interferes with the ability of PRPF4 to integrate into the tri-snRNP, as shown in a human cell line and in zebrafish embryos. These data suggest that the p.R192H variant of PRPF4 represents a functional null allele. The resulting haploinsufficiency of PRPF4 compromises the function of the tri-snRNP, reinforcing the notion that this spliceosomal particle is of crucial importance in the physiology of the retina.

Published

2014

11. Sensory neuropathy with bone destruction due to a mutation in the membrane-shaping atlastin GTPase 3.

Author

Kornak U, Mademan I, Schinke M, Voigt M, Krawitz P, Hecht J, Barvencik F, Schinke T, Gießelmann S, Beil FT, Pou-Serradell A, Vílchez JJ, Beetz C, Deconinck T, Timmerman V, Kaether C, De Jonghe P, Hübner CA, Gal A, Amling M, Mundlos S, Baets J, and Kurth I

Subjects

Adult, Age of Onset, Bone Diseases etiology, Bone Diseases physiopathology, Cohort Studies, Cough genetics, Cough pathology, Cough physiopathology, Endoplasmic Reticulum pathology, Exome genetics, Female, Fractures, Bone genetics, Fractures, Bone pathology, Gastroesophageal Reflux genetics, Gastroesophageal Reflux pathology, Gastroesophageal Reflux physiopathology, Genes, Dominant genetics, Haplotypes genetics, Hereditary Sensory and Autonomic Neuropathies complications, Hereditary Sensory and Autonomic Neuropathies pathology, Hereditary Sensory and Autonomic Neuropathies physiopathology, Humans, Intracellular Space genetics, Male, Mutation, Mutation, Missense genetics, Pedigree, Phenotype, Young Adult, Bone Diseases genetics, Endoplasmic Reticulum genetics, GTP Phosphohydrolases genetics, Hereditary Sensory and Autonomic Neuropathies genetics

Abstract

Many neurodegenerative disorders present with sensory loss. In the group of hereditary sensory and autonomic neuropathies loss of nociception is one of the disease hallmarks. To determine underlying factors of sensory neurodegeneration we performed whole-exome sequencing in affected individuals with the disorder. In a family with sensory neuropathy with loss of pain perception and destruction of the pedal skeleton we report a missense mutation in a highly conserved amino acid residue of atlastin GTPase 3 (ATL3), an endoplasmic reticulum-shaping GTPase. The same mutation (p.Tyr192Cys) was identified in a second family with similar clinical outcome by screening a large cohort of 115 patients with hereditary sensory and autonomic neuropathies. Both families show an autosomal dominant pattern of inheritance and the mutation segregates with complete penetrance. ATL3 is a paralogue of ATL1, a membrane curvature-generating molecule that is involved in spastic paraplegia and hereditary sensory neuropathy. ATL3 proteins are enriched in three-way junctions, branch points of the endoplasmic reticulum that connect membranous tubules to a continuous network. Mutant ATL3 p.Tyr192Cys fails to localize to branch points, but instead disrupts the structure of the tubular endoplasmic reticulum, suggesting that the mutation exerts a dominant-negative effect. Identification of ATL3 as novel disease-associated gene exemplifies that long-term sensory neuronal maintenance critically depends on the structural organisation of the endoplasmic reticulum. It emphasizes that alterations in membrane shaping-proteins are one of the major emerging pathways in axonal degeneration and suggests that this group of molecules should be considered in neuroprotective strategies.

Published

2014

12. Increasing the yield in targeted next-generation sequencing by implicating CNV analysis, non-coding exons and the overall variant load: the example of retinal dystrophies.

Author

Eisenberger T, Neuhaus C, Khan AO, Decker C, Preising MN, Friedburg C, Bieg A, Gliem M, Charbel Issa P, Holz FG, Baig SM, Hellenbroich Y, Galvez A, Platzer K, Wollnik B, Laddach N, Ghaffari SR, Rafati M, Botzenhart E, Tinschert S, Börger D, Bohring A, Schreml J, Körtge-Jung S, Schell-Apacik C, Bakur K, Al-Aama JY, Neuhann T, Herkenrath P, Nürnberg G, Nürnberg P, Davis JS, Gal A, Bergmann C, Lorenz B, and Bolz HJ

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Heterozygote, Humans, Male, Middle Aged, Mutation, Pedigree, Retinal Dystrophies diagnosis, Young Adult, DNA Copy Number Variations, Exons genetics, High-Throughput Nucleotide Sequencing, Retinal Dystrophies genetics, Sequence Analysis, DNA

Abstract

Retinitis pigmentosa (RP) and Leber congenital amaurosis (LCA) are major causes of blindness. They result from mutations in many genes which has long hampered comprehensive genetic analysis. Recently, targeted next-generation sequencing (NGS) has proven useful to overcome this limitation. To uncover "hidden mutations" such as copy number variations (CNVs) and mutations in non-coding regions, we extended the use of NGS data by quantitative readout for the exons of 55 RP and LCA genes in 126 patients, and by including non-coding 5' exons. We detected several causative CNVs which were key to the diagnosis in hitherto unsolved constellations, e.g. hemizygous point mutations in consanguineous families, and CNVs complemented apparently monoallelic recessive alleles. Mutations of non-coding exon 1 of EYS revealed its contribution to disease. In view of the high carrier frequency for retinal disease gene mutations in the general population, we considered the overall variant load in each patient to assess if a mutation was causative or reflected accidental carriership in patients with mutations in several genes or with single recessive alleles. For example, truncating mutations in RP1, a gene implicated in both recessive and dominant RP, were causative in biallelic constellations, unrelated to disease when heterozygous on a biallelic mutation background of another gene, or even non-pathogenic if close to the C-terminus. Patients with mutations in several loci were common, but without evidence for di- or oligogenic inheritance. Although the number of targeted genes was low compared to previous studies, the mutation detection rate was highest (70%) which likely results from completeness and depth of coverage, and quantitative data analysis. CNV analysis should routinely be applied in targeted NGS, and mutations in non-coding exons give reason to systematically include 5'-UTRs in disease gene or exome panels. Consideration of all variants is indispensable because even truncating mutations may be misleading.

Published

2013

13. Sorafenib sensitizes head and neck squamous cell carcinoma cells to ionizing radiation.

Author

Laban S, Steinmeister L, Gleißner L, Grob TJ, Grénman R, Petersen C, Gal A, Knecht R, Dikomey E, and Kriegs M

Subjects

Carcinoma, Squamous Cell pathology, Cell Line, Tumor, DNA Repair, Head and Neck Neoplasms pathology, Humans, Niacinamide therapeutic use, Sorafenib, Squamous Cell Carcinoma of Head and Neck, Carcinoma, Squamous Cell radiotherapy, Head and Neck Neoplasms radiotherapy, Niacinamide analogs & derivatives, Phenylurea Compounds therapeutic use, Radiation-Sensitizing Agents therapeutic use, raf Kinases antagonists & inhibitors

Abstract

Background and Purpose: There is a great need to improve the outcome of locoregionally advanced squamous cell carcinomas of the head and neck (HNSCC). Standard treatment includes a combination of surgery, radio- and chemotherapy. The addition of molecular targeting agents to conventional treatment may improve outcomes. In this study the Raf inhibitor sorafenib was used to increase the radiosensitivity of HNSCC cell lines., Material and Methods: In a panel of six cell lines (A549, FaDu, UTSCC 60A, UTSCC 42A, UTSCC 42B, UTSCC 29) radiosensitivity was measured by colony formation assay and apoptosis and cell cycle analysis were performed by flow cytometry. DNA repair was analyzed by 53BP1 immunohistochemistry., Results: Sorafenib added prior to irradiation resulted in an increased cellular radiosensitivity (DEF0.5=1.11-1.84). Radiosensitization was not caused by an enhanced rate of apoptosis or cell cycle effects. In contrast, sorafenib was shown for the first time to block the repair of DNA double-strand breaks (DSB)., Conclusion: Our data suggest that sorafenib may be used to overcome the radioresistance of HNSCC through the inhibition of DSB repair., (Copyright © 2013 Elsevier Ireland Ltd. All rights reserved.)

Published

2013

14. Mucopolysaccharidosis type II in a female carrying a heterozygous stop mutation of the iduronate-2-sulfatase gene and showing a skewed X chromosome inactivation.

Author

Piña-Aguilar RE, Zaragoza-Arévalo GR, Rau I, Gal A, Alcántara-Ortigoza MA, López-Martínez MS, and Santillán-Hernández Y

Subjects

Child, Preschool, Exons, Female, Humans, Receptors, Androgen genetics, Heterozygote, Iduronate Sulfatase genetics, Mucopolysaccharidosis II diagnosis, Mucopolysaccharidosis II genetics, Mutation, X Chromosome Inactivation genetics

Abstract

We report a Mexican girl showing the full blown clinical picture of mucopolysaccharidosis type II (MPSII). Iduronate-2-sulfatase (IDS) activity was low and she carried a heterozygous de novo c.1327C>T transition in exon 9, that changes codon 443 for a premature stop (TGA; p.Arg443(*)). Analysis of X-chromosome inactivation in androgen receptor (AR) locus showed a highly skewed ratio of 92:8 suggesting a functional hemizygosity with dominant expression of the mutant IDS and explaining the disease manifestation. This is one of the rare cases of females affected by MPSII due to the combined effect of a skewed X-chromosome inactivation and a de novo IDS mutation. We recommend that clinicians should consider the diagnosis of MPSII even in a girl without positive family history for this condition., (Copyright © 2012 Elsevier Masson SAS. All rights reserved.)

Published

2013

15. A high-throughput resequencing microarray for autosomal dominant spastic paraplegia genes.

Author

Dufke C, Schlipf N, Schüle R, Bonin M, Auer-Grumbach M, Stevanin G, Depienne C, Kassubek J, Klebe S, Klimpe S, Klopstock T, Otto S, Poths S, Seibel A, Stolze H, Gal A, Schöls L, and Bauer P

Subjects

Codon, Nonsense, Cohort Studies, Computational Biology methods, Exons, Genotype, Humans, Mutation, Mutation, Missense, Reproducibility of Results, Sensitivity and Specificity, Oligonucleotide Array Sequence Analysis methods, Polymorphism, Single Nucleotide, Sequence Analysis, DNA, Spastic Paraplegia, Hereditary genetics

Abstract

Hereditary spastic paraplegias (HSP) are a heterogeneous group of neurological disorders. Insidiously progressive spastic weakness of the lower extremities is the common criterion in all forms described. Clinically, HSP is differentiated into pure (uncomplicated) and complex (complicated) forms. While pure HSP is predominantly characterized by signs and symptoms of pyramidal tract dysfunction, additional neurological and non-neurological symptoms occur in complicated forms. Autosomal dominant, autosomal recessive, and X-linked modes of inheritance have been described and at least 48 subtypes, termed SPG1-48, have been genetically defined. Although in autosomal dominant HSP families 50-60% of etiologies can be established by genetic testing, genotype predictions based on the phenotype are limited. In order to realize high-throughput genotyping for dominant HSP, we designed a resequencing microarray for six autosomal dominant genes on the Affymetrix CustomSEQ array platform. For validation purposes, 10 previously Sanger sequenced patients with autosomal dominant HSP and 40 positive controls with known mutations in ATL1, SPAST, NIPA1, KIF5A, and BSCL2 (32 base exchanges, eight small indels) were resequenced on this array. DNA samples of 45 additional patients with AD spastic paraplegia were included in the study. With two different sequencing analysis software modules (GSEQ, SeqC), all missense/nonsense mutations in the positive controls were identified while indels had a detection rate of only 50%. In total, 244 common synonymous single-nucleotide polymorphisms (SNPs) annotated in dbSNP (build 132) corresponding to 22 distinct sequence variations were found in the 53 analyzed patients. Among the 22 different sequence variations (SPAST n = 15, ATL1 n = 3, KIF5A n = 2, HSPD1 n = 1, BSCL2 n = 1, NIPA1 n = 0), 12 were rare variants that have not been previously described and whose clinical significance is unknown. In SPAST-negative cases, a genetic diagnosis could be established in 11% by resequencing. Resequencing microarray technology can therefore efficiently be used to study genotypes and mutations in large patient cohorts.

Published

2012

16. Clinical utility gene card for: adrenoleukodystrophy.

Author

Krasemann E, Kemp S, and Gal A

Subjects

ATP Binding Cassette Transporter, Subfamily D, Member 1, Adrenoleukodystrophy diagnosis, Adrenoleukodystrophy epidemiology, Diagnosis, Differential, Genetic Testing, Humans, Prevalence, Sensitivity and Specificity, ATP-Binding Cassette Transporters genetics, Adrenoleukodystrophy genetics, Mutation

Published

2012

17. Clinical utility gene card for: Fabry disease.

Author

Gal A, Beck M, and Winchester B

Subjects

Fabry Disease diagnosis, Genetic Testing methods, Humans, Mutation, Sensitivity and Specificity, Fabry Disease genetics, alpha-Galactosidase genetics

Published

2012

18. Clinical utility gene card for: mucopolysaccharidosis type II.

Author

Beck M, Wijburg FA, and Gal A

Subjects

Diagnosis, Differential, Female, Genotype, Humans, Male, Mucopolysaccharidosis II epidemiology, Mucopolysaccharidosis II genetics, Point Mutation, Prevalence, Sensitivity and Specificity, Genetic Testing methods, Glycoproteins genetics, Mucopolysaccharidosis II diagnosis

Published

2012

19. Ccdc66 null mutation causes retinal degeneration and dysfunction.

Author

Gerding WM, Schreiber S, Schulte-Middelmann T, de Castro Marques A, Atorf J, Akkad DA, Dekomien G, Kremers J, Dermietzel R, Gal A, Rülicke T, Ibrahim S, Epplen JT, and Petrasch-Parwez E

Subjects

Animals, Disease Models, Animal, Female, Gene Silencing, Humans, Male, Mice, Mice, Knockout, Retina metabolism, Retina pathology, Retina physiopathology, Retinal Degeneration metabolism, Retinal Degeneration pathology, Retinitis Pigmentosa metabolism, Retinitis Pigmentosa pathology, Eye Proteins genetics, Retinal Degeneration genetics, Retinal Degeneration physiopathology, Retinitis Pigmentosa genetics, Retinitis Pigmentosa physiopathology, Sequence Deletion

Abstract

Retinitis pigmentosa (RP) is a group of human retinal disorders, with more than 100 genes involved in retinal degeneration. Canine and murine models are useful for investigating human RP based on known, naturally occurring mutations. In Schapendoes dogs, for example, a mutation in the CCDC66 gene has been shown to cause autosomal recessively inherited, generalized progressive retinal atrophy (gPRA), the canine counterpart to RP. Here, a novel mouse model with a disrupted Ccdc66 gene was investigated to reveal the function of protein CCDC66 and the pathogenesis of this form of gPRA. Homozygous Ccdc66 mutant mice lack retinal Ccdc66 RNA and protein expression. Light and electron microscopy reveal an initial degeneration of photoreceptors already at 13 days of age, followed by a slow, progressive retinal degeneration over months. Retinal dysfunction causes reduced scotopic a-wave amplitudes, declining from 1 to 7 months of age as well as an early reduction of the photopic b-wave at 1 month, improving slightly at 7 months, as evidenced by electroretinography. In the retina of the wild-type (WT) mouse, protein CCDC66 is present at highest levels after birth, followed by a decline until adulthood, suggesting a crucial role in early development. Protein CCDC66 is expressed predominantly in the developing rod outer segments as confirmed by subcellular analyses. These findings illustrate that the lack of protein CCDC66 causes early, slow progressive rod-cone dysplasia in the novel Ccdc66 mutant mouse model, thus providing a sound foundation for the development of therapeutic strategies.

Published

2011

20. Residual activity and proteasomal degradation of p.Ser298Pro sulfamidase identified in patients with a mild clinical phenotype of Sanfilippo A syndrome.

Author

Muschol N, Pohl S, Meyer A, Gal A, Ullrich K, and Braulke T

Subjects

Adolescent, Adult, Amino Acid Substitution genetics, Animals, Cell Line, Child, Child, Preschool, Cricetinae, Enzyme Stability genetics, Female, Genetic Association Studies, Humans, Male, Mutation genetics, Young Adult, Hydrolases genetics, Hydrolases metabolism, Mucopolysaccharidosis III enzymology, Mucopolysaccharidosis III genetics, Phenotype, Proteasome Endopeptidase Complex metabolism

Abstract

Mucopolysaccharidosis type IIIA (MPS IIIA, Sanfilippo syndrome) is a fatal inherited lysosomal storage disease accompanied by progressive neurologic degeneration. The gene underlying MPS IIIA, SGSH, encodes a lysosomal enzyme, N-sulfoglucosamine sulfohydrolase (sulfamidase). Mutational analysis of a large cohort of MPS IIIA patients showed a correlation of the missense mutation p.Ser298Pro and a slowly progressive course of the disease. We report here on the expression of the mutant p.Ser298Pro sulfamidase in BHK cells retaining low residual activity. Pulse-chase experiments showed that rapid degradation is responsible for the low steady state level of the mutant protein. Processing and secretion of p.Ser298Pro sulfamidase suggests that small amounts of the newly synthesized enzyme are transported to lysosomes. Most of the mutant sulfamidase exits the endoplasmic reticulum for proteasomal degradation. The ability to predict the clinical course of MPS IIIA in patients with the p.Ser298Pro mutation, as well as the residual enzymatic activity, and the reduced stability of the mutant sulfamidase suggest that this subgroup of patients is especially well suited to early sulfamidase replacement therapy or treatment with selective pharmacological chaperones., (Copyright © 2011 Wiley-Liss, Inc.)

Published

2011

21. Nonsense mutations in SMPX, encoding a protein responsive to physical force, result in X-chromosomal hearing loss.

Author

Huebner AK, Gandia M, Frommolt P, Maak A, Wicklein EM, Thiele H, Altmüller J, Wagner F, Viñuela A, Aguirre LA, Moreno F, Maier H, Rau I, Giesselmann S, Nürnberg G, Gal A, Nürnberg P, Hübner CA, del Castillo I, and Kurth I

Subjects

Adolescent, Age of Onset, Alleles, Animals, Child, Child, Preschool, Cochlea, Ear, Inner embryology, Ear, Inner metabolism, Female, Genetic Linkage, Genome-Wide Association Study, Hair Cells, Auditory metabolism, Haplotypes, HeLa Cells, Humans, Male, Mice, Mice, Inbred C57BL, Pedigree, Chromosomes, Human, X genetics, Codon, Nonsense, Hearing Loss genetics, Muscle Proteins genetics

Abstract

The fact that hereditary hearing loss is the most common sensory disorder in humans is reflected by, among other things, an extraordinary allelic and nonallelic genetic heterogeneity. X-chromosomal hearing impairment represents only a minor fraction of all cases. In a study of a Spanish family the locus for one of the X-chromosomal forms was assigned to Xp22 (DFNX4). We mapped the disease locus in the same chromosomal region in a large German pedigree with X-chromosomal nonsyndromic hearing impairment by using genome-wide linkage analysis. Males presented with postlingual hearing loss and onset at ages 3-7, whereas onset in female carriers was in the second to third decades. Targeted DNA capture with high-throughput sequencing detected a nonsense mutation in the small muscle protein, X-linked (SMPX) of affected individuals. We identified another nonsense mutation in SMPX in patients from the Spanish family who were previously analyzed to map DFNX4. SMPX encodes an 88 amino acid, cytoskeleton-associated protein that is responsive to mechanical stress. The presence of Smpx in hair cells and supporting cells of the murine cochlea indicates its role in the inner ear. The nonsense mutations detected in the two families suggest a loss-of-function mechanism underlying this form of hearing impairment. Results obtained after heterologous overexpression of SMPX proteins were compatible with this assumption. Because responsivity to physical force is a characteristic feature of the protein, we propose that long-term maintenance of mechanically stressed inner-ear cells critically depends on SMPX function., (Copyright © 2011 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2011

22. Talipes equinovarus as leading symptom of congenital myotonic dystrophy type 2.

Author

Kruse B and Gal A

Subjects

Clubfoot complications, Congenital Abnormalities diagnosis, Humans, Myotonic Disorders complications, Myotonic Disorders diagnosis, Myotonic Dystrophy, Clubfoot diagnosis

Published

2011

23. Toward a consensus in the laboratory diagnostics of Fabry disease - recommendations of a European expert group.

Author

Gal A, Hughes DA, and Winchester B

Subjects

Consensus, Decision Support Techniques, Europe, Female, Humans, Male, Societies, Medical, alpha-Galactosidase blood, alpha-Galactosidase genetics, Clinical Laboratory Techniques standards, Fabry Disease blood, Fabry Disease diagnosis, Mutation

Published

2011

24. Autosomal-recessive posterior microphthalmos is caused by mutations in PRSS56, a gene encoding a trypsin-like serine protease.

Author

Gal A, Rau I, El Matri L, Kreienkamp HJ, Fehr S, Baklouti K, Chouchane I, Li Y, Rehbein M, Fuchs J, Fledelius HC, Vilhelmsen K, Schorderet DF, Munier FL, Ostergaard E, Thompson DA, and Rosenberg T

Subjects

Amino Acid Sequence, Animals, Base Sequence, DNA Mutational Analysis, Eye enzymology, Eye pathology, Family, Gene Expression Regulation, Enzymologic, Genetic Loci genetics, Humans, Meiosis genetics, Mice, Microphthalmos enzymology, Models, Molecular, Molecular Sequence Data, Serine Endopeptidases chemistry, Serine Endopeptidases metabolism, Serine Proteases chemistry, Serine Proteases metabolism, Genes, Recessive genetics, Microphthalmos genetics, Mutation genetics, Serine Endopeptidases genetics, Serine Proteases genetics

Abstract

Posterior microphthalmos (MCOP) is a rare isolated developmental anomaly of the eye characterized by extreme hyperopia due to short axial length. The population of the Faroe Islands shows a high prevalence of an autosomal-recessive form (arMCOP) of the disease. Based on published linkage data, we refined the position of the disease locus (MCOP6) in an interval of 250 kb in chromosome 2q37.1 in two large Faroese families. We detected three different mutations in PRSS56. Patients of the Faroese families were either homozygous for c.926G>C (p.Trp309Ser) or compound heterozygous for c.926G>C and c.526C>G (p.Arg176Gly), whereas a homozygous 1 bp duplication (c.1066dupC) was identified in five patients with arMCOP from a consanguineous Tunisian family. In one patient with MCOP from the Faroe Islands and in another one from Turkey, no PRSS56 mutation was detected, suggesting nonallelic heterogeneity of the trait. Using RT-PCR, PRSS56 transcripts were detected in samples derived from the human adult retina, cornea, sclera, and optic nerve. The expression of the mouse ortholog could be first detected in the eye at E17 and was maintained into adulthood. The predicted PRSS56 protein is a 603 amino acid long secreted trypsin-like serine peptidase. The c.1066dupC is likely to result in a functional null allele, whereas the two point mutations predict the replacement of evolutionary conserved and functionally important residues. Molecular modeling of the p.Trp309Ser mutant suggests that both the affinity and reactivity of the enzyme toward in vivo protein substrates are likely to be substantially reduced., (Copyright © 2011 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2011

25. Risk gene variants for nicotine dependence in the CHRNA5-CHRNA3-CHRNB4 cluster are associated with cognitive performance.

Author

Winterer G, Mittelstrass K, Giegling I, Lamina C, Fehr C, Brenner H, Breitling LP, Nitz B, Raum E, Müller H, Gallinat J, Gal A, Heim K, Prokisch H, Meitinger T, Hartmann AM, Möller HJ, Gieger C, Wichmann HE, Illig T, Dahmen N, and Rujescu D

Subjects

Adult, Aged, Chromosomes, Human, Pair 15 genetics, Female, Gene Expression, Gene Expression Profiling, Genetic Association Studies, Genetic Predisposition to Disease, Genetic Variation, Genotype, Humans, Male, Middle Aged, Multigene Family, Polymorphism, Single Nucleotide, RNA, Messenger blood, RNA, Messenger genetics, Risk, Wechsler Scales, Cognition, Nerve Tissue Proteins genetics, Receptors, Nicotinic genetics, Tobacco Use Disorder genetics

Abstract

Recent studies strongly support an association of the nicotinic acetylcholine receptor gene cluster CHRNA5-CHRNA3-CHRNB4 with nicotine dependence (ND). However, the precise genotype-phenotype relationship is still unknown. Clinical and epidemiological data on smoking behavior raise the possibility that the relevant gene variants may indirectly contribute to the development of ND by affecting cognitive performance in some smokers who consume nicotine for reasons of "cognition enhancement." Here, we tested seven single nucleotide polymorphisms (SNPs) rs684513, rs637137, rs16969968, rs578776, rs1051730, rs3743078, rs3813567 from the CHRNA5-CHRNA3-CHRNB4 gene cluster for association with ND, measures of cognitive performance and gene expression. As expected, we found all SNPs being associated with ND in three independent cohorts (KORA, NCOOP, ESTHER) comprising 5,561 individuals. In an overlapping sample of 2,186 subjects we found three SNPs (rs16969968, rs1051730, rs3743078) being associated with cognitive domains from the Wechsler-Adult-Intelligence Scale (WAIS-R)-most notably in the performance subtest "object assembly" and the verbal subtest "similarities." In a refined analysis of a subsample of 485 subjects, two of these three SNPs (rs16969968, rs1051730) were associated with n-back task performance/Continuous Performance Test. Furthermore, two CHRNA5 risk alleles (rs684513, rs637137) were associated with CHRNA5 mRNA expression levels in whole blood in a subgroup of 190 subjects. We here report for the first time an association of CHRNA5-CHRNA3-CHRNB4 gene variants with cognition possibly mediating in part risk for developing ND. The observed phenotype-genotype associations may depend on altered levels of gene expression. © 2010 Wiley-Liss, Inc., (Copyright © 2010 Wiley-Liss, Inc.)

Published

2010

26. Nonsense mutations in FAM161A cause RP28-associated recessive retinitis pigmentosa.

Author

Langmann T, Di Gioia SA, Rau I, Stöhr H, Maksimovic NS, Corbo JC, Renner AB, Zrenner E, Kumaramanickavel G, Karlstetter M, Arsenijevic Y, Weber BH, Gal A, and Rivolta C

Subjects

Amino Acid Sequence, Animals, Base Sequence, Binding Sites, DNA Mutational Analysis, Eye Proteins chemistry, Eye Proteins metabolism, Gene Expression Regulation, Developmental, Genes, Reporter, Humans, Mice, Molecular Sequence Data, RNA, Messenger genetics, RNA, Messenger metabolism, Retina pathology, Retinal Degeneration genetics, Retinal Degeneration pathology, Codon, Nonsense genetics, Eye Proteins genetics, Genes, Recessive genetics, Genetic Loci genetics, Retinitis Pigmentosa genetics

Abstract

Retinitis pigmentosa (RP) is a degenerative disease of the retina leading to progressive loss of vision and, in many instances, to legal blindness at the end stage. The RP28 locus was assigned in 1999 to the short arm of chromosome 2 by homozygosity mapping in a large Indian family segregating autosomal-recessive RP (arRP). Following a combined approach of chromatin immunoprecipitation and parallel sequencing of genomic DNA, we identified a gene, FAM161A, which was shown to carry a homozygous nonsense mutation (p.Arg229X) in patients from the original RP28 pedigree. Another homozygous FAM161A stop mutation (p.Arg437X) was detected in three subjects from a cohort of 118 apparently unrelated German RP patients. Age at disease onset in these patients was in the second to third decade, with severe visual handicap in the fifth decade and legal blindness in the sixth to seventh decades. FAM161A is a phylogenetically conserved gene, expressed in the retina at relatively high levels and encoding a putative 76 kDa protein of unknown function. In the mouse retina, Fam161a mRNA is developmentally regulated and controlled by the transcription factor Crx, as demonstrated by chromatin immunoprecipitation and organotypic reporter assays on explanted retinas. Fam161a protein localizes to photoreceptor cells during development, and in adult animals it is present in the inner segment as well as the outer plexiform layer of the retina, the synaptic interface between photoreceptors and their efferent neurons. Taken together, our data indicate that null mutations in FAM161A are responsible for the RP28-associated arRP., (2010 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2010

27. Female carriers of X-chromosomal adrenoleukodystrophy: a major differential diagnosis in progressive myelopathy.

Author

Guettsches AK, Kuechler A, Gal A, Schmitz W, Tegenthoff M, and Vorgerd M

Subjects

ATP Binding Cassette Transporter, Subfamily D, Member 1, ATP-Binding Cassette Transporters genetics, Adrenoleukodystrophy physiopathology, Aged, Diagnosis, Differential, Female, Genetic Predisposition to Disease genetics, Humans, Male, Middle Aged, Mutation, Pedigree, Adrenoleukodystrophy diagnosis, Adrenoleukodystrophy genetics, Heterozygote

Abstract

Adrenoleukodystrophy (ALD) and adrenomyeloneuropathy (AMN) are allelic X-chromosomal disorders of peroxisomal lipid metabolism due to mutations of the ABCD1-gene, leading, respectively, to leukoencephalopathy or myeloneuropathy in male patients. We report a family with two symptomatic carriers in subsequent generations who both suffer from symptoms of an AMN. In both patients, molecular genetic testing revealed a heterozygous c.1552C>T-transition (p.Arg518Trp) in exon 6 of ABCD1. Our observations underline the importance of identifying such symptomatic ALD carriers.

Published

2010

28. Ultra high throughput sequencing excludes MDH1 as candidate gene for RP28-linked retinitis pigmentosa.

Author

Rio Frio T, Panek S, Iseli C, Di Gioia SA, Kumar A, Gal A, and Rivolta C

Subjects

Humans, Polymorphism, Single Nucleotide genetics, Genetic Loci genetics, Genetic Predisposition to Disease, High-Throughput Screening Assays methods, Malate Dehydrogenase genetics, Retinitis Pigmentosa enzymology, Retinitis Pigmentosa genetics, Sequence Analysis, DNA methods

Abstract

Purpose: Mutations in IDH3B, an enzyme participating in the Krebs cycle, have recently been found to cause autosomal recessive retinitis pigmentosa (arRP). The MDH1 gene maps within the RP28 arRP linkage interval and encodes cytoplasmic malate dehydrogenase, an enzyme functionally related to IDH3B. As a proof of concept for candidate gene screening to be routinely performed by ultra high throughput sequencing (UHTs), we analyzed MDH1 in a patient from each of the two families described so far to show linkage between arRP and RP28., Methods: With genomic long-range PCR, we amplified all introns and exons of the MDH1 gene (23.4 kb). PCR products were then sequenced by short-read UHTs with no further processing. Computer-based mapping of the reads and mutation detection were performed by three independent software packages., Results: Despite the intrinsic complexity of human genome sequences, reads were easily mapped and analyzed, and all algorithms used provided the same results. The two patients were homozygous for all DNA variants identified in the region, which confirms previous linkage and homozygosity mapping results, but had different haplotypes, indicating genetic or allelic heterogeneity. None of the DNA changes detected could be associated with the disease., Conclusions: The MDH1 gene is not the cause of RP28-linked arRP. Our experimental strategy shows that long-range genomic PCR followed by UHTs provides an excellent system to perform a thorough screening of candidate genes for hereditary retinal degeneration.

Published

2009

29. A homozygous p.Glu150Lys mutation in the opsin gene of two Pakistani families with autosomal recessive retinitis pigmentosa.

Author

Azam M, Khan MI, Gal A, Hussain A, Shah ST, Khan MS, Sadeque A, Bokhari H, Collin RW, Orth U, van Genderen MM, den Hollander AI, Cremers FP, and Qamar R

Subjects

Alleles, Amino Acid Sequence, Base Sequence, Chi-Square Distribution, Family, Female, Fundus Oculi, Haplotypes genetics, Humans, Male, Microsatellite Repeats genetics, Molecular Sequence Data, Pakistan, Pedigree, Polymorphism, Single Nucleotide genetics, Rhodopsin chemistry, Sequence Analysis, Amino Acid Substitution genetics, Asian People genetics, Genes, Recessive, Homozygote, Mutation genetics, Retinitis Pigmentosa genetics, Rhodopsin genetics

Abstract

Purpose: To identify the gene mutations responsible for autosomal recessive retinitis pigmentosa (arRP) in Pakistani families., Methods: A cohort of consanguineous families with typical RP phenotype in patients was screened by homozygosity mapping using microsatellite markers that mapped close to 21 known arRP genes and five arRP loci. Mutation analysis was performed by direct sequencing of the candidate gene., Results: In two families, RP21 and RP53, homozygosity mapping suggested RHO, the gene encoding rhodopsin, as a candidate disease gene on chromosome 3q21. In six out of seven affected members from the two families, direct sequencing of RHO identified a homozygous c.448G>A mutation resulting in the p.Glu150Lys amino acid change. This variant was first reported in PMK197, an Indian arRP family. Single nucleotide polymorphism analysis in RP21, RP53, and PMK197 showed a common disease-associated haplotype in the three families., Conclusions: In two consanguineous Pakistani families with typical arRP phenotype in the patients, we identified a disease-causing mutation (p.Glu150Lys) in the RHO gene. Single nucleotide polymorphism analysis suggests that the previously reported Indian family (PMK197) and the two Pakistani families studied here share the RHO p.Glu150Lys mutation due to a common ancestry.

Published

2009

30. Mutations in FAM134B, encoding a newly identified Golgi protein, cause severe sensory and autonomic neuropathy.

Author

Kurth I, Pamminger T, Hennings JC, Soehendra D, Huebner AK, Rotthier A, Baets J, Senderek J, Topaloglu H, Farrell SA, Nürnberg G, Nürnberg P, De Jonghe P, Gal A, Kaether C, Timmerman V, and Hübner CA

Subjects

Adult, Animals, Female, Hereditary Sensory and Autonomic Neuropathies metabolism, Hereditary Sensory and Autonomic Neuropathies pathology, Humans, Intracellular Signaling Peptides and Proteins, Male, Membrane Proteins metabolism, Mice, Pedigree, RNA Interference, Golgi Apparatus metabolism, Hereditary Sensory and Autonomic Neuropathies genetics, Membrane Proteins genetics, Mutation, Neoplasm Proteins genetics

Abstract

Hereditary sensory and autonomic neuropathy type II (HSAN II) leads to severe mutilations because of impaired nociception and autonomic dysfunction. Here we show that loss-of-function mutations in FAM134B, encoding a newly identified cis-Golgi protein, cause HSAN II. Fam134b knockdown results in structural alterations of the cis-Golgi compartment and induces apoptosis in some primary dorsal root ganglion neurons. This implicates FAM134B as critical in long-term survival of nociceptive and autonomic ganglion neurons.

Published

2009

31. Rdh12 activity and effects on retinoid processing in the murine retina.

Author

Chrispell JD, Feathers KL, Kane MA, Kim CY, Brooks M, Khanna R, Kurth I, Hübner CA, Gal A, Mears AJ, Swaroop A, Napoli JL, Sparrow JR, and Thompson DA

Subjects

Alcohol Oxidoreductases, Animals, Heterozygote, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Transgenic, Models, Biological, Phenotype, Polymorphism, Genetic, Retina metabolism, Retinal Dehydrogenase genetics, Retinal Dehydrogenase metabolism, Retinoids metabolism, Superoxide Dismutase genetics, Retinal Dehydrogenase physiology, Retinal Photoreceptor Cell Outer Segment metabolism

Abstract

RDH12 mutations are responsible for early-onset autosomal recessive retinal dystrophy, which results in profound retinal pathology and severe visual handicap in patients. To investigate the function of RDH12 within the network of retinoid dehydrogenases/reductases (RDHs) present in retina, we studied the retinal phenotype of Rdh12-deficient mice. In vivo rates of all-trans-retinal reduction and 11-cis-retinal formation during recovery from bleaching were similar in Rdh12-deficient and wild-type mice matched for an Rpe65 polymorphism that impacts visual cycle efficiency. However, retinal homogenates from Rdh12-deficient mice exhibited markedly decreased capacity to reduce exogenous retinaldehydes in vitro. Furthermore, in vivo levels of the bisretinoid compound diretinoid-pyridinium-ethanolamine (A2E) were increased in Rdh12-deficient mice of various genetic backgrounds. Conversely, in vivo levels of retinoic acid and total retinol were significantly decreased. Rdh12 transcript levels in wild-type mice homozygous for the Rpe65-Leu(450) polymorphism were greater than in Rpe65-Met(450) mice and increased during postnatal development in wild-type mice and Nrl-deficient mice having an all-cone retina. Rdh12-deficient mice did not exhibit increased retinal degeneration relative to wild-type mice at advanced ages, when bred on the light-sensitive BALB/c background, or when heterozygous for a null allele of superoxide dismutase 2 (Sod2(+/-)). Our findings suggest that a critical function of RDH12 is the reduction of all-trans-retinal that exceeds the reductive capacity of the photoreceptor outer segments.

Published

2009

32. Duplications of noncoding elements 5' of SOX9 are associated with brachydactyly-anonychia.

Author

Kurth I, Klopocki E, Stricker S, van Oosterwijk J, Vanek S, Altmann J, Santos HG, van Harssel JJ, de Ravel T, Wilkie AO, Gal A, and Mundlos S

Subjects

Animals, Gene Expression Regulation, Developmental, Humans, Mice, SOX9 Transcription Factor metabolism, DNA, Intergenic genetics, Gene Duplication, Limb Deformities, Congenital genetics, Nail Diseases genetics, Regulatory Sequences, Nucleic Acid genetics, SOX9 Transcription Factor genetics

Published

2009

33. Mutations in TOPORS: a rare cause of autosomal dominant retinitis pigmentosa in continental Europe?

Author

Schob C, Orth U, Gal A, Kindler S, Chakarova CF, Bhattacharya SS, and Rüther K

Subjects

Europe, Genes, Dominant, Humans, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Polymorphism, Single-Stranded Conformational, RNA, Messenger metabolism, Mutation, Neoplasm Proteins genetics, Nuclear Proteins genetics, Retinitis Pigmentosa genetics, Ubiquitin-Protein Ligases genetics

Abstract

Mutations in TOPORS cause autosomal dominant retinitis pigmentosa (adRP). Examination of 160 adRP patients from continental Europe revealed nine exonic single nucleotide variants, eight of which reside in the coding region; three synonymous single nucleotide polymorphisms (SNPs; c.2319T > C, c.2991T > C and c.1560A > G), three nonsynonymous SNPs (c.58C > T/p.P20S, c.74C >G/p.S25W and c.1730C > A/p.S577Y) and two novel missense mutations (c.1205A > C/p.Q402P and c.1818T > G/p.S606R). Whether the latter two variants represent adRP causing mutations awaits further analysis.

Published

2009

34. A 4-year study of the efficacy and tolerability of enzyme replacement therapy with agalsidase alfa in 36 women with Fabry disease.

Author

Whybra C, Miebach E, Mengel E, Gal A, Baron K, Beck M, and Kampmann C

Subjects

Adult, Aged, Analysis of Variance, Drug Administration Schedule, Fabry Disease genetics, Fabry Disease pathology, Female, Glomerular Filtration Rate drug effects, Humans, Isoenzymes therapeutic use, Leukocytes enzymology, Middle Aged, Mutation, Prospective Studies, Recombinant Proteins, Severity of Illness Index, Treatment Outcome, Young Adult, alpha-Galactosidase genetics, alpha-Galactosidase metabolism, Fabry Disease drug therapy, alpha-Galactosidase therapeutic use

Abstract

Purpose: Although Fabry disease is X linked and considered to affect primarily male hemizygotes, female heterozygotes may experience all the signs and symptoms of this metabolic disorder. This prospective, single-center, open-label, clinical trial was performed to evaluate the long-term response of female patients with Fabry disease to enzyme replacement therapy., Methods: Symptomatic women (average age = 47 years) enrolled in this 4-year study were treated with agalsidase alfa (Replagal, Shire HGT, Inc.) at a dose of 0.2 mg/kg, every other week for 4 years (N = 36). Clinical and biochemical assessments were conducted at 12-month intervals., Results: The Mainz Severity Score Index, a measure of total disease burden, was significantly reduced after 12 months (P < 0.01) of treatment and continuously improved over 4 years. Brief Pain Inventory "pain at its worst" score was reduced from 4.6 +/- 2.9 at baseline to 3.3 +/- 2.9 after 12 months (P = 0.001) and remained reduced through 4 years. Mean left-ventricular mass decreased from 89.4 +/- 29.3(2.7) g/m at baseline to 66.5 +/- 29.3(2.7) g/m after 12 months (P < 0.001) and remained reduced through 4 years. Average kidney function (estimated glomerular filtration rate and proteinuria) remained constant during the study. No safety issues were identified., Conclusions: Long-term agalsidase alfa is effective and was well tolerated in women with Fabry disease.

Published

2009

35. Phenotypic variability and long-term follow-up of patients with known and novel PRPH2/RDS gene mutations.

Author

Renner AB, Fiebig BS, Weber BH, Wissinger B, Andreasson S, Gal A, Cropp E, Kohl S, and Kellner U

Subjects

Adolescent, Adult, Aged, Child, Color Perception Tests, DNA Mutational Analysis, Diseases in Twins genetics, Electroretinography, Female, Fluorescein Angiography, Follow-Up Studies, Humans, Male, Peripherins, Phenotype, Polymerase Chain Reaction, Retinal Degeneration diagnosis, Retinal Degeneration physiopathology, Retrospective Studies, Tomography, Optical Coherence, Twins, Monozygotic genetics, Intermediate Filament Proteins genetics, Membrane Glycoproteins genetics, Mutation, Nerve Tissue Proteins genetics, Retinal Degeneration genetics

Abstract

Purpose: To describe the phenotypic variability in 22 patients with PRPH2 gene mutations and to report six novel mutations., Design: Retrospective study., Methods: Clinical examinations included color vision testing, perimetry, fundus autofluorescence (FAF), fluorescein angiography, optical coherence tomography (OCT), and full-field and multifocal electroretinography (International Society for Clinical Electrophysiology of Vision standards). Blood samples were taken for deoxyribonucleic acid (DNA) extraction and mutation screening was performed by direct sequencing of polymerase chain reaction amplicons., Results: Eleven unrelated patients and four unrelated families each with two affected members as well as one family with three affected members were examined. Diagnoses included central areolar choroidal dystrophy (CACD; n = 9), autosomal dominant retinitis pigmentosa (adRP; n = 7), adult vitelliform macular dystrophy (n = 3), and cone-rod dystrophy (CRD; n = 3). FAF was abnormal in all patients and showed various retinal pigment epithelial alterations, in CACD with a speckled FAF pattern. OCT revealed reduced retinal thickness, mostly in CACD, subretinal lesions, macula edema, or was normal. Follow-up (n = 12; range, 1.3 to 26 years) showed a slow progression of the retinal dystrophies. DNA testing revealed previously reported PRPH2 mutations in two families and eight individuals of whom two carried the same mutation but had different phenotypes. Novel PRPH2 mutations were detected in two families with adRP, in identical twins with CACD, and in each of an individual with CACD, CRD, and adRP., Conclusions: This series describes the broad spectrum of phenotypes associated with PRPH2 mutations. FAF and OCT are helpful tools for diagnosis and evaluation of disease progression. We report novel PRPH2 mutations in patients with CACD, CRD, and adRP.

Published

2009

36. Onset and progression of the Anderson-Fabry disease related cardiomyopathy.

Author

Kampmann C, Linhart A, Baehner F, Palecek T, Wiethoff CM, Miebach E, Whybra C, Gal A, Bultas J, and Beck M

Subjects

Adolescent, Adult, Age of Onset, Aged, Cardiomyopathies diagnostic imaging, Child, Child, Preschool, Cross-Sectional Studies, Disease Progression, Echocardiography, Fabry Disease drug therapy, Female, Follow-Up Studies, Humans, Hypertrophy, Left Ventricular diagnostic imaging, Hypertrophy, Left Ventricular epidemiology, Hypertrophy, Left Ventricular physiopathology, Linear Models, Male, Middle Aged, Prevalence, Young Adult, Cardiomyopathies epidemiology, Cardiomyopathies physiopathology, Fabry Disease epidemiology, Fabry Disease physiopathology

Abstract

Background: Cardiac involvement is responsible for substantial morbidity and mortality in Anderson-Fabry disease (AFD). We sought to document its onset and progression in a population of male and female AFD patients., Methods: We performed a cross sectional echocardiographic study of a cohort of 177 male and female AFD patients with subsequent longitudinal follow-up of 76 patients (38 males and 38 females; mean follow-up 4.5 years) who did not receive enzyme replacement therapy., Results: In this population, aged 3.3 to 70.8 years, a strong correlation between age and left ventricular mass indexed (LVMi, g/m(2.7)) was found in both males and females (P<0.0001 for both). At the initial examination 48.6% of the male patients and 36.4% of the female patients were classified as having left ventricular hypertrophy (LVH). The cumulative prevalence of LVH peaked at age 40 years in males and 60 years in females. In patients with longitudinal follow-up, LVMi increased by 4.07+/-1.03 g/m(2.7) per year in males and by 2.31+/-0.81 g/m(2.7) in females (P<0.01, Wilcoxon rank sum). In patients with LVH at baseline, the median progression rate was 5.52 g/m(2.7) per year in males and by 1.80 g/m(2.7) in females (P=0.12)., Conclusion: AFD is associated with high prevalence of LVH in both genders. However, the age of onset is delayed in females and progression rate slower.

Published

2008

37. Does proximal myotonic myopathy show anticipation?

Author

Kruse B, Wöhrle D, Steinbach P, and Gal A

Subjects

Adult, Age Factors, Blotting, Southern, Child, Preschool, DNA Mutational Analysis, Family Health, Female, Humans, Male, Myotonic Disorders congenital, Polymerase Chain Reaction, RNA-Binding Proteins genetics, Time Factors, Trinucleotide Repeat Expansion, Anticipation, Genetic, Myotonic Disorders genetics

Abstract

Proximal myotonic myopathy (DM2, PROMM) has not been reported in patients younger than 18 years, and apparent lack of congenital and childhood forms is thought to be one of the distinctive clinical characteristics of this trait. We now describe a 2-year-old boy, the youngest member of a family with a history for myotonia in 2 generations. The patient's 35-year-old mother was diagnosed with DM2 of late juvenile onset. She developed aggravating myotonic symptoms during pregnancy. Remarkably few intrauterine child movements were noticed. After birth the child showed general muscular hypotonia with delayed statomotoric development (sitting and crawling at 13 months, first lifting into standing position at 18 months). Muscle reflexes were normal. In the CL3N58 region of ZNF9, DM2-typical unstable expanded CCTG arrays of about 14.5 kb (about 2,500 repeats) were detected both in the mother and the patient by Southern blotting. Expansion of the DM1-specific DMPK CTG repeat was excluded.

Published

2008

38. Identification of novel mutations in X-linked retinitis pigmentosa families and implications for diagnostic testing.

Author

Neidhardt J, Glaus E, Lorenz B, Netzer C, Li Y, Schambeck M, Wittmer M, Feil S, Kirschner-Schwabe R, Rosenberg T, Cremers FP, Bergen AA, Barthelmes D, Baraki H, Schmid F, Tanner G, Fleischhauer J, Orth U, Becker C, Wegscheider E, Nürnberg G, Nürnberg P, Bolz HJ, Gal A, and Berger W

Subjects

Exons genetics, Eye Proteins genetics, Family, Female, GTP-Binding Proteins, Genes, Dominant, Heterozygote, Humans, Inheritance Patterns genetics, Intracellular Signaling Peptides and Proteins genetics, Male, Membrane Proteins genetics, Pedigree, Polymorphism, Genetic, Sequence Deletion, Genetic Diseases, X-Linked diagnosis, Genetic Diseases, X-Linked genetics, Mutation genetics, Retinitis Pigmentosa diagnosis, Retinitis Pigmentosa genetics

Abstract

Purpose: The goal of this study was to identify mutations in X-chromosomal genes associated with retinitis pigmentosa (RP) in patients from Germany, The Netherlands, Denmark, and Switzerland., Methods: In addition to all coding exons of RP2, exons 1 through 15, 9a, ORF15, 15a and 15b of RPGR were screened for mutations. PCR products were amplified from genomic DNA extracted from blood samples and analyzed by direct sequencing. In one family with apparently dominant inheritance of RP, linkage analysis identified an interval on the X chromosome containing RPGR, and mutation screening revealed a pathogenic variant in this gene. Patients of this family were examined clinically and by X-inactivation studies., Results: This study included 141 RP families with possible X-chromosomal inheritance. In total, we identified 46 families with pathogenic sequence alterations in RPGR and RP2, of which 17 mutations have not been described previously. Two of the novel mutations represent the most 3'-terminal pathogenic sequence variants in RPGR and RP2 reported to date. In exon ORF15 of RPGR, we found eight novel and 14 known mutations. All lead to a disruption of open reading frame. Of the families with suggested X-chromosomal inheritance, 35% showed mutations in ORF15. In addition, we found five novel mutations in other exons of RPGR and four in RP2. Deletions in ORF15 of RPGR were identified in three families in which female carriers showed variable manifestation of the phenotype. Furthermore, an ORF15 mutation was found in an RP patient who additionally carries a 6.4 kbp deletion downstream of the coding region of exon ORF15. We did not identify mutations in 39 sporadic male cases from Switzerland., Conclusions: RPGR mutations were confirmed to be the most frequent cause of RP in families with an X-chromosomal inheritance pattern. We propose a screening strategy to provide molecular diagnostics in these families.

Published

2008

39. The mutation p.Ser298Pro in the sulphamidase gene (SGSH) is associated with a slowly progressive clinical phenotype in mucopolysaccharidosis type IIIA (Sanfilippo A syndrome).

Author

Meyer A, Kossow K, Gal A, Steglich C, Mühlhausen C, Ullrich K, Braulke T, and Muschol N

Subjects

Adolescent, Adult, Child, Child, Preschool, Disease Progression, Female, Genotype, Humans, Infant, Infant, Newborn, Male, Mucopolysaccharidosis III physiopathology, Phenotype, Hydrolases genetics, Mucopolysaccharidosis III genetics, Mutation, Proline genetics, Serine genetics

Abstract

Mucopolysaccharidosis type IIIA (MPS IIIA, Sanfilippo A syndrome) is caused by mutations in the N-sulfoglucosamine sulfohydrolase (SGSH) gene and the resulting defective lysosomal degradation of the glycosaminoglycan heparan sulfate. The onset and progression of the disease are highly variable. Seventy-five mutations distributed over the SGSH gene have been described. We here report on the analysis of the natural course of the disease in 54 MPS IIIA patients through the use of a detailed questionnaire and four-point scoring system and an examination of the underlying mutations. By assessing the degree of developmental regression over time a group of seven patients with a slowly progressive course of the disease were identified. In these seven patients and in 3 other mildly affected patients the missense mutation c.892T>C (p.Ser298Pro) was found on one allele. These patients showed a lower frequency and later onset of the typical symptoms of the disease. The onset of regression in speech abilities and cognitive functions were delayed by 0.7 and 0.8 years, respectively, and the onset of regression of motor functions occurred 6.1 years later than in all other MPS IIIA patients. Severe regression in speech, cognitive and motor functions were delayed by 5, 5.9, and 11.2 years, respectively. These data suggest that in MPS IIIA patients carrying the mutation p.Ser298Pro a slowly progressive phenotype can be predicted and this may have an important impact on parental counselling and therapeutic interventions.

Published

2008

40. Scoring evaluation of the natural course of mucopolysaccharidosis type IIIA (Sanfilippo syndrome type A).

Author

Meyer A, Kossow K, Gal A, Mühlhausen C, Ullrich K, Braulke T, and Muschol N

Subjects

Adolescent, Adult, Child, Child, Preschool, Cohort Studies, Disease Progression, Female, Humans, Infant, Infant, Newborn, Male, Mucopolysaccharidosis III diagnosis, Surveys and Questionnaires, Mucopolysaccharidosis III classification, Mucopolysaccharidosis III pathology, Research Design

Abstract

Objective: Mucopolysaccharidosis types IIIA through IIID (Sanfilippo syndrome) are caused by deficiencies of enzymes involved in the degradation of heparan sulfate. The onset and severity of the disease are highly variable. The purpose of this study was to describe the natural course of mucopolysaccharidosis type IIIA in a large cohort of patients., Patients and Methods: The natural course of mucopolysaccharidosis type IIIA was assessed in 71 patients by using a detailed questionnaire and a 4-point scoring system and compared with the course of the disease in 14 patients with mucopolysaccharidosis type IIIB and 4 patients with mucopolysaccharidosis type IIIC., Results: In the cohort of patients with mucopolysaccharidosis type IIIA, first symptoms of disease were observed, on average, at 7 months of age. Speech and motor development were delayed in 66.2% and 33.9% of patients, respectively. The median age at diagnosis was 4.5 years. The onset of regression in speech, motor, and cognitive function was observed at an average age of 3.3 years. The loss of all 3 of the assessed abilities was observed at an average age of 12.5 years. Speech was lost before motor and cognitive functions. In a small group of patients who were >12.5 years of age (9.9%), speech, motor, and cognitive skills were partially preserved up to a maximum age of 23.8 years., Conclusions: To our knowledge, this is the first systematic and comprehensive study on the natural course of mucopolysaccharidosis type IIIA. The 4-point scoring system may be used to classify patients into groups with a rapid or slower course of the disease. This may have an important impact on parental counseling as well as therapeutic interventions.

Published

2007

41. Mutations in TOPORS cause autosomal dominant retinitis pigmentosa with perivascular retinal pigment epithelium atrophy.

Author

Chakarova CF, Papaioannou MG, Khanna H, Lopez I, Waseem N, Shah A, Theis T, Friedman J, Maubaret C, Bujakowska K, Veraitch B, Abd El-Aziz MM, Prescott de Q, Parapuram SK, Bickmore WA, Munro PM, Gal A, Hamel CP, Marigo V, Ponting CP, Wissinger B, Zrenner E, Matter K, Swaroop A, Koenekoop RK, and Bhattacharya SS

Subjects

Adolescent, Adult, Base Sequence, Child, Chromosomes, Human, DNA Mutational Analysis, Exons genetics, Female, Humans, Male, Middle Aged, Molecular Sequence Data, Neoplasm Proteins metabolism, Nuclear Proteins metabolism, Pedigree, Ubiquitin-Protein Ligases metabolism, Genes, Dominant, Mutation genetics, Neoplasm Proteins genetics, Nuclear Proteins genetics, Pigment Epithelium of Eye blood supply, Pigment Epithelium of Eye pathology, Retinitis Pigmentosa genetics, Ubiquitin-Protein Ligases genetics

Abstract

We report mutations in the gene for topoisomerase I-binding RS protein (TOPORS) in patients with autosomal dominant retinitis pigmentosa (adRP) linked to chromosome 9p21.1 (locus RP31). A positional-cloning approach, together with the use of bioinformatics, identified TOPORS (comprising three exons and encoding a protein of 1,045 aa) as the gene responsible for adRP. Mutations that include an insertion and a deletion have been identified in two adRP-affected families--one French Canadian and one German family, respectively. Interestingly, a distinct phenotype is noted at the earlier stages of the disease, with an unusual perivascular cuff of retinal pigment epithelium atrophy, which was found surrounding the superior and inferior arcades in the retina. TOPORS is a RING domain-containing E3 ubiquitin ligase and localizes in the nucleus in speckled loci that are associated with promyelocytic leukemia bodies. The ubiquitous nature of TOPORS expression and a lack of mutant protein in patients are highly suggestive of haploinsufficiency, rather than a dominant negative effect, as the molecular mechanism of the disease and make rescue of the clinical phenotype amenable to somatic gene therapy.

Published

2007

42. L1CAM mutation in a boy with hydrocephalus and duplex kidneys.

Author

Liebau MC, Gal A, Superti-Furga A, Omran H, and Pohl M

Subjects

Abnormalities, Multiple genetics, Base Sequence, Child, Humans, Intellectual Disability genetics, Introns, Kidney diagnostic imaging, Kidney surgery, Kidney Function Tests, Male, Sequence Deletion, Treatment Outcome, Ultrasonography, Ureter abnormalities, Chromosomes, Human, X, Hydrocephalus genetics, Kidney abnormalities, Mutation, Neural Cell Adhesion Molecule L1 genetics

Abstract

Mutations in the X-chromosomal gene (L1CAM) for cell adhesion molecule L1 are associated with a heterogeneous group of conditions that include agenesis of the corpus callosum, hydrocephalus, spastic paraplegia, adducted thumbs and mental retardation (L1-spectrum disease, CRASH or MASA syndrome). Although L1CAM is expressed during renal development and L1cam-deficient mice have congenital malformations of the kidney and the urinary tract, L1CAM mutations have not been associated with renal anomalies in men. We report on a boy with prenatally detected hydrocephalus. After his birth, bilateral duplex kidneys and ureters, with a unilateral mega-ureter serving a hydronephrotic upper pole, as well as agenesis of the corpus callosum, adducted thumbs, spasticity, and mental retardation were recognized, fulfilling the criteria of an L1-spectrum disease. Genetic testing of the patient and his mother identified a 2 bp deletion in the invariant splice consensus sequence of intron 18 of L1CAM, predicting a largely truncated or absent protein. At the age of 9 years, 7 years after heminephrectomy, the boy has normal renal function. This observation suggests that patients with L1CAM mutations may have renal abnormalities as seen in the L1cam-deficient mouse model. L1CAM might, therefore, also be considered a possible candidate gene for renal malformations.

Published

2007

43. p.Gln200Glu, a putative constitutively active mutant of rod alpha-transducin (GNAT1) in autosomal dominant congenital stationary night blindness.

Author

Szabo V, Kreienkamp HJ, Rosenberg T, and Gal A

Subjects

Female, Heterotrimeric GTP-Binding Proteins chemistry, Humans, Male, Models, Molecular, Molecular Structure, Night Blindness congenital, Pedigree, Transducin, Genes, Dominant, Heterotrimeric GTP-Binding Proteins genetics, Mutation, Missense, Night Blindness genetics, Retinal Rod Photoreceptor Cells chemistry

Abstract

Congenital stationary night blindness (CSNB) is a non-progressive Mendelian condition resulting from a functional defect in rod photoreceptors. A small number of unique missense mutations in the genes encoding various members of the rod phototransduction cascade, e.g. rhodopsin (RHO), cGMP phosphodiesterase beta-subunit (PDE6B), and transducin alpha-subunit (GNAT1) have been reported to cause autosomal dominant (ad) CSNB. While the RHO and PDE6B mutations result in constitutively active proteins, the only known adCSNB-associated GNAT1 change (p.Gly38Asp) produces an alpha-transducin that is unable to activate its downstream effector molecule in vitro. In a multigeneration Danish family with adCSNB, we identified a novel heterozygous C to G transversion (c.598C>G) in exon 6 of GNAT1 that should result in a p.Gln200Glu substitution in the evolutionarily highly conserved Switch 2 region of alpha-transducin, a domain that has an important role in binding and hydrolyzing GTP. Computer modeling based on the known crystal structure of transducin suggests that the p.Gln200Glu mutant exhibits impaired GTPase activity, and thereby leads to constitutive activation of phototransduction. This assumption is in line with our results of trypsin protection assays as well as previously published biochemical data on mutants of this glutamine in the GTPase active site of alpha-transducin following in vitro expression, and observations that inappropriately activating mutants of various members of the rod phototransduction cascade represent one of the major molecular causes of adCSNB., ((c) 2007 Wiley-Liss, Inc.)

Published

2007

44. The phenotype of early-onset retinal degeneration in persons with RDH12 mutations.

Author

Schuster A, Janecke AR, Wilke R, Schmid E, Thompson DA, Utermann G, Wissinger B, Zrenner E, and Gal A

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, Color Perception, Electroretinography, Humans, Middle Aged, Phenotype, Photoreceptor Cells, Vertebrate pathology, Retinal Degeneration diagnosis, Visual Acuity, Visual Fields, Alcohol Oxidoreductases genetics, Mutation, Retinal Degeneration genetics

Abstract

Purpose: To describe the retinal dystrophy phenotype associated with mutations in RDH12, the gene encoding a retinoid dehydrogenase/reductase expressed in the photoreceptor cells., Methods: Sixteen persons from 12 families with pathogenic RDH12 mutations on both alleles were studied. Retinal phenotypes were characterized by ophthalmic examination, including psychophysical and standardized electrophysiological methods and multifocal electroretinography (mfERG)., Results: The retinal disease in persons with RDH12 mutations in the homozygous (p.G127X, p.Q189X, p.Y226C, p.A269GfsX1, and p.L274P) or compound heterozygous state (p.R65X/p.A269GfsX1, p.H151D/p.T155I, p.H151D/p.A269GfsX1) was diagnosed initially as Leber congenital amaurosis (LCA) or early-onset retinitis pigmentosa. These individuals appeared to share a common clinical picture, independent of the type of mutation, characterized by poor, yet useful visual function in early life, followed by progressive decline due to both rod and cone degeneration. Marked pigmentary retinopathy, including bone spicules in the peripheral retina, was present in all persons older than age 6, and pronounced maculopathy was evident in persons older than 7 years. A unique view into the progressive nature of the disorder was achieved by evaluation of seven affected persons from three consanguineous families, all carrying the homozygous p.Y226C mutation., Conclusions: Ophthalmic findings in persons with RDH12 mutations suggest that RDH12 loss-of-function results in a characteristic form of early and progressive rod-cone degeneration distinct from that caused by mutations in other LCA genes. From our data, it seems likely that various clinical designations appropriately describe the diagnosis in these persons, including early-onset retinitis pigmentosa, LCA type II, and childhood retinal dystrophy.

Published

2007

45. Targeted disruption of the murine retinal dehydrogenase gene Rdh12 does not limit visual cycle function.

Author

Kurth I, Thompson DA, Rüther K, Feathers KL, Chrispell JD, Schroth J, McHenry CL, Schweizer M, Skosyrski S, Gal A, and Hübner CA

Subjects

Alcohol Oxidoreductases, Animals, Electroretinography, Gene Expression Regulation, Humans, Immunohistochemistry, Mice, Oxidative Stress, Photoreceptor Cells, Vertebrate cytology, Photoreceptor Cells, Vertebrate enzymology, Photoreceptor Cells, Vertebrate ultrastructure, Protein Transport, RNA, Messenger genetics, RNA, Messenger metabolism, Retinal Dehydrogenase deficiency, Retinal Dehydrogenase immunology, Retinoids analysis, Vision, Ocular genetics, Gene Targeting, Retinal Dehydrogenase genetics, Retinal Dehydrogenase metabolism, Vision, Ocular physiology

Abstract

RDH12 codes for a member of the family of short-chain alcohol dehydrogenases/reductases proposed to function in the visual cycle that supplies the chromophore 11-cis retinal to photoreceptor cells. Mutations in RDH12 cause severe and progressive childhood onset autosomal-recessive retinal dystrophy, including Leber congenital amaurosis. We generated Rdh12 knockout mice, which exhibited grossly normal retinal histology at 10 months of age. Levels of all-trans and 11-cis retinoids in dark- and light-adapted animals and scotopic and photopic electroretinogram (ERG) responses were similar to those for the wild type, as was recovery of the ERG response following bleaching, for animals matched for an Rpe65 polymorphism (p.L450M). Lipid peroxidation products and other measures of oxidative stress did not appear to be elevated in Rdh12(-/-) animals. RDH12 was localized to photoreceptor inner segments and the outer nuclear layer in both mouse and human retinas by immunohistochemistry. The present findings, together with those of earlier studies showing only minor functional deficits in mice deficient for Rdh5, Rdh8, or Rdh11, suggest that the activity of any one isoform is not rate limiting in the visual response.

Published

2007

46. Mutations of the mitochondrial holocytochrome c-type synthase in X-linked dominant microphthalmia with linear skin defects syndrome.

Author

Wimplinger I, Morleo M, Rosenberger G, Iaconis D, Orth U, Meinecke P, Lerer I, Ballabio A, Gal A, Franco B, and Kutsche K

Subjects

Amino Acid Sequence, Animals, Base Sequence, CHO Cells, Child, Child, Preschool, Cricetinae, DNA genetics, Female, Genes, Dominant, Genes, X-Linked, Genetic Complementation Test, Haplotypes, Holoenzymes genetics, Humans, Male, Mitochondria enzymology, Molecular Sequence Data, Pedigree, Phenotype, Polymorphism, Single Nucleotide, Sequence Deletion, Syndrome, X Chromosome Inactivation, Genetic Diseases, X-Linked enzymology, Genetic Diseases, X-Linked genetics, Lyases genetics, Microphthalmos enzymology, Microphthalmos genetics, Skin Abnormalities enzymology, Skin Abnormalities genetics

Abstract

The microphthalmia with linear skin defects syndrome (MLS, or MIDAS) is an X-linked dominant male-lethal disorder almost invariably associated with segmental monosomy of the Xp22 region. In two female patients, from two families, with MLS and a normal karyotype, we identified heterozygous de novo point mutations--a missense mutation (p.R217C) and a nonsense mutation (p.R197X)--in the HCCS gene. HCCS encodes the mitochondrial holocytochrome c-type synthase that functions as heme lyase by covalently adding the prosthetic heme group to both apocytochrome c and c(1). We investigated a third family, displaying phenotypic variability, in which the mother and two of her daughters carry an 8.6-kb submicroscopic deletion encompassing part of the HCCS gene. Functional analysis demonstrates that both mutant proteins (R217C and Delta 197-268) were unable to complement a Saccharomyces cerevisiae mutant deficient for the HCCS orthologue Cyc3p, in contrast to wild-type HCCS. Moreover, ectopically expressed HCCS wild-type and the R217C mutant protein are targeted to mitochondria in CHO-K1 cells, whereas the C-terminal-truncated Delta 197-268 mutant failed to be sorted to mitochondria. Cytochrome c, the final product of holocytochrome c-type synthase activity, is implicated in both oxidative phosphorylation (OXPHOS) and apoptosis. We hypothesize that the inability of HCCS-deficient cells to undergo cytochrome c-mediated apoptosis may push cell death toward necrosis that gives rise to severe deterioration of the affected tissues. In summary, we suggest that disturbance of both OXPHOS and the balance between apoptosis and necrosis, as well as the X-inactivation pattern, may contribute to the variable phenotype observed in patients with MLS.

Published

2006

47. Critical assessment of chitotriosidase analysis in the rational laboratory diagnosis of children with Gaucher disease and Niemann-Pick disease type A/B and C.

Author

Ries M, Schaefer E, Lührs T, Mani L, Kuhn J, Vanier MT, Krummenauer F, Gal A, Beck M, and Mengel E

Subjects

Chemistry, Clinical methods, Child, Child, Preschool, Diagnosis, Differential, Gene Duplication, Humans, Infant, Predictive Value of Tests, Retrospective Studies, Sensitivity and Specificity, Gaucher Disease diagnosis, Gaucher Disease genetics, Hexosaminidases metabolism, Niemann-Pick Disease, Type A diagnosis, Niemann-Pick Disease, Type B diagnosis, Niemann-Pick Disease, Type C diagnosis

Abstract

Laboratory diagnosis of lysosomal storage disorders, especially sphingomyelinase deficiency (Niemann-Pick disease type A/B) and Niemann-Pick disease type C (NPC) can be challenging. We therefore aimed to analyse the feasibility of first-step screening with specific chitotriosidase cut-off values in children

Published

2006

48. IgA nephropathy in two adolescent sisters heterozygous for Fabry disease.

Author

Whybra C, Schwarting A, Kriegsmann J, Gal A, Mengel E, Kampmann C, Baehner F, Schaefer E, and Beck M

Subjects

Adult, Female, Humans, Fabry Disease genetics, Genetic Carrier Screening, Glomerulonephritis, IGA genetics, Glomerulonephritis, IGA physiopathology

Abstract

We report a 16-year-old girl and her one-year-younger sister, both heterozygous for the c.34del24 mutation of the GLA (alpha-galactosidase A) gene, which they inherited from their father who is affected by Fabry disease (FD). Both girls presented with macrohematuria and rapidly progressing proteinuria. Urine analysis revealed glomerular hematuria and a nephrotic range of proteinuria suggesting a concomitant glomerulonephritis. Light microscopy of kidney biopsy was characteristic of IgA nephropathy (IgA deposits in mesangial areas and glomerular capillary loops, and mesangial hypercellularity), whereas electron microscopy showed changes typical of Fabry disease (multiple osmiophilic inclusions in the subendothelial and mesangial areas). These two cases and similar reports in the literature suggest that IgA nephropathy in FD is not merely coincidental.

Published

2006

49. Prevalence of uncontrolled hypertension in patients with Fabry disease.

Author

Kleinert J, Dehout F, Schwarting A, de Lorenzo AG, Ricci R, Kampmann C, Beck M, Ramaswami U, Linhart A, Gal A, Houge G, Widmer U, Mehta A, and Sunder-Plassmann G

Subjects

Antihypertensive Agents therapeutic use, Blood Pressure, Dialysis, Fabry Disease drug therapy, Fabry Disease physiopathology, Female, Humans, Hypertension drug therapy, Hypertension physiopathology, Kidney physiology, Kidney Transplantation, Male, Prevalence, Sex Ratio, Fabry Disease complications, Fabry Disease epidemiology, Hypertension complications, Hypertension epidemiology

Abstract

Background: Fabry disease is a rare X-linked disease arising from deficiency of alpha-galactosidase A. It results in early death related to renal, cardiac, and cerebrovascular disease, which are also important outcomes in patients with elevated blood pressure (BP). The prevalence of uncontrolled hypertension, as well as the effect of enzyme replacement therapy on BP, in patients with Fabry disease is unknown., Methods: We examined uncontrolled hypertension (systolic BP [SBP] >or=130 mm Hg or diastolic BP [DBP] >or=80 mm Hg) among 391 patients with Fabry disease who were participating in the Fabry Outcome Survey (FOS)., Results: Uncontrolled hypertension was present in 57% of men and 47% of women. In patients with chronic kidney disease (CKD) stage 1 (n100), median SBP was 120 mm Hg and median DBP was 74 mm Hg. In patients with CKD stage 2 (n172), median SBP was 125 mm Hg and median DBP was 75 mm Hg. In patients with CKD stage 3 (n63), median SBP was 130 mm Hg and median DBP was 75 mm Hg. There was a significant decrease in both SBP and DBP during a 2-year course of enzyme replacement therapy., Conclusions: This study revealed a high prevalence of uncontrolled hypertension among patients with Fabry disease. Thus there is a need to improve BP control and renoprotection in patients with Fabry disease.

Published

2006

50. Multiplex ligation-dependent probe amplification for rapid detection of proteolipid protein 1 gene duplications and deletions in affected males and carrier females with Pelizaeus-Merzbacher disease.

Author

Warshawsky I, Chernova OB, Hübner CA, Stindl R, Henneke M, Gal A, and Natowicz MR

Subjects

Female, Gene Deletion, Gene Duplication, Humans, Male, Nucleic Acid Amplification Techniques, Oligonucleotide Probes, Reference Values, Carrier State, Membrane Proteins genetics, Myelin Proteolipid Protein genetics, Pelizaeus-Merzbacher Disease genetics

Abstract

Background: Pelizaeus-Merzbacher disease is a rare X-linked neurodegenerative disorder caused by sequence variations in the proteolipid protein 1 gene (PLP1). PLP1 gene duplications account for approximately 50%-75% of cases and point variations for approximately 15%-20% of cases; deletions and insertions occur infrequently. We used multiplex ligation-dependent probe amplification (MLPA) to detect PLP1 gene alterations, especially gene duplications and deletions., Methods: We performed MLPA on 102 samples from individuals with diverse PLP1 gene abnormalities and from controls, including 50 samples previously characterized for the PLP1 gene by quantitative PCR but which were anonymized for prior results and sex., Results: All males with PLP1 gene duplications (n = 13), 1 male with a triplication, 2 males with whole gene deletions, and all controls (n = 72) were unambiguously assigned to their correct genotype. Of 4 female carriers tested by MLPA and quantitative PCR, 3 were duplication carriers by both methods, and 1 was a triplication carrier by MLPA and a duplication carrier by quantitative PCR. For 1 sample with a partial deletion, MLPA showed exon 3 deleted but PCR showed exons 3 and 4 deleted. Sequence analysis of 2 samples with reduced dosage for exons 3 and 5 revealed point variations overlapping the annealing site for the corresponding MLPA probe. The precision of MLPA analysis was excellent and comparable to or better than quantitative PCR, with CVs of 4.3%-9.8%., Conclusions: MLPA is a rapid and reliable method to determine PLP1 gene copies. Samples with partial PLP1 gene dosage alterations require confirmation with a non-MLPA method.

Published

2006