Your search keyword '"O Rieß"' showing total 611 results

101. Characterization of the gene for human neutrophil-activating peptide 78 (ENA-78)

Author

O. Riess, M.S. Corbett, Ina Schmitt, and A. Walz

Subjects

Chemokine CXCL5, DNA, Complementary, Molecular Sequence Data, Biophysics, EcoRI, Regulatory Sequences, Nucleic Acid, Biochemistry, Cell Line, Exon, Complementary DNA, Humans, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, Gene, Southern blot, Binding Sites, biology, Base Sequence, Interleukin-8, Cell Biology, Molecular biology, Open reading frame, genomic DNA, biology.protein, Cosmid, Chromosomes, Human, Pair 4, Chemokines, CXC, Transcription Factors

Abstract

The genomic DNA for ENA-78 has been obtained from a human chromosome 4 flow-sorted cosmid library. Three out of 25′000 screened single colonies yielded the same 2.2-kB EcoRI ENA-78 gene fragment. A similar size fragment was observed on genomic southern blots, suggesting the presence of a single ENA-78 gene. The transcriptional start site was localized using a 5′ RACE protocol on first strand cDNA prepared from stimulated alveolar type-II epithelial cell (A549) poly(A) mRNA. The ENA-78 gene contains four exons and three introns and the open reading frame of 342 nucleotides encodes for a protein of total 114 amino acids. The 5′ flanking region contains potential binding sites for several nuclear factors such as AP-2, NF-κB, and interferon regulatory factor-1.

Published

1994

102. Delineation of a 50 kilobase DNA segment containing the recombination site in a sporadic case of Huntington's disease

Author

Colin Collins, Michael R. Hayden, Rona K. Graham, J Theilmann, O. Riess, S E Andrew, Bernhard H. F. Weber, and Gerhard Wolff

Subjects

Adult, Genetic Markers, Male, Mutation rate, Molecular Sequence Data, Locus (genetics), Biology, chemistry.chemical_compound, Chromosome Walking, Huntington's disease, Genetics, medicine, Humans, Cloning, Molecular, Child, Gene, Alleles, Gene Rearrangement, Recombination, Genetic, Polymorphism, Genetic, Base Sequence, Haplotype, Chromosome Mapping, medicine.disease, Molecular biology, Telomere, Pedigree, Huntington Disease, chemistry, Haplotypes, Mutation, Female, Chromosomes, Human, Pair 4, Recombination, DNA

Abstract

No detectable rearrangements involving chromosome 4p16.3 have been observed in patients with Huntington's disease (HD). New mutations for HD could involve structural alterations which might aid the localization of the defective gene. We have reinvestigated a well documented sporadic case of HD. DNA haplotyping with markers between D4S10 and the telomeric locus D4S141 reveals a recombination event in one chromosome of the sporadic HD patient. The site of recombination maps within a 50 kilobase (kb) region, about 700 kb from the 4p telomere. Based on the extremely low HD mutation rate and significantly decreased recombination in the distal region of 4p, we hypothesize a direct link between the site of the recombination and HD in this patient.

Published

1992

103. Identification of multiple CpG islands and associated conserved sequences in a candidate region for the Huntington disease gene

Author

Colin Collins, Michael R. Hayden, David Kowbel, Bernhard H. F. Weber, and O. Riess

Subjects

Molecular Sequence Data, Restriction Mapping, Locus (genetics), Biology, Methylation, Conserved sequence, Chromosome Walking, Restriction map, Sequence Homology, Nucleic Acid, Genetics, Primer walking, Animals, Humans, Cloning, Molecular, Gene, Repetitive Sequences, Nucleic Acid, Contig, Base Sequence, DNA, Cosmids, Biological Evolution, Electrophoresis, Gel, Pulsed-Field, Restriction site, Huntington Disease, Cosmid, Chromosomes, Human, Pair 4, Dinucleoside Phosphates

Abstract

The HD locus has been assigned to 4p16.3 distal to the DNA segment D4S10. However, the precise location of this gene is still unknown. At least three regions, together encompassing more than 3.5 Mb of DNA, can still be considered as candidate regions for the HD gene. Our efforts are directed toward the cloning and the complete characterization of one of these regions. Thus far we have cloned 460 kb of DNA in contiguously overlapping cosmids distal to D4S111 and have developed a detailed long-range restriction map orienting the contig within the terminal region of 4p16.3. We characterized 15 CpG-rich islands defined by tightly clustered rare cutter restriction sites for the enzymes NotI, BssHII, EagI, NruI, and SacII. In addition, we show that the sequences associated with the CpG-rich islands detect cross-species conservation. The detailed genetic analysis of the 460-kb contig provides a framework for the identification of genes, which can be assessed for the characteristics expected for the HD gene.

Published

1991

104. The codon 408 mutation associated with haplotype 2 is predominant in Polish families with phenylketonuria

Author

Jadwiga Jaruzelska, Karen Friis Henriksen, Krzysztof Borski, Ryszard Słomski, Nikolaus Blin, Flemming Güttler, and O. Riess

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Linkage disequilibrium, Phenylalanine hydroxylase, Genetic Linkage, Restriction Mapping, Locus (genetics), Polymerase Chain Reaction, Phenylketonurias, Genotype, Genetics, Humans, Allele, Codon, Genetics (clinical), Alleles, biology, Incidence, Haplotype, nutritional and metabolic diseases, Phenylalanine Hydroxylase, Eastern european, Haplotypes, Mutation, biology.protein, Poland, Restriction fragment length polymorphism, Polymorphism, Restriction Fragment Length

Abstract

The incidence of phenylketonuria (PKU) in the western part of Poland is 1 in 5000 live births. Restriction fragment length polymorphism (RFLP) haplotypes at the phenylalanine hydroxylase locus have been analysed in 46 Polish families with PKU. Among 43 fully-informative families 16 RFLP haplotypes were identified. Haplotype 2 is the most frequently (62%) associated with Polish PKU alleles, and the codon 408 mutation is in complete linkage disequilibrium with this haplotype in Poland. This finding is in agreement with observations in other eastern European countries (German Democratic Republic, Czechoslovakia, and Hungary) and in contrast to the genotype distribution observed in western European countries. The present observation suggests the spread of classical PKU, due to the codon 408 mutation associated with haplotype 2, from east to west in European populations. Perhaps more important for genetic counselling, 62% of all PKU chromosomes in the Polish population can now be detected using only one mutant-specific oligonucleotide probe.

Published

1991

105. A polymorphic DNA marker at the D8S131 locus

Author

Bernhard H. F. Weber, O. Riess, C. N. Kreklywich, Michael R. Hayden, and Stephen Wood

Subjects

Genetic Markers, Genetics, ddc:610, Base Sequence, Molecular Sequence Data, 610 Medizin, Chromosome Mapping, Locus (genetics), Biology, Molecular biology, law.invention, Gene mapping, Genetic marker, law, Humans, Microsatellite, Restriction fragment length polymorphism, Allele, Allele frequency, Polymorphism, Restriction Fragment Length, Polymerase chain reaction, Chromosomes, Human, Pair 8

Published

1991

106. 3.002 PD: Genetics

Author

O. Riess and M. Yamamoto

Subjects

Genetics, Neurology, Neurology (clinical), Geriatrics and Gerontology, Biology

Published

2007

107. DNA analysis of Huntington’s disease

Author

Bernhard H. F. Weber, K. Marczinek, H. Weirich-Schwaiger, Deborah J. Morris-Rosendahl, Dagmar Nolte, G. Schluter, Christine Zühlke, M. Weigell-Weber, Ana Maria Menezes Vieira-Saecker, G. von Beust, Franco Laccone, U. Engel, K. Fuchs, O. Riess, Elke Holinski-Feder, University of Zurich, and Laccone, Franco

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Pathology, 10039 Institute of Medical Genetics, Population, 610 Medicine & health, 03 medical and health sciences, 0302 clinical medicine, Huntington's disease, Risk Factors, Germany, Epidemiology, Humans, Medicine, Family history, Predictive testing, education, Genetics (clinical), Alleles, Aged, Retrospective Studies, 0303 health sciences, Pregnancy, education.field_of_study, business.industry, Incidence (epidemiology), 030305 genetics & heredity, Retrospective cohort study, DNA, Middle Aged, medicine.disease, 3. Good health, 2728 Neurology (clinical), Huntington Disease, Tandem Repeat Sequences, Austria, 570 Life sciences, biology, Female, Neurology (clinical), business, Switzerland, 030217 neurology & neurosurgery

Abstract

Objective: To review the direct DNA testing for Huntington’s disease (HD) in Germany, Switzerland, and Austria from 1993 to 1997, and to analyze the population with regard to age structure, gender, and family history.Methods: Twelve laboratories (nine in Germany, two in Austria, and one in Switzerland) recorded data pertaining to repeat number, gender, age at molecular diagnosis, and family history of probands. The molecular test was categorized as either diagnostic (for symptomatic individuals), presymptomatic (for individuals at risk), and prenatal (for pregnancies at risk).Results: A total of 3,090 HD patients, 992 individuals at risk, and 24 fetuses were investigated using DNA analysis. The clinical diagnosis was confirmed in 65.6% of patients. A total of 38.5% of individuals at risk inherited an expanded CAG repeat. The female-to-male ratio showed a distinct predominance of women both in the diagnostic and presymptomatic groups. Of the fetuses tested, six were carriers of an expanded CAG repeat. Two pregnancies were interrupted; one pregnancy was not. No information about the parents’ decision was obtained for the remaining three pregnancies.Conclusions: Approximately 20% of the estimated 10,000 HD patients living in Germany, Switzerland, and Austria have been identified by DNA analysis (total population, approximately 100 million; incidence of HD, 1:10,000). Assuming a ratio of HD patients to individuals at risk of 1:3, approximately 30,000 individuals are, in principle, eligible for a presymptomatic test. Less than 3 to 4% of individuals at risk have requested a presymptomatic test. This shows that the assumed enormous request of predictive testing has not occurred. More surprisingly, prenatal diagnoses were found to be rare.

Published

1999

108. Subject Index Vol. 65, 1994

Author

R. Tupler, S.D. Wilton, G. Melmer, P.A. Akkari, I. Todorov, J.L. Cassady, D. Werner, M.A. Garrido-Ramos, N.A. Mazurok, D.A. Miller, L.L. Deaven, P.F.R. Little, M. Cortinovis, Y. Agid, P. Bouche, A. Blancher, O. Riess, N. Ravisé, J.-M. Blanchard, D.O. Weghuis, D. Francis, A. Plet, E.I. Yantsen, P.M.T. Deen, D.F. Callen, T.M. Fink, C. Meredith, P. Calvas, M Janson, M. Lafage-Pochitaloff, Angela Maria Vianna-Morgante, S. Kredtke, A. Geurts van Kessel, C.H. van Os, N.M. Matveeva, G. Chazot, M.-G. Mattéi, P.-M. Gonnaud, E.Kh. Ginsburg, Carla Rosenberg, N.G. Laing, S.M. Zakian, A. Mincheva, O.J. Miller, S.A. Lane, L. Tiepolo, M. Jamilena, David W. Hale, H.J. Eyre, M. Gugenheim, B. Chérif-Zahar, C. Bonnebouche, I. Siedlaczck, S.J. Goss, L. Kedes, A. Vandenberghe, B. Wieringa, E. Le Guern, A. Brice, C. Cerdan, S. Tardieu, D.I. Francis, R.A. Sturm, R. Lozano, F. Sturtz, E. Dainotti, M. Nordeskjöld, C. Ruiz Rejón, Q.-Q. Cai, Anne Lise Børresen, J.T. Epplen, I. Salvignol, P. Maraschio, R. Gouider, A.G. Shilov, M. Ruiz Rejón, J. Imbert, Peter Lichter, T.B. Nesterova, J.A.M. Graves, and D. Depétris

Subjects

Index (economics), Statistics, Genetics, Subject (documents), Biology, Molecular Biology, Genetics (clinical)

Published

1994

109. (CA)n-dinucleotide repeat at the PDEB locus in 4p16.3

Author

Hossein Daneshvar, Michael R. Hayden, Rona K. Graham, Bernhard H. F. Weber, and O. Riess

Subjects

Genetic Markers, Molecular Sequence Data, Locus (genetics), Biology, Polymerase Chain Reaction, Gene Frequency, Gene mapping, 3',5'-Cyclic-GMP Phosphodiesterases, Genetics, Humans, Base sequence, Allele, Repeated sequence, Molecular Biology, Gene, Allele frequency, Alleles, Genetics (clinical), Repetitive Sequences, Nucleic Acid, Polymorphism, Genetic, Base Sequence, General Medicine, Dinucleotide Repeat, Molecular biology, Genes, Oligodeoxyribonucleotides, Chromosomes, Human, Pair 4

Published

1993

110. 'The Middle East' The Problem of Geographic Terminology

Author

Richard O. Riess

Subjects

Middle East, Geography, Geography, Planning and Development, Ethnology, Far East, Earth-Surface Processes, Terminology

Published

1969

111. RELP-discordance within the human phenylalanine hydroxylase locus

Author

O. Riess, Jörg T. Epplen, Wolfgang Berger, Adelheid Michel, Peter Nürnberg, Astrid Speer, and Charles Coutelle

Subjects

Male, Genetics, Polymorphism, Genetic, Phenylalanine hydroxylase, biology, Phenylalanine Hydroxylase, Locus (genetics), DNA, Molecular biology, Pedigree, Chromosomal crossover, DNA profiling, Complementary DNA, biology.protein, Humans, Female, Crossing Over, Genetic, Restriction fragment length polymorphism, DNA Probes, Oligomer restriction, Molecular probe, Polymorphism, Restriction Fragment Length, Genetics (clinical)

Abstract

A search for crossover events was performed in seven families with two phenylketonuria-affected children applying seven enzymes for the detection of eight restriction fragment length polymorphisms (RFLPs) by hybridisation with a human phenylalanine hydroxylase (PAH) cDNA probe. A discordance was detected within the PvuIIb-RFLP pattern of two affected sibs. This observation is most likely the result of a cross-over event in the PAH locus. Alternative explanations are discussed. Non-paternity could be excluded by DNA fingerprinting using the oligonucleotide probe (GTG)5.

Published

1989

112. Ver�nderungen des Mineralsalzgehaltes der Darmschleimhaut nach peroraler Verabreichung von Mineralw�ssern. (Veraschungsmethode nach Liesegang.)

Author

O. Rieß and W. Strauch

Subjects

Gynecology, medicine.medical_specialty, Colloid and Surface Chemistry, Polymers and Plastics, Chemistry, Materials Chemistry, medicine, Physical and Theoretical Chemistry

Published

1939

113. Letters …

Author

Kirk H. Stone, Richard O. Riess, and Kenneth S. Fagg

Subjects

Geography, Planning and Development, Earth-Surface Processes

Published

1959

114. Prenatal diagnosis of classical phenylketonuria by linked restriction fragment length polymorphism analysis

Author

A. Michel, R. Hanke, R Neumann, A. Speer, O. Riess, G. Cobet, Ch. Coutelle, R. Bollman, and Ch. Bommer

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Phenylalanine hydroxylase, Prenatal diagnosis, HindIII, law.invention, Restriction fragment, law, Pregnancy, Complementary DNA, Phenylketonurias, Prenatal Diagnosis, Humans, Genetics (clinical), Genetics, Fetus, biology, Obstetrics and Gynecology, Nucleic Acid Hybridization, DNA, Molecular biology, Trophoblasts, Recombinant DNA, biology.protein, Autoradiography, Female, Restriction fragment length polymorphism, Polymorphism, Restriction Fragment Length

Abstract

Since the isolation of a recombinant containing a cDNA sequence for human phenylalanine hydroxylase (hPH) (Woo et al., 1983; Speer et al., 1986) prenatal diagnosis by linked restriction fragment length polymorphism (RFLPs) has become possible for families in which phenylketonuria (PKU) occurs (Lidsky et al., 1985a). We describe here the application of a Hind III three-allele RFLP in a single family, which allowed the prenatal diagnosis of an affected fetus.

Published

1986

115. Haplotype analysis of phenylalanine hydroxylase alleles in polish families with phenylketonuria

Author

J, Jaruzelska, K, Borski, O, Riess, N, Blin, and R, Słomski

Subjects

Male, Haplotypes, Phenylketonurias, Humans, Phenylalanine Hydroxylase, Female, Poland, Alleles, Polymorphism, Restriction Fragment Length

Abstract

Eight polymorphic restriction enzyme sites at phenylalanine hydroxylase locus from the parental chromosomes in Polish families with phenylketonuria were analyzed. Among 28 chromosomes studied, we identified haplotypes found within the Danish population. Haplotype 2 has been found in 25% of affected alleles. One of the patients studied is homozygous for this haplotype.

Published

1989

116. [Report of the Leipzig congress of internists]

Author

O, RIESS

Subjects

Physicians, Internal Medicine, Humans, Medicine, Germany, East, Congresses as Topic

Published

1951

117. [Regierungsrat Dr. phil. W. von Brehmer's method of diagnosing and curing cancer]

Author

O, RIESS

Subjects

Neoplasms, Humans

Published

1950

118. [Changes in theories on peptic ulcer]

Author

O, RIESS

Subjects

Peptic Ulcer, Humans

Published

1951

119. [Cancerogenic substances in food]

Author

O, RIESS

Subjects

Food, Neoplasms, Coloring Agents

Published

1950

120. [Spagirics]

Author

O, RIESS

Subjects

Medicine

Published

1950

121. [The importance of fluorines in modern therapy]

Author

O, RIESS

Subjects

Fluorides, Humans, Fluorine

Published

1950

122. Experimental investigations on Thomson's law of wave-motion on water

Author

O. Riess

Subjects

Physics, Classical mechanics, Wave motion

Abstract

n/a

Published

1891

123. [Human urine as a remedy]

Author

O, RIESS

Subjects

Humans, Urine, Body Fluids

Published

1950

124. The overheating bath, a natural healing method

Author

O, RIESS

Subjects

Humans, Baths, Hydrotherapy

Published

1948

125. Allelic distribution of CTG18.1 in Caucasian populations: Association studies in bipolar disorder, schizophrenia, and ataxia

Author

J. R. Depaulo, Sylvia G. Simpson, Melvin G. McInnis, O. Riess, R. L. Margolis, A. T. Mahoney, T. Swift-Scanlanl, Christopher A. Ross, Elliot S. Gershon, Francis J. McMahon, Haiming Chen, G. Verheyen, T. Hung Lan, L. Oruc, James L. Kennedy, C. Van Broeckhoven, D. F. MacKinnon, John I. Nurnberger, J. Vincent, and T. Reich

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Psychosis, Bipolar Disorder, Ataxia, Population, Linkage Disequilibrium, White People, Cellular and Molecular Neuroscience, Transcription Factor 4, Gene Frequency, Trinucleotide Repeats, medicine, Humans, Allele, education, Molecular Biology, Allele frequency, Alleles, Genetic association, Genetics, education.field_of_study, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, medicine.disease, Introns, DNA-Binding Proteins, Psychiatry and Mental health, Schizophrenia, Anticipation (genetics), Trans-Activators, Female, medicine.symptom, TCF Transcription Factors, Psychology, Transcription Factor 7-Like 2 Protein, Transcription Factors

Abstract

CTG18.1 is a highly polymorphic and unstable CTG repeat within an intron of the SEF2-1 gene. We tested the CTG18.1 repeat length in affective disorder, schizophrenia, and nonspecific ataxia; these diseases all have shown clinical evidence for anticipation. There was no difference in the allele frequencies comparing the controls and disease groups. The most common allele contains 11 CAGs (35%) followed by alleles with 14-17 CAGs (35%). There was no difference in the distribution of the alleles in the cases vs controls for ataxia (P = 0.11), affective disorders (P = 0.21), or schizophrenia (P = 0.26). The frequency of unstable CTG18.1 alleles was approximately 3% in a population of N. European descent and is not related to the phenotypes tested.

126. Ceruloplasmin gene variations and substantia nigra hyperechogenicity in Parkinson disease

Author

B. Zeiler, Uwe Walter, Helmine Hochstrasser, O. Riess, Daniela Berg, Peter Bauer, Jörg Spiegel, S. Behnke, Ilona Csoti, Antje Bornemann, Georg Becker, and Jens Pahnke

Subjects

Male, Pathology, medicine.medical_specialty, Ultrasonography, Doppler, Transcranial, Iron, DNA Mutational Analysis, Central nervous system, Mutation, Missense, Substantia nigra, Biology, Central nervous system disease, Pathogenesis, Degenerative disease, medicine, Humans, Point Mutation, Missense mutation, Chromatography, High Pressure Liquid, Aged, Ceruloplasmin, Genetic Variation, Parkinson Disease, Middle Aged, medicine.disease, Transcranial Doppler, Substantia Nigra, medicine.anatomical_structure, Amino Acid Substitution, biology.protein, Female, Lewy Bodies, Neurology (clinical), Polymorphism, Restriction Fragment Length

Abstract

Background: Transcranial ultrasound may be used to detect increased iron levels of the substantia nigra (SN) in patients with Parkinson disease (PD) and in control subjects. It is not known whether iron accumulation in PD is a primary or secondary phenomenon. However, sequence variations in genes involved in iron metabolism have been linked to basal ganglia disorders. One of these is ceruloplasmin (Cp), which is vitally involved in iron transport across the cell membrane. Methods: One hundred seventy-six patients with PD according to the UK Brain Bank criteria and 180 ethnically matched control subjects, who were previously examined for SN iron signal changes by transcranial ultrasound, were examined for mutations in the Cp gene using denaturing high-performance liquid chromatography and subsequent sequencing for verification of unequivocal signals. Immunohistochemistry of PD midbrains was performed to examine the presence of Cp in Lewy bodies. Results: Five novel missense variations were detected. One of these (I63T) was found in a single PD patient. A known variation (D554E) was significantly associated with PD and the ultrasound marker for increased SN iron levels. Moreover, a third sequence variation (R793H) was found to segregate with the ultrasound marker for increased iron levels in patients and control subjects. Immunohistochemistry demonstrated that Cp co-localizes with Lewy bodies in PD. Conclusions: Detection of sequence variations in a single Parkinson disease (PD) patient or associated with the ultrasound marker for increased substantia nigra iron levels and the presence of ceruloplasmin (Cp) immunoreactivity in Lewy bodies underline a suspected role for Cp in the pathogenesis of PD. Further functional analyses are warranted to investigate whether these variations are causally linked to the complex pathogenesis of PD in a subset of cases.

127. Trinucleotide repeat expansion in SCA17/TBP in white patients with Huntington's disease-like phenotype

Author

M. Scheible, Ullrich Wüllner, S. Bösch, Deborah J. Morris-Rosendahl, Peter Bauer, S. Liebscher, Bernhard H. F. Weber, Jörg T. Epplen, O. Riess, Helga Weirich-Schwaiger, Arndt Rolfs, Hartmut Peters, Elke Holinski-Feder, Franco Laccone, and J. Andrich

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Ataxia, Genotype, Choreiform movement, Biology, White People, Autosomal recessive trait, Atrophy, Huntington's disease, mental disorders, Genetics, medicine, Huntingtin Protein, Humans, Genetics (clinical), Base Sequence, Chorea, TATA-Box Binding Protein, medicine.disease, Huntington Disease, Phenotype, medicine.symptom, Trinucleotide Repeat Expansion, Trinucleotide repeat expansion, Letter to JMG

Abstract

Huntington’s disease (HD) is characterized by movement abnormalities and psychiatric symptoms. Prominent features include choreiform movements, dysarthria, ataxia, depression, dementia, and personality changes. The disease usually manifests during the third or fourth decade of live and progresses with dysphagia and subsequent cachexia causing death some 20 years later. Neuropathologically, the disease is characterized by atrophy of the caudate and putamen and, to a lesser extent, of the cortex, globus pallidum, thalamus, subthalamic region, and substantia nigra.1 A CAG repeat expansion in the HD gene resulting in an expanded polyglutamine chain in the huntingtin protein was identified as the major cause of HD.2 Phenocopies of HD have been described and designated as Huntington disease-like (HD-like). These disorders are genetically heterogeneous. In a consanguineous family of Saudi Arabian ancestry a juvenile-onset choreiform disease resembling HD was described, inherited as an autosomal recessive trait. The chromosomal mapping might point to 4p15.3, but still is controversial.3,4 In senile chorea, CAG repeat expansions in the HD gene have been excluded but a gene locus for this HD-like condition is not known.5 Several families have been reported with clinical features closely resembling HD and autosomal dominant inheritance. Among these, an early-onset non-progressive chorea with benign course has been associated with mutations in TITF-1 mapped …

128. Carl Haeberlin

Author

O. Riess

Subjects

General Medicine

Published

1940

129. Dynamics of cell-free tumor DNA correlate with early MRI response during chemoradiotherapy in rectal cancer.

Author

Clasen K, Gani C, Schuetz L, Clasen S, Ballin N, Bonzheim I, Orth M, Ossowski S, Riess O, Niyazi M, Schroeder C, and Kelemen O

Subjects

Humans, Male, Female, Middle Aged, Aged, Biomarkers, Tumor blood, Neoadjuvant Therapy, Adult, Prognosis, Pilot Projects, Rectal Neoplasms therapy, Rectal Neoplasms diagnostic imaging, Rectal Neoplasms pathology, Rectal Neoplasms blood, Chemoradiotherapy, Magnetic Resonance Imaging methods, Circulating Tumor DNA blood, Circulating Tumor DNA analysis

Abstract

Background: In locally advanced rectal cancer, the prediction of tumor response during and after neoadjuvant treatment remains challenging. In terms of organ preservation, adaptive radiotherapy, and intensified (total) neoadjuvant therapies, biomarkers are desirable for patient stratification., Methods: In 16 patients, weekly blood samples (n = 86) to detect cell-free tumor DNA (ctDNA) during long-course neoadjuvant chemoradiotherapy were analyzed. Data were correlated with initial tumor volumes, MRI response in week 2 and 5 of radiotherapy as well as with pathologic tumor response after resection and outcome parameters., Results: Most patients showed decreasing ctDNA during the course of radiochemotherapy. However, we found heterogenous dynamics of ctDNA and could identify three groups: (1) decline (2) no clear decline and/or late shedding (3) persistence of ctDNA. In seven patients we could detect significant amounts of ctDNA in week 5 or week 6 of treatment. In our pilot cohort, we did not find significant correlations of ctDNA dynamics with pathologic response or outcome parameters. However, patients with distinct decline of ctDNA had larger tumor volumes prior to treatment, and MRI imaging in week 2 and 5 revealed bigger absolute decrease of tumor volumes. If significant levels of ctDNA were found in week 5 and / or 6, patients showed less absolute tumor volume decrease in week 2 and 5., Conclusions: Weekly measurement of ctDNA during radiochemotherapy is feasible and might represent a promising biomarker. Bigger initial primary tumors showed different ctDNA shedding profiles compared with smaller primary tumors and correlations of ctDNA dynamics with early imaging response were found., (© 2024. The Author(s).)

Published

2024

130. Brain malformations and seizures by impaired chaperonin function of TRiC.

Author

Kraft F, Rodriguez-Aliaga P, Yuan W, Franken L, Zajt K, Hasan D, Lee TT, Flex E, Hentschel A, Innes AM, Zheng B, Julia Suh DS, Knopp C, Lausberg E, Krause J, Zhang X, Trapane P, Carroll R, McClatchey M, Fry AE, Wang L, Giesselmann S, Hoang H, Baldridge D, Silverman GA, Radio FC, Bertini E, Ciolfi A, Blood KA, de Sainte Agathe JM, Charles P, Bergant G, Čuturilo G, Peterlin B, Diderich K, Streff H, Robak L, Oegema R, van Binsbergen E, Herriges J, Saunders CJ, Maier A, Wolking S, Weber Y, Lochmüller H, Meyer S, Aleman A, Polavarapu K, Nicolas G, Goldenberg A, Guyant L, Pope K, Hehmeyer KN, Monaghan KG, Quade A, Smol T, Caumes R, Duerinckx S, Depondt C, Van Paesschen W, Rieubland C, Poloni C, Guipponi M, Arcioni S, Meuwissen M, Jansen AC, Rosenblum J, Haack TB, Bertrand M, Gerstner L, Magg J, Riess O, Schulz JB, Wagner N, Wiesmann M, Weis J, Eggermann T, Begemann M, Roos A, Häusler M, Schedl T, Tartaglia M, Bremer J, Pak SC, Frydman J, Elbracht M, and Kurth I

Subjects

Humans, Male, Fibroblasts metabolism, Intellectual Disability genetics, Intellectual Disability metabolism, Protein Subunits metabolism, Protein Subunits genetics, Proteome metabolism, Transcriptome, Magnetic Resonance Imaging, Caenorhabditis elegans, Adult, Brain abnormalities, Brain diagnostic imaging, Brain metabolism, Chaperonin Containing TCP-1 chemistry, Chaperonin Containing TCP-1 genetics, Chaperonin Containing TCP-1 metabolism, Protein Folding, Seizures diagnostic imaging, Seizures genetics, Seizures metabolism

Abstract

Malformations of the brain are common and vary in severity, from negligible to potentially fatal. Their causes have not been fully elucidated. Here, we report pathogenic variants in the core protein-folding machinery TRiC/CCT in individuals with brain malformations, intellectual disability, and seizures. The chaperonin TRiC is an obligate hetero-oligomer, and we identify variants in seven of its eight subunits, all of which impair function or assembly through different mechanisms. Transcriptome and proteome analyses of patient-derived fibroblasts demonstrate the various consequences of TRiC impairment. The results reveal an unexpected and potentially widespread role for protein folding in the development of the central nervous system and define a disease spectrum of "TRiCopathies."

Published

2024

131. Stratified analyses refine association between TLR7 rare variants and severe COVID-19.

Author

Boos J, van der Made CI, Ramakrishnan G, Coughlan E, Asselta R, Löscher BS, Valenti LVC, de Cid R, Bujanda L, Julià A, Pairo-Castineira E, Baillie JK, May S, Zametica B, Heggemann J, Albillos A, Banales JM, Barretina J, Blay N, Bonfanti P, Buti M, Fernandez J, Marsal S, Prati D, Ronzoni L, Sacchi N, Schultze JL, Riess O, Franke A, Rawlik K, Ellinghaus D, Hoischen A, Schmidt A, and Ludwig KU

Subjects

Humans, Male, Female, Middle Aged, Adult, Spain epidemiology, Case-Control Studies, Italy epidemiology, Aged, Severity of Illness Index, Genetic Variation genetics, Toll-Like Receptor 7 genetics, COVID-19 genetics, COVID-19 epidemiology, Genetic Predisposition to Disease, SARS-CoV-2 genetics

Abstract

Despite extensive global research into genetic predisposition for severe COVID-19, knowledge on the role of rare host genetic variants and their relation to other risk factors remains limited. Here, 52 genes with prior etiological evidence were sequenced in 1,772 severe COVID-19 cases and 5,347 population-based controls from Spain/Italy. Rare deleterious TLR7 variants were present in 2.4% of young (<60 years) cases with no reported clinical risk factors (n = 378), compared to 0.24% of controls (odds ratio [OR] = 12.3, p = 1.27 × 10 -10 ). Incorporation of the results of either functional assays or protein modeling led to a pronounced increase in effect size (OR max  = 46.5, p = 1.74 × 10 -15 ). Association signals for the X-chromosomal gene TLR7 were also detected in the female-only subgroup, suggesting the existence of additional mechanisms beyond X-linked recessive inheritance in males. Additionally, supporting evidence was generated for a contribution to severe COVID-19 of the previously implicated genes IFNAR2, IFIH1, and TBK1. Our results refine the genetic contribution of rare TLR7 variants to severe COVID-19 and strengthen evidence for the etiological relevance of genes in the interferon signaling pathway., Competing Interests: Declaration of interests K.U.L. is a co-founder of LAMPseq Diagnostics GmbH., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

132. Bridging the divide: addressing discrepancies between clinical guidelines, policy guidelines, and biomarker utilization.

Author

Horgan D, Hofman P, Buttner R, Rieß O, Lugowska I, Dube F, Singh J, Nadal E, Stokłosa T, Sīviņa E, Van der Buckle M, Mosoiu S, Bertolaccini L, Girard N, Meerbeeck JV, Omar I, Capoluongo ED, Bielack S, Hills T, Baldwin D, and Subbiah V

Abstract

Objectives: This paper aims to identify and address gaps in cancer treatment and diagnosis within European health services, focusing specifically on discrepancies between clinical guidelines and policy guidelines. It seeks to highlight how the underutilization of advanced diagnostic techniques recommended by medical societies contributes to missed opportunities for improving patient outcomes., Methods: A comprehensive analysis was conducted across multiple European countries to assess the compliance and integration of clinical guidelines with the availability of advanced diagnostic technologies. Secondary data related to clinical and policy guidelines in cancer care were collected and analyzed. Key indicators of adoption and utilization of next-generation sequencing and liquid biopsy were examined to evaluate their impact on health service efficiency and patient care., Results: The analysis revealed significant discrepancies between the recommendations of medical societies regarding advanced diagnostic techniques and their adoption in health policy decisions across Europe. Country-specific assessments indicated varying levels of alignment between clinical guidelines and the availability of advanced diagnostics. These findings underscored missed opportunities for optimizing patient care and health service efficiency through better alignment and integration of clinical guidelines with policy decisions., Conclusions: This study concludes that there is a critical need for health policy decision-makers to prioritize the adoption of clinical guidelines in resource allocation and health service organization. Greater attention to the recommendations of medical societies regarding advanced diagnostic techniques could significantly enhance diagnostic accuracy, treatment efficacy, and overall patient outcomes in cancer care. The paper advocates for policy reforms that acknowledge and leverage the potential benefits of advanced diagnostics in improving health service performance and patient-centered care across Europe., (© 2024 Walter de Gruyter GmbH, Berlin/Boston.)

Published

2024

133. The parkin V380L variant is a genetic modifier of Machado-Joseph disease with impact on mitophagy.

Author

Weber JJ, Czisch L, Pereira Sena P, Fath F, Huridou C, Schwarz N, Incebacak Eltemur RD, Würth A, Weishäupl D, Döcker M, Blumenstock G, Martins S, Sequeiros J, Rouleau GA, Jardim LB, Saraiva-Pereira ML, França MC Jr, Gordon CR, Zaltzman R, Cornejo-Olivas MR, van de Warrenburg BPC, Durr A, Brice A, Bauer P, Klockgether T, Schöls L, Riess O, and Schmidt T

Subjects

Humans, Male, Female, Middle Aged, Adult, Polymorphism, Single Nucleotide, Ataxin-3 genetics, Age of Onset, Repressor Proteins, Machado-Joseph Disease genetics, Machado-Joseph Disease pathology, Ubiquitin-Protein Ligases genetics, Mitophagy genetics, Mitophagy physiology

Abstract

Machado-Joseph disease (MJD) is an autosomal dominant neurodegenerative spinocerebellar ataxia caused by a polyglutamine-coding CAG repeat expansion in the ATXN3 gene. While the CAG length correlates negatively with the age at onset, it accounts for approximately 50% of its variability only. Despite larger efforts in identifying contributing genetic factors, candidate genes with a robust and plausible impact on the molecular pathogenesis of MJD are scarce. Therefore, we analysed missense single nucleotide polymorphism variants in the PRKN gene encoding the Parkinson's disease-associated E3 ubiquitin ligase parkin, which is a well-described interaction partner of the MJD protein ataxin-3, a deubiquitinase. By performing a correlation analysis in the to-date largest MJD cohort of more than 900 individuals, we identified the V380L variant as a relevant factor, decreasing the age at onset by 3 years in homozygous carriers. Functional analysis in an MJD cell model demonstrated that parkin V380L did not modulate soluble or aggregate levels of ataxin-3 but reduced the interaction of the two proteins. Moreover, the presence of parkin V380L interfered with the execution of mitophagy-the autophagic removal of surplus or damaged mitochondria-thereby compromising cell viability. In summary, we identified the V380L variant in parkin as a genetic modifier of MJD, with negative repercussions on its molecular pathogenesis and disease age at onset., (© 2024. The Author(s).)

Published

2024

134. Next-generation phenotyping integrated in a national framework for patients with ultrarare disorders improves genetic diagnostics and yields new molecular findings.

Author

Schmidt A, Danyel M, Grundmann K, Brunet T, Klinkhammer H, Hsieh TC, Engels H, Peters S, Knaus A, Moosa S, Averdunk L, Boschann F, Sczakiel HL, Schwartzmann S, Mensah MA, Pantel JT, Holtgrewe M, Bösch A, Weiß C, Weinhold N, Suter AA, Stoltenburg C, Neugebauer J, Kallinich T, Kaindl AM, Holzhauer S, Bührer C, Bufler P, Kornak U, Ott CE, Schülke M, Nguyen HHP, Hoffjan S, Grasemann C, Rothoeft T, Brinkmann F, Matar N, Sivalingam S, Perne C, Mangold E, Kreiss M, Cremer K, Betz RC, Mücke M, Grigull L, Klockgether T, Spier I, Heimbach A, Bender T, Brand F, Stieber C, Morawiec AM, Karakostas P, Schäfer VS, Bernsen S, Weydt P, Castro-Gomez S, Aziz A, Grobe-Einsler M, Kimmich O, Kobeleva X, Önder D, Lesmann H, Kumar S, Tacik P, Basin MA, Incardona P, Lee-Kirsch MA, Berner R, Schuetz C, Körholz J, Kretschmer T, Di Donato N, Schröck E, Heinen A, Reuner U, Hanßke AM, Kaiser FJ, Manka E, Munteanu M, Kuechler A, Cordula K, Hirtz R, Schlapakow E, Schlein C, Lisfeld J, Kubisch C, Herget T, Hempel M, Weiler-Normann C, Ullrich K, Schramm C, Rudolph C, Rillig F, Groffmann M, Muntau A, Tibelius A, Schwaibold EMC, Schaaf CP, Zawada M, Kaufmann L, Hinderhofer K, Okun PM, Kotzaeridou U, Hoffmann GF, Choukair D, Bettendorf M, Spielmann M, Ripke A, Pauly M, Münchau A, Lohmann K, Hüning I, Hanker B, Bäumer T, Herzog R, Hellenbroich Y, Westphal DS, Strom T, Kovacs R, Riedhammer KM, Mayerhanser K, Graf E, Brugger M, Hoefele J, Oexle K, Mirza-Schreiber N, Berutti R, Schatz U, Krenn M, Makowski C, Weigand H, Schröder S, Rohlfs M, Vill K, Hauck F, Borggraefe I, Müller-Felber W, Kurth I, Elbracht M, Knopp C, Begemann M, Kraft F, Lemke JR, Hentschel J, Platzer K, Strehlow V, Abou Jamra R, Kehrer M, Demidov G, Beck-Wödl S, Graessner H, Sturm M, Zeltner L, Schöls LJ, Magg J, Bevot A, Kehrer C, Kaiser N, Turro E, Horn D, Grüters-Kieslich A, Klein C, Mundlos S, Nöthen M, Riess O, Meitinger T, Krude H, Krawitz PM, Haack T, Ehmke N, and Wagner M

Subjects

Humans, Female, Male, Child, Germany, Exome Sequencing methods, Adolescent, Genetic Association Studies methods, Genetic Testing methods, Child, Preschool, Prospective Studies, Adult, Neurodevelopmental Disorders genetics, Neurodevelopmental Disorders diagnosis, Infant, Young Adult, Phenotype, High-Throughput Nucleotide Sequencing methods

Abstract

Individuals with ultrarare disorders pose a structural challenge for healthcare systems since expert clinical knowledge is required to establish diagnoses. In TRANSLATE NAMSE, a 3-year prospective study, we evaluated a novel diagnostic concept based on multidisciplinary expertise in Germany. Here we present the systematic investigation of the phenotypic and molecular genetic data of 1,577 patients who had undergone exome sequencing and were partially analyzed with next-generation phenotyping approaches. Molecular genetic diagnoses were established in 32% of the patients totaling 370 distinct molecular genetic causes, most with prevalence below 1:50,000. During the diagnostic process, 34 novel and 23 candidate genotype-phenotype associations were identified, mainly in individuals with neurodevelopmental disorders. Sequencing data of the subcohort that consented to computer-assisted analysis of their facial images with GestaltMatcher could be prioritized more efficiently compared with approaches based solely on clinical features and molecular scores. Our study demonstrates the synergy of using next-generation sequencing and phenotyping for diagnosing ultrarare diseases in routine healthcare and discovering novel etiologies by multidisciplinary teams., (© 2024. The Author(s).)

Published

2024

135. ZSCAN10 deficiency causes a neurodevelopmental disorder with characteristic oto-facial malformations.

Author

Laugwitz L, Cheng F, Collins SC, Hustinx A, Navarro N, Welsch S, Cox H, Hsieh TC, Vijayananth A, Buchert R, Bender B, Efthymiou S, Murphy D, Zafar F, Rana N, Grasshoff U, Falb RJ, Grimmel M, Seibt A, Zheng W, Ghaedi H, Thirion M, Couette S, Azizimalamiri R, Sadeghian S, Galehdari H, Zamani M, Zeighami J, Sedaghat A, Ramshe SM, Zare A, Alipoor B, Klee D, Sturm M, Ossowski S, Houlden H, Riess O, Wieczorek D, Gavin R, Maroofian R, Krawitz P, Yalcin B, Distelmaier F, and Haack TB

Subjects

Adolescent, Animals, Child, Child, Preschool, Female, Humans, Infant, Male, Mice, Transcription Factors genetics, Mice, Knockout, Neurodevelopmental Disorders genetics, Neurodevelopmental Disorders pathology

Abstract

Neurodevelopmental disorders are major indications for genetic referral and have been linked to more than 1500 loci including genes encoding transcriptional regulators. The dysfunction of transcription factors often results in characteristic syndromic presentations; however, at least half of these patients lack a genetic diagnosis. The implementation of machine learning approaches has the potential to aid in the identification of new disease genes and delineate associated phenotypes. Next generation sequencing was performed in seven affected individuals with neurodevelopmental delay and dysmorphic features. Clinical characterization included reanalysis of available neuroimaging datasets and 2D portrait image analysis with GestaltMatcher. The functional consequences of ZSCAN10 loss were modelled in mouse embryonic stem cells (mESCs), including a knockout and a representative ZSCAN10 protein truncating variant. These models were characterized by gene expression and western blot analyses, chromatin immunoprecipitation and quantitative PCR (ChIP-qPCR) and immunofluorescence staining. Zscan10 knockout mouse embryos were generated and phenotyped. We prioritized bi-allelic ZSCAN10 loss-of-function variants in seven affected individuals from five unrelated families as the underlying molecular cause. RNA-sequencing analyses in Zscan10-/- mESCs indicated dysregulation of genes related to stem cell pluripotency. In addition, we established in mESCs the loss-of-function mechanism for a representative human ZSCAN10 protein truncating variant by showing alteration of its expression levels and subcellular localization, interfering with its binding to DNA enhancer targets. Deep phenotyping revealed global developmental delay, facial asymmetry and malformations of the outer ear as consistent clinical features. Cerebral MRI showed dysplasia of the semicircular canals as an anatomical correlate of sensorineural hearing loss. Facial asymmetry was confirmed as a clinical feature by GestaltMatcher and was recapitulated in the Zscan10 mouse model along with inner and outer ear malformations. Our findings provide evidence of a novel syndromic neurodevelopmental disorder caused by bi-allelic loss-of-function variants in ZSCAN10., (© The Author(s) 2024. Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2024

136. Model matchmaking via the Solve-RD Rare Disease Models & Mechanisms Network (RDMM-Europe).

Author

Ellwanger K, Brill JA, de Boer E, Efthymiou S, Elgersma Y, Icmat M, Lecoquierre F, Lobato AG, Morleo M, Ori M, Schaffer AE, Vitobello A, Wells S, Yalcin B, Zhai RG, Sturm M, Zurek B, Graessner H, Bermejo-Sánchez E, Evangelista T, Hoogerbrugge N, Nigro V, Schüle R, Verloes A, Brunner H, Campeau PM, Lasko P, and Riess O

Subjects

Animals, Europe, Humans, Disease Models, Animal, Rare Diseases

Published

2024

137. A Novel PINK1 p.F385S Loss-of-Function Mutation in an Indian Family with Parkinson's Disease.

Author

Sharma K, Kishore A, Lechado-Terradas A, Passannanti R, Raimondi F, Sturm M, Sreelatha AAK, Puthenveedu DK, Sarma G, Casadei N, Krüger R, Gasser T, Kahle P, Riess O, Fitzgerald JC, and Sharma M

Subjects

Humans, India, Female, Male, Middle Aged, Loss of Function Mutation genetics, Adult, Ubiquitin-Protein Ligases genetics, Mutation genetics, Exome Sequencing, Mitophagy genetics, Protein Kinases genetics, Parkinson Disease genetics, Pedigree

Abstract

Background: Most Parkinson's disease (PD) loci have shown low prevalence in the Indian population, highlighting the need for further research., Objective: The aim of this study was to characterize a novel phosphatase tensin homolog-induced serine/threonine kinase 1 (PINK1) mutation causing PD in an Indian family., Methods: Exome sequencing of a well-characterized Indian family with PD. A novel PINK1 mutation was studied by in silico modeling using AlphaFold2, expression of mutant PINK1 in human cells depleted of functional endogenous PINK1, followed by quantitative image analysis and biochemical assessment., Results: We identified a homozygous chr1:20648535-20648535 T>C on GRCh38 (p.F385S) mutation in exon 6 of PINK1, which was absent in 1029 genomes from India and in other known databases. PINK1 F385S lies within the highly conserved DFG motif, destabilizes its active state, and impairs phosphorylation of ubiquitin at serine 65 and proper engagement of parkin upon mitochondrial depolarization., Conclusions: We characterized a novel nonconservative mutation in the DFG motif of PINK1, which causes loss of its ubiquitin kinase activity and inhibition of mitophagy. © 2024 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society., (© 2024 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.)

Published

2024

138. A GGC-repeat expansion in ZFHX3 encoding polyglycine causes spinocerebellar ataxia type 4 and impairs autophagy.

Author

Figueroa KP, Gross C, Buena-Atienza E, Paul S, Gandelman M, Kakar N, Sturm M, Casadei N, Admard J, Park J, Zühlke C, Hellenbroich Y, Pozojevic J, Balachandran S, Händler K, Zittel S, Timmann D, Erdlenbruch F, Herrmann L, Feindt T, Zenker M, Klopstock T, Dufke C, Scoles DR, Koeppen A, Spielmann M, Riess O, Ossowski S, Haack TB, and Pulst SM

Subjects

Humans, Male, Female, Induced Pluripotent Stem Cells metabolism, Autophagy genetics, Pedigree, Trinucleotide Repeat Expansion genetics, Homeodomain Proteins genetics, Spinocerebellar Ataxias genetics

Abstract

Despite linkage to chromosome 16q in 1996, the mutation causing spinocerebellar ataxia type 4 (SCA4), a late-onset sensory and cerebellar ataxia, remained unknown. Here, using long-read single-strand whole-genome sequencing (LR-GS), we identified a heterozygous GGC-repeat expansion in a large Utah pedigree encoding polyglycine (polyG) in zinc finger homeobox protein 3 (ZFHX3), also known as AT-binding transcription factor 1 (ATBF1). We queried 6,495 genome sequencing datasets and identified the repeat expansion in seven additional pedigrees. Ultrarare DNA variants near the repeat expansion indicate a common distant founder event in Sweden. Intranuclear ZFHX3-p62-ubiquitin aggregates were abundant in SCA4 basis pontis neurons. In fibroblasts and induced pluripotent stem cells, the GGC expansion led to increased ZFHX3 protein levels and abnormal autophagy, which were normalized with small interfering RNA-mediated ZFHX3 knockdown in both cell types. Improving autophagy points to a therapeutic avenue for this novel polyG disease. The coding GGC-repeat expansion in an extremely G+C-rich region was not detectable by short-read whole-exome sequencing, which demonstrates the power of LR-GS for variant discovery., (© 2024. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2024

139. RFC1 repeat expansions in downbeat nystagmus syndromes: frequency and phenotypic profile.

Author

Pellerin D, Heindl F, Traschütz A, Rujescu D, Hartmann AM, Brais B, Houlden H, Dufke C, Riess O, Haack T, Strupp M, and Synofzik M

Subjects

Humans, Male, Female, Middle Aged, Adult, Aged, DNA Repeat Expansion genetics, Fibroblast Growth Factors genetics, Young Adult, Bilateral Vestibulopathy genetics, Bilateral Vestibulopathy physiopathology, Replication Protein C genetics, Phenotype, Nystagmus, Pathologic genetics

Abstract

Objectives: The cause of downbeat nystagmus (DBN) remains unknown in a substantial number of patients ("idiopathic"), although intronic GAA expansions in FGF14 have recently been shown to account for almost 50% of yet idiopathic cases. Here, we hypothesized that biallelic RFC1 expansions may also represent a recurrent cause of DBN syndrome., Methods: We genotyped the RFC1 repeat and performed in-depth phenotyping in 203 patients with DBN, including 65 patients with idiopathic DBN, 102 patients carrying an FGF14 GAA expansion, and 36 patients with presumed secondary DBN., Results: Biallelic RFC1 AAGGG expansions were identified in 15/65 patients with idiopathic DBN (23%). None of the 102 GAA-FGF14-positive patients, but 2/36 (6%) of patients with presumed secondary DBN carried biallelic RFC1 expansions. The DBN syndrome in RFC1-positive patients was characterized by additional cerebellar impairment in 100% (15/15), bilateral vestibulopathy (BVP) in 100% (15/15), and polyneuropathy in 80% (12/15) of cases. Compared to GAA-FGF14-positive and genetically unexplained patients, RFC1-positive patients had significantly more frequent neuropathic features on examination and BVP. Furthermore, vestibular function, as measured by the video head impulse test, was significantly more impaired in RFC1-positive patients., Discussion: Biallelic RFC1 expansions are a common monogenic cause of DBN syndrome., (© 2024. The Author(s).)

Published

2024

140. Resequencing the complete SNCA locus in Indian patients with Parkinson's disease.

Author

Kishore A, Sturm M, Soman Pillai K, Hakkaart C, Kalikavil Puthanveedu D, Urulangodi M, Krishnan S, Ashok Kumar Sreelatha A, Rajan R, Pal PK, Yadav R, Sarma G, Casadei N, Gasser T, Bauer P, Riess O, and Sharma M

Abstract

The genetic loci implicated in familial Parkinson's disease (PD) have limited generalizability to the Indian PD population. We tested mutations and the frequency of known mutations in the SNCA gene in a PD cohort from India. We selected 298 PD cases and 301 age-matched controls for targeted resequencing (before QC), along with 363 PD genomes of Indian ancestry and 1029 publicly available whole genomes from India as healthy controls (IndiGenomes), to determine the frequency of monogenic SNCA mutations. The raw sequence reads were analyzed using an in-house analysis pipeline, allowing the detection of small variants and structural variants using Manta. The in-depth analysis of the SNCA locus did not identify missense or structural variants, including previously identified SNCA mutations, in the Indian population. The familial forms of SNCA gene variants do not play a major role in the Indian PD population and this warrants further research in the under-represented population., (© 2024. The Author(s).)

Published

2024

141. Blood and cerebellar abundance of ATXN3 splice variants in spinocerebellar ataxia type 3/Machado-Joseph disease.

Author

Raposo M, Hübener-Schmid J, Tagett R, Ferreira AF, Vieira Melo AR, Vasconcelos J, Pires P, Kay T, Garcia-Moreno H, Giunti P, Santana MM, Pereira de Almeida L, Infante J, van de Warrenburg BP, de Vries JJ, Faber J, Klockgether T, Casadei N, Admard J, Schöls L, Riess O, Costa MDC, and Lima M

Subjects

Humans, Ataxin-3 genetics, Ataxin-3 metabolism, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Cerebellum pathology, Protein Isoforms genetics, Protein Isoforms metabolism, Repressor Proteins genetics, Repressor Proteins metabolism, Machado-Joseph Disease metabolism

Abstract

Spinocerebellar ataxia type 3 (SCA3)/Machado-Joseph disease (MJD) is a heritable proteinopathy disorder, whose causative gene, ATXN3, undergoes alternative splicing. Ataxin-3 protein isoforms differ in their toxicity, suggesting that certain ATXN3 splice variants may be crucial in driving the selective toxicity in SCA3. Using RNA-seq datasets we identified and determined the abundance of annotated ATXN3 transcripts in blood (n = 60) and cerebellum (n = 12) of SCA3 subjects and controls. The reference transcript (ATXN3-251), translating into an ataxin-3 isoform harbouring three ubiquitin-interacting motifs (UIMs), showed the highest abundance in blood, while the most abundant transcript in the cerebellum (ATXN3-208) was of unclear function. Noteworthy, two of the four transcripts that encode full-length ataxin-3 isoforms but differ in the C-terminus were strongly related with tissue expression specificity: ATXN3-251 (3UIM) was expressed in blood 50-fold more than in the cerebellum, whereas ATXN3-214 (2UIM) was expressed in the cerebellum 20-fold more than in the blood. These findings shed light on ATXN3 alternative splicing, aiding in the comprehension of SCA3 pathogenesis and providing guidance in the design of future ATXN3 mRNA-lowering therapies., Competing Interests: Declaration of competing interest TK is receiving research support from the Bundesministerium für Bildung und Forschung (BMBF), the National Institutes of Health (NIH) and Servier. Within the last 24 months, he has received consulting fees from Biogen, UCB and Vico Therapeutics. BvdW is supported by grants from ZonMw, NOW, Hersenstichting, Gossweiler Foundation, and Radboud university medical center; he has served on the scientific advisory boards or steering committees of uniQure, VICO Therapeutics, and Servier. LS is receiving research support from the European Commission, the Bundesministerium für Bildung und Forschung (BMBF) and the Bundesministerium für Gesundheit (BMG) as well as the Deutsche Forschungsgemeinschaft (DFG), Servier and Vigil Neuroscience. Within the last 24 months, he has received consulting fees from Vico Therapeutics. The remaining authors declare that they have nothing to report., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

142. Genomes in clinical care.

Author

Riess O, Sturm M, Menden B, Liebmann A, Demidov G, Witt D, Casadei N, Admard J, Schütz L, Ossowski S, Taylor S, Schaffer S, Schroeder C, Dufke A, and Haack T

Abstract

In the era of precision medicine, genome sequencing (GS) has become more affordable and the importance of genomics and multi-omics in clinical care is increasingly being recognized. However, how to scale and effectively implement GS on an institutional level remains a challenge for many. Here, we present Genome First and Ge-Med, two clinical implementation studies focused on identifying the key pillars and processes that are required to make routine GS and predictive genomics a reality in the clinical setting. We describe our experience and lessons learned for a variety of topics including test logistics, patient care processes, data reporting, and infrastructure. Our model of providing clinical care and comprehensive genomic analysis from a single source may be used by other centers with a similar structure to facilitate the implementation of omics-based personalized health concepts in medicine., (© 2024. The Author(s).)

Published

2024

143. Stage-Dependent Biomarker Changes in Spinocerebellar Ataxia Type 3.

Author

Faber J, Berger M, Wilke C, Hubener-Schmid J, Schaprian T, Santana MM, Grobe-Einsler M, Onder D, Koyak B, Giunti P, Garcia-Moreno H, Gonzalez-Robles C, Lima M, Raposo M, Melo ARV, de Almeida LP, Silva P, Pinto MM, van de Warrenburg BP, van Gaalen J, de Vries J, Oz G, Joers JM, Synofzik M, Schols L, Riess O, Infante J, Manrique L, Timmann D, Thieme A, Jacobi H, Reetz K, Dogan I, Onyike C, Povazan M, Schmahmann J, Ratai EM, Schmid M, and Klockgether T

Subjects

Humans, Cross-Sectional Studies, Ataxia, Biomarkers, Machado-Joseph Disease genetics, Cerebellar Ataxia

Abstract

Spinocerebellar ataxia type 3/Machado-Joseph disease is the most common autosomal dominant ataxia. In view of the development of targeted therapies, knowledge of early biomarker changes is needed. We analyzed cross-sectional data of 292 spinocerebellar ataxia type 3/Machado-Joseph disease mutation carriers. Blood concentrations of mutant ATXN3 were high before and after ataxia onset, whereas neurofilament light deviated from normal 13.3 years before onset. Pons and cerebellar white matter volumes decreased and deviated from normal 2.2 years and 0.6 years before ataxia onset. We propose a staging model of spinocerebellar ataxia type 3/Machado-Joseph disease that includes a biomarker stage characterized by objective indicators of neurodegeneration before ataxia onset. ANN NEUROL 2024;95:400-406., (© 2023 The Authors. Annals of Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association.)

Published

2024

144. Augmenting MEK inhibitor efficacy in BRAF wild-type melanoma: synergistic effects of disulfiram combination therapy.

Author

Meraz-Torres F, Niessner H, Plöger S, Riel S, Schörg B, Casadei N, Kneilling M, Schaller M, Flatz L, Macek B, Eigentler T, Rieß O, Garbe C, Amaral T, and Sinnberg T

Subjects

Humans, Animals, Mice, Proto-Oncogene Proteins B-raf, Copper, Ditiocarb, Disease Models, Animal, Mitogen-Activated Protein Kinase Kinases, Disulfiram, Melanoma

Abstract

Background: MEK inhibitors (MEKi) were shown to be clinically insufficiently effective in patients suffering from BRAF wild-type (BRAF WT) melanoma, even if the MAPK pathway was constitutively activated due to mutations in NRAS or NF-1. Thus, novel combinations are needed to increase the efficacy and duration of response to MEKi in BRAF WT melanoma. Disulfiram and its metabolite diethyldithiocarbamate are known to have antitumor effects related to cellular stress, and induction of endoplasmic reticulum (ER) stress was found to synergize with MEK inhibitors in NRAS-mutated melanoma cells. Therefore, we investigated the combination of both therapeutics to test their effects on BRAF-WT melanoma cells and compared them with monotherapy using the MEKi trametinib., Methods: The effects of combined therapy with disulfiram or its metabolite diethyldithiocarbamate and the MEKi trametinib were evaluated in a series of BRAF-WT melanoma cell lines by measuring cell viability and apoptosis induction. Cytotoxicity was additionally assessed in 3D spheroids, ex vivo melanoma slice cultures, and in vivo xenograft mouse models. The response of melanoma cells to treatment was studied at the RNA and protein levels to decipher the mode of action. Intracellular and intratumoral copper measurements were performed to investigate the role of copper ions in the antitumor cytotoxicity of disulfiram and its combination with the MEKi., Results: Diethyldithiocarbamate enhanced trametinib-induced cytotoxicity and apoptosis induction in 2D and 3D melanoma culture models. Mechanistically, copper-dependent induction of oxidative stress and ER stress led to Janus kinase (JNK)-mediated apoptosis in melanoma cells. This mechanism was also detectable in patient-derived xenograft melanoma models and resulted in a significantly improved therapeutic effect compared to monotherapy with the MEKi trametinib., Conclusions: Disulfiram and its metabolite represent an attractive pharmaceutical approach to induce ER stress in melanoma cells that potentiates the antitumor effect of MEK inhibition and may be an interesting candidate for combination therapy of BRAF WT melanoma., (© 2024. The Author(s).)

Published

2024

145. Diagnostic genome sequencing improves diagnostic yield: a prospective single-centre study in 1000 patients with inherited eye diseases.

Author

Weisschuh N, Mazzola P, Zuleger T, Schaeferhoff K, Kühlewein L, Kortüm F, Witt D, Liebmann A, Falb R, Pohl L, Reith M, Stühn LG, Bertrand M, Müller A, Casadei N, Kelemen O, Kelbsch C, Kernstock C, Richter P, Sadler F, Demidov G, Schütz L, Admard J, Sturm M, Grasshoff U, Tonagel F, Heinrich T, Nasser F, Wissinger B, Ossowski S, Kohl S, Riess O, Stingl K, and Haack TB

Subjects

Humans, Prospective Studies, Base Sequence, RNA, Exome, Eye Diseases diagnosis, Eye Diseases genetics

Abstract

Purpose: Genome sequencing (GS) is expected to reduce the diagnostic gap in rare disease genetics. We aimed to evaluate a scalable framework for genome-based analyses 'beyond the exome' in regular care of patients with inherited retinal degeneration (IRD) or inherited optic neuropathy (ION)., Methods: PCR-free short-read GS was performed on 1000 consecutive probands with IRD/ION in routine diagnostics. Complementary whole-blood RNA-sequencing (RNA-seq) was done in a subset of 74 patients. An open-source bioinformatics analysis pipeline was optimised for structural variant (SV) calling and combined RNA/DNA variation interpretation., Results: A definite genetic diagnosis was established in 57.4% of cases. For another 16.7%, variants of uncertain significance were identified in known IRD/ION genes, while the underlying genetic cause remained unresolved in 25.9%. SVs or alterations in non-coding genomic regions made up for 12.7% of the observed variants. The RNA-seq studies supported the classification of two unclear variants., Conclusion: GS is feasible in clinical practice and reliably identifies causal variants in a substantial proportion of individuals. GS extends the diagnostic yield to rare non-coding variants and enables precise determination of SVs. The added diagnostic value of RNA-seq is limited by low expression levels of the major IRD disease genes in blood., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2024

146. A further case of AFG2B-related neurodevelopmental disorder with hearing loss and microcephaly allows further clarification of pathogenicity of the variant c.1313T>C, p.(Leu438Pro).

Author

Grosch S, Kehrer M, Riess O, Bevot A, and Haack TB

Subjects

Humans, Female, Middle Aged, Virulence, Microcephaly genetics, Microcephaly pathology, Neurodevelopmental Disorders genetics, Nervous System Malformations, Deafness

Abstract

Background: Bi-allelic variants in AFG2B (previously known as SPATA5L1) have recently been associated with a neurodevelopmental disorder with hearing loss and spasticity, as well as isolated hearing loss. We report on a 6 1/2-year-old girl with a history of global developmental delay, subsequent intellectual disability without relevant language acquisition, sensorineural hearing loss, muscular hypotonia and microcephaly., Methods: We performed trio exome sequencing on the patient and her parents., Results: Trio exome sequencing revealed likely pathogenic compound heterozygous missense variants in AFG2B [c.527G>T, p.(Gly176Val) and c.1313T>C, p.(Leu438Pro)] in the patient., Conclusion: Of note, the change c.1313T>C, p.(Leu438Pro) has been observed in a previously published patient as part of a complex disease allele along with a second homozygous missense change, so the exact contribution of the two alterations to this patient's disease had initially remained unclear. Our results support the pathogenic relevance of the c.1313T>C, p.(Leu438Pro) allele while providing detailed insights into the disease manifestation of a further patient., (© 2023 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals LLC.)

Published

2024

147. Blood transcriptome sequencing identifies biomarkers able to track disease stages in spinocerebellar ataxia type 3.

Author

Raposo M, Hübener-Schmid J, Ferreira AF, Vieira Melo AR, Vasconcelos J, Pires P, Kay T, Garcia-Moreno H, Giunti P, Santana MM, Pereira de Almeida L, Infante J, van de Warrenburg BP, de Vries JJ, Faber J, Klockgether T, Casadei N, Admard J, Schöls L, Riess O, and Lima M

Subjects

Humans, Transcriptome, Ataxin-3 genetics, Biomarkers, Adaptor Proteins, Signal Transducing genetics, Microtubule-Associated Proteins metabolism, Microfilament Proteins genetics, Intracellular Signaling Peptides and Proteins genetics, Machado-Joseph Disease genetics, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias complications

Abstract

Transcriptional dysregulation has been described in spinocerebellar ataxia type 3/Machado-Joseph disease (SCA3/MJD), an autosomal dominant ataxia caused by a polyglutamine expansion in the ataxin-3 protein. As ataxin-3 is ubiquitously expressed, transcriptional alterations in blood may reflect early changes that start before clinical onset and might serve as peripheral biomarkers in clinical and research settings. Our goal was to describe enriched pathways and report dysregulated genes, which can track disease onset, severity or progression in carriers of the ATXN3 mutation (pre-ataxic subjects and patients). Global dysregulation patterns were identified by RNA sequencing of blood samples from 40 carriers of ATXN3 mutation and 20 controls and further compared with transcriptomic data from post-mortem cerebellum samples of MJD patients and controls. Ten genes-ABCA1, CEP72, PTGDS, SAFB2, SFSWAP, CCDC88C, SH2B1, LTBP4, MEG3 and TSPOAP1-whose expression in blood was altered in the pre-ataxic stage and simultaneously, correlated with ataxia severity in the overt disease stage, were analysed by quantitative real-time PCR in blood samples from an independent set of 170 SCA3/MJD subjects and 57 controls. Pathway enrichment analysis indicated the Gαi signalling and the oestrogen receptor signalling to be similarly affected in blood and cerebellum. SAFB2, SFSWAP and LTBP4 were consistently dysregulated in pre-ataxic subjects compared to controls, displaying a combined discriminatory ability of 79%. In patients, ataxia severity was associated with higher levels of MEG3 and TSPOAP1. We propose expression levels of SAFB2, SFSWAP and LTBP4 as well as MEG3 and TSPOAP1 as stratification markers of SCA3/MJD progression, deserving further validation in longitudinal studies and in independent cohorts., (© The Author(s) 2023. Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2023

148. Clinical trio genome sequencing facilitates the interpretation of variants in cancer predisposition genes in paediatric tumour patients.

Author

Schroeder C, Faust U, Krauße L, Liebmann A, Abele M, Demidov G, Schütz L, Kelemen O, Pohle A, Gauß S, Sturm M, Roggia C, Streiter M, Buchert R, Armenau-Ebinger S, Nann D, Beschorner R, Handgretinger R, Ebinger M, Lang P, Holzer U, Skokowa J, Ossowski S, Haack TB, Mau-Holzmann UA, Dufke A, Riess O, and Brecht IB

Subjects

Humans, Child, Germ-Line Mutation, Genetic Testing methods, Genotype, Ribonuclease III genetics, DEAD-box RNA Helicases genetics, Genetic Predisposition to Disease, Neoplasms genetics

Abstract

The prevalence of pathogenic and likely pathogenic (P/LP) variants in genes associated with cancer predisposition syndromes (CPS) is estimated to be 8-18% for paediatric cancer patients. In more than half of the carriers, the family history is unsuspicious for CPS. Therefore, broad genetic testing could identify germline predisposition in additional children with cancer resulting in important implications for themselves and their families. We thus evaluated clinical trio genome sequencing (TGS) in a cohort of 72 paediatric patients with solid cancers other than retinoblastoma or CNS-tumours. The most prevalent cancer types were sarcoma (n = 26), neuroblastoma (n = 15), and nephroblastoma (n = 10). Overall, P/LP variants in CPS genes were identified in 18.1% of patients (13/72) and P/LP variants in autosomal-dominant CPS genes in 9.7% (7/72). Genetic evaluation would have been recommended for the majority of patients with P/LP variants according to the Jongmans criteria. Four patients (5.6%, 4/72) carried P/LP variants in autosomal-dominant genes known to be associated with their tumour type. With the immediate information on variant inheritance, TGS facilitated the identification of a de novo P/LP in NF1, a gonadosomatic mosaic in WT1 and two pathogenic variants in one patient (DICER1 and PALB2). TGS allows a more detailed characterization of structural variants with base-pair resolution of breakpoints which can be relevant for the interpretation of copy number variants. Altogether, TGS allows comprehensive identification of children with a CPS and supports the individualised clinical management of index patients and high-risk relatives., (© 2023. The Author(s).)

Published

2023

149. UV-radiation and MC1R germline mutations are risk factors for the development of conventional and spitzoid melanomas in children and adolescents.

Author

Liebmann A, Admard J, Armeanu-Ebinger S, Wild H, Abele M, Gschwind A, Seibel-Kelemen O, Seitz C, Bonzheim I, Riess O, Demidov G, Sturm M, Schadeck M, Pogoda M, Bien E, Krawczyk M, Jüttner E, Mentzel T, Cesen M, Pfaff E, Kunc M, Forchhammer S, Forschner A, Leiter-Stöppke U, Eigentler TK, Schneider DT, Schroeder C, Ossowski S, and Brecht IB

Abstract

Background: Genomic characterisation has led to an improved understanding of adult melanoma. However, the aetiology of melanoma in children is still unclear and identifying the correct diagnosis and therapeutic strategies remains challenging., Methods: Exome sequencing of matched tumour-normal pairs from 26 paediatric patients was performed to study the mutational spectrum of melanomas. The cohort was grouped into different categories: spitzoid melanoma (SM), conventional melanoma (CM), and other melanomas (OT)., Findings: In all patients with CM (n = 10) germline variants associated with melanoma were found in low to moderate melanoma risk genes: in 8 patients MC1R variants, in 2 patients variants in MITF, PTEN and BRCA2. Somatic BRAF mutations were detected in 60% of CMs, homozygous deletions of CDKN2A in 20%, TERTp mutations in 30%. In the SM group (n = 12), 5 patients carried at least one MC1R variant; somatic BRAF mutations were detected in 8.3%, fusions in 25% of the cases. No SM showed a homozygous CDKN2A deletion nor a TERTp mutation. In 81.8% of the CM/SM cases the UV damage signatures SBS7 and/or DBS1 were detected. The patient with melanoma arising in giant congenital nevus (CNM) demonstrated the characteristic NRAS Q61K mutation., Interpretation: UV-radiation and MC1R germline variants are risk factors in the development of conventional and spitzoid paediatric melanomas. Paediatric CMs share genomic similarities with adult CMs while the SMs differ genetically from the CM group. Consistent genetic characterization of all paediatric melanomas will potentially lead to better subtype differentiation, treatment, and prevention in the future., Funding: Found in Acknowledgement., Competing Interests: Declaration of interests Outside of submitted work: IBB: Institutional grant from Biontech. O.R. and C.Sc.: grants: Deutsche Forschungsgemeinschaft (DFG), Deutsche Krebshilfe (DKH), European Union (EU), grants to the institution from Illumina and BMS Stiftung Immunonkologie. U.L.S: grants: MSD; support for attending meeting and/or travel: Sun Pharma, Pierre Fabre; participation on a Data Safety Monitoring Board or Advisory Board: MSD, Novartis, Sun Pharma, Almirall, Roche, Sanofi; ADO board member. T.E.: Consulting fees: Bristol-Myers Squibb, MSD, Novartis, Almirall, Hermal, CureVac, Immunocore, Sanofi. S.O.: grants: DFG, Deutsche Luft und Raumfahrt Gesellschaft (DLR), European Union (EU), Bundesministerium für Bildung und Forschung (BMBF), Deutsche Krebshilfe, Bundesministerium für Arbeit und Soziales (BMSA); presentation: Illumina; support for attending meeting and/or travel: Oxford Nanopore Technologies. S.F.: grants: NeraCare, Skyline Dx, Biontech,; speakers honoraria: Kyowa Kirin, Recordati, Takeda Pharmaceuticals., (Copyright © 2023 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2023

150. Heterozygous UCHL1 loss-of-function variants cause a neurodegenerative disorder with spasticity, ataxia, neuropathy, and optic atrophy.

Author

Park J, Tucci A, Cipriani V, Demidov G, Rocca C, Senderek J, Butryn M, Velic A, Lam T, Galanaki E, Cali E, Vestito L, Maroofian R, Deininger N, Rautenberg M, Admard J, Hahn GA, Bartels C, van Os NJH, Horvath R, Chinnery PF, Tiet MY, Hewamadduma C, Hadjivassiliou M, Downes SM, Németh AH, Tofaris GK, Wood NW, Hayer SN, Bender F, Menden B, Cordts I, Klein K, Nguyen HP, Krauss JK, Blahak C, Strom TM, Sturm M, van de Warrenburg B, Lerche H, Maček B, Synofzik M, Ossowski S, Timmann D, Wolf ME, Smedley D, Riess O, Schöls L, Houlden H, Haack TB, and Hengel H

Published

2023