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1. Genetic Complexity and Parkinson's Disease

Author

Scott, William K., Stajich, Jeffrey M., Yamaoka, Larry H., Speer, Marcy C., Vance, Jeffery M., Roses, Allen D., Pericak-Vance, Margaret A., Gasser, T., Müller-Myhsok, B., Wszolek, Z. K., Dürr, A., Vaughan, J. R., Bonifati, V., Meco, G., Bereznai, B., Oehlmann, R., Agid, Y., Brice, A., Wood, N., and Polymeropoulos, Michael H.

Published
1997

6. Rare variants in β-Amyloid Precursor Protein (APP) and Parkinson's disease

Author

Schulte, E.C., Fukumori, A., Mollenhauer, B., Hor, H., Arzberger, T., Perneczky, R., Kurz, A., Diehl-Schmid, J., Hüll, M., Lichtner, P., Eckstein, G.N., Haubenberger, D., Pirker, W., Brücke, T., Bereznai, B., Molnar, M.J., Lorenzo-Betancor, O., Pastor, P., Peters, A., Gieger, C., Estivill, X., Meitinger, T., Kretzschmar, H.A., Trenkwalder, C., Haass, C., and Winkelmann, J.

Subjects
mental disorders
Abstract

Many individuals with Parkinson's disease (PD) develop cognitive deficits, and a phenotypic and molecular overlap between neurodegenerative diseases exists. We investigated the contribution of rare variants in seven genes of known relevance to dementias (β-amyloid precursor protein (APP), PSEN1/2, MAPT (microtubule-associated protein tau), fused in sarcoma (FUS), granulin (GRN) and TAR DNA-binding protein 43 (TDP-43)) to PD and PD plus dementia (PD+D) in a discovery sample of 376 individuals with PD and followed by the genotyping of 25 out of the 27 identified variants with a minor allele frequency A(p.(E599K))) was significantly associated with the PD phenotype but was not found in either the PD cases or controls of an independent replication sample. One of the identified rare variants (c.2125G>A (p.(G709S))) shifted the Aβ spectrum from Aβ40 to Aβ39 and Aβ37. Although the precise mechanism remains to be elucidated, our data suggest a possible role for APP in modifying the PD phenotype as well as a general contribution of genetic factors to the development of dementia in individuals with PD.

Published
2015

7. Rare variants in PLXNA4 and Parkinson's disease

Author

Schulte, E.C., Stahl, I., Czamara, D., Ellwanger, D.C., Eck, S., Graf, E., Mollenhauer, B., Lichtner, P., Haubenberger, D., Pirker, W., Brücke, T., Bereznai, B., Molnar, M.J., Peters, A., Gieger, C., Müller-Myhsok, B., Trenkwalder, C., and Winkelmann, J.

Abstract

Approximately 20% of individuals with Parkinson's disease (PD) report a positive family history. Yet, a large portion of causal and disease-modifying variants is still unknown. We used exome sequencing in two affected individuals from a family with late-onset familial PD followed by frequency assessment in 975 PD cases and 1014 ethnically-matched controls and linkage analysis to identify potentially causal variants. Based on the predicted penetrance and the frequencies, a variant in PLXNA4 proved to be the best candidate and PLXNA4 was screened for additional variants in 862 PD cases and 940 controls, revealing an excess of rare non-synonymous coding variants in PLXNA4 in individuals with PD. Although we cannot conclude that the variant in PLXNA4 is indeed the causative variant, these findings are interesting in the light of a surfacing role of axonal guidance mechanisms in neurodegenerative disorders but, at the same time, highlight the difficulties encountered in the study of rare variants identified by next-generation sequencing in diseases with autosomal dominant or complex patterns of inheritance.

Published
2013

10. Therapie der multiplen Sklerose

Author

Bereznai, B., primary, Goebels, N., additional, Dang, T., additional, Voltz, R., additional, Walther, E., additional, Zimmermann, C., additional, and Hohlfeld, R., additional

Published
2008
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16. Rare variants in Alzheimer's disease and frontotemporal dementia genes in Parkinson's disease

Author

Schulte, E. C., Fukumori, A., Mollenhauer, B., Hor, H., Perneczky, R., Kurz, A., Huell, M., Arzberger, T., Lichtner, P., Eckstein, G., Zimprich, A., Haubenberger, D., Pirker, W., Bruecke, T., Bereznai, B., Molnar, M. J., Lorenzo-Betancor, O., Pau Pastor, Peters, A., Gieger, C., Estivill, X., Kretzschmar, H. A., Meitinger, T., Trenkwalder, C., Haass, C., and Winkelmann, J.

19. The Ile93Met mutation in the ubiquitin carboxy-terminal-hydrolase-L1 gene is not observed in European cases with familial Parkinson’s disease

Author

Giuseppe De Michele, John Hardy, Ben A. Oostra, Alexandra Durr, B. Sanjay Harhangi, Benjamin Bereznai, Monique M.B. Breteler, Sarah Lincoln, J. R. Vaughan, Matthew J. Farrer, Thomas Gasser, Vincenzo Bonifati, Alexis Brice, Giuseppe Meco, Maria Martinez, Nicholas W. Wood, Harhangi, B, Farrer, Mj, Lincoln, S, Bonifati, V, Meco, G, DE MICHELE, Giuseppe, Brice, A, Drr, A, Martinez, M, Gasser, T, Bereznai, B, Vaughan, Jr, Wood, Nw, Oostra, Ba, Breteler, Mmb, THE ITALIAN PARKINSON GENETIC STUDY GROUP AND THE EUROPEAN CONSORTIUM ON GENETIC SUSCEPTIBILITY TO PARKINSONS, Diseas, Epidemiology, and Clinical Genetics

Subjects
Male, Candidate gene, Nerve Tissue Proteins, Biology, medicine.disease_cause, Polymerase Chain Reaction, White People, Nuclear Family, chemistry.chemical_compound, Germany, medicine, Humans, Point Mutation, Coding region, Gene, Aged, DNA Primers, Netherlands, Alpha-synuclein, Genetics, Mutation, General Neuroscience, Parkinson Disease, Exons, Middle Aged, Ubiquitin carboxy-terminal hydrolase L1, Major gene, Amino Acid Substitution, Italy, chemistry, Mutation testing, Female, France, Thiolester Hydrolases, Ubiquitin Thiolesterase
Abstract

Recently an Ile93Met mutation in the ubiquitin-carboxy-terminal-hydrolase-L1 gene (UCH-L1) has been described in a German family with Parkinson's disease (PD). The authors showed that this mutation is responsible for an impaired proteolytic activity of the UCH-L1 protein and may lead to an abnormal aggregation of proteins in the brain. In order to determine the importance of this or any other mutation in the coding region of the UCH-L1 gene in PD, we performed mutation analysis on Caucasian families with at least two affected sibs. We did not detect any mutations in the UCH-L1 gene, however, we cannot exclude mutations in the regulatory or intronic regions of the UCH-L1 gene since these regions were not sequenced. We conclude that the UCH-L1 gene is not a major gene responsible for familial PD.

Published
1999

20. Guillain-Barré syndrome during SARS-CoV-2 pandemic: A case report and review of recent literature.

Author

Scheidl E, Canseco DD, Hadji-Naumov A, and Bereznai B

Subjects
Ageusia etiology, COVID-19, Electromyography, Female, Guillain-Barre Syndrome diagnosis, Guillain-Barre Syndrome physiopathology, Guillain-Barre Syndrome therapy, Humans, Immunoglobulins, Intravenous therapeutic use, Middle Aged, Motor Neurons physiology, Neural Conduction, Olfaction Disorders etiology, SARS-CoV-2, Symptom Assessment, Betacoronavirus, Coronavirus Infections complications, Guillain-Barre Syndrome etiology, Pandemics, Pneumonia, Viral complications
Abstract

Acute demyelinating inflammatory polyneuropathy (AIDP) is the most common type of Guillain-Barré syndrome (GBS) in Europe, following several viral and bacterial infections. Data on AIDP-patients associated with SARS-CoV-2 (coronavirus-2) infection are scarce. We describe the case of a 54-years-old Caucasian female patient with typical clinical and electrophysiological manifestations of AIDP, who was reported positive with PCR for SARS-CoV-2, 3 weeks prior to onset of the neurological symptoms. She did not experience a preceding fever or respiratory symptoms, but a transient loss of smell and taste. At the admission to our neurological department, a progressive proximally pronounced paraparesis, areflexia, and sensory loss with tingling of all extremities were found, which began 10 days before. The modified Erasmus Giullain-Barré Syndrome outcome score (mEGOS) was 3/9 at admission and 1/12 at day 7 of hospitalization. The electrophysiological assessment proved a segmental demyelinating polyneuropathy and cerebrospinal fluid examination showed an albuminocytologic dissociation. The neurological symptoms improved significantly during treatment with immunoglobulins. Our case draws attention to the occurrence of GBS also in patients with COVID-19 (coronavirus disease 2019), who did not experience respiratory or general symptoms. It emphasizes that SARS-CoV-2 induces immunological processes, regardless from the lack of prodromic symptoms. However, it is likely that there is a connection between the severity of the respiratory syndrome and further neurological consequences., (© 2020 Peripheral Nerve Society.)

Published
2020
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21. The rs13388259 Intergenic Polymorphism in the Genomic Context of the BCYRN1 Gene Is Associated with Parkinson's Disease in the Hungarian Population.

Author

Márki S, Göblös A, Szlávicz E, Török N, Balicza P, Bereznai B, Takáts A, Engelhardt J, Klivényi P, Vécsei L, Molnár MJ, Nagy N, and Széll M

Abstract

Parkinson's disease (PD) is a common neurodegenerative disorder characterized by bradykinesia, resting tremor, and muscle rigidity. To date, approximately 50 genes have been implicated in PD pathogenesis, including both Mendelian genes with rare mutations and low-penetrance genes with common polymorphisms. Previous studies of low-penetrance genes focused on protein-coding genes, and less attention was given to long noncoding RNAs (lncRNAs). In this study, we aimed to investigate the susceptibility roles of lncRNA gene polymorphisms in the development of PD. Therefore, polymorphisms ( n =15) of the PINK1-AS , UCHL1-AS , BCYRN1 , SOX2-OT , ANRIL and HAR1A lncRNAs genes were genotyped in Hungarian PD patients ( n =160) and age- and sex-matched controls ( n =167). The rare allele of the rs13388259 intergenic polymorphism, located downstream of the BCYRN1 gene, was significantly more frequent among PD patients than control individuals (OR = 2.31; p =0.0015). In silico prediction suggested that this polymorphism is located in a noncoding region close to the binding site of the transcription factor HNF4A, which is a central regulatory hub gene that has been shown to be upregulated in the peripheral blood of PD patients. The rs13388259 polymorphism may interfere with the binding affinity of transcription factor HNF4A, potentially resulting in abnormal expression of target genes, such as BCYRN1 .

Published
2018
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22. Three novel mutations and genetic epidemiology analysis of the Gap Junction Beta 1 (GJB1) gene among Hungarian Charcot-Marie-Tooth disease patients.

Author

Milley GM, Varga ET, Grosz Z, Bereznai B, Aranyi Z, Boczan J, Dioszeghy P, Kálmán B, Gal A, and Molnar MJ

Subjects
Adult, Age of Onset, Cohort Studies, Female, Humans, Hungary epidemiology, Male, Middle Aged, Phenotype, Severity of Illness Index, Sex Factors, Gap Junction beta-1 Protein, Charcot-Marie-Tooth Disease epidemiology, Charcot-Marie-Tooth Disease genetics, Connexins genetics, Mutation, Missense
Abstract

Pathogenic variants of the gap junction beta 1 (GJB1) gene are responsible for the Charcot-Marie-Tooth neuropathy X type 1 (CMTX1). In this study, we report the mutation frequency of GJB1 in 210 Hungarian CMT patients and the phenotype comparison between male and female CMTX1 patients. Altogether, 13 missense substitutions were found in the GJB1 gene. Among them, 10 have been previously described as pathogenic variants (p.Arg15Trp, p.Val63Ile, p.Leu89Val, p.Ala96Gly, p.Arg107Trp, p.Arg142Gln, p.Arg164Trp, p.Arg164Gln, p.Pro172Ala and p.Asn205Ser), while 3 were novel, likely pathogenic alterations (p.Val13Glu, p.Glu186Gly, p.Met194Ile). These variants were not present in controls and were predicted as disease causing by in silico analysis. The frequency of the variants was 6.7% in our cohort which refers to a common cause of hereditary neuropathy among Hungarian patients. In addition to the classical phenotype, CNS involvement was proved in 26.1% of the CMTX1 patients. GJB1 pathogenic alterations were found mainly in males but we also detected them in female probands. The statistical analysis of CMTX1 patients revealed a significant difference between the two genders regarding the age of onset, Charcot-Marie-Tooth neuropathy and examination scores., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published
2016
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23. Rare variants in β-Amyloid precursor protein (APP) and Parkinson's disease.

Author

Schulte EC, Fukumori A, Mollenhauer B, Hor H, Arzberger T, Perneczky R, Kurz A, Diehl-Schmid J, Hüll M, Lichtner P, Eckstein G, Zimprich A, Haubenberger D, Pirker W, Brücke T, Bereznai B, Molnar MJ, Lorenzo-Betancor O, Pastor P, Peters A, Gieger C, Estivill X, Meitinger T, Kretzschmar HA, Trenkwalder C, Haass C, and Winkelmann J

Subjects
Aged, Alzheimer Disease genetics, Cell Line, DNA-Binding Proteins genetics, Dementia genetics, Female, Gene Frequency genetics, Genotype, HEK293 Cells, Humans, Male, Neurodegenerative Diseases genetics, Amyloid beta-Protein Precursor genetics, Genetic Variation genetics, Parkinson Disease genetics
Abstract

Many individuals with Parkinson's disease (PD) develop cognitive deficits, and a phenotypic and molecular overlap between neurodegenerative diseases exists. We investigated the contribution of rare variants in seven genes of known relevance to dementias (β-amyloid precursor protein (APP), PSEN1/2, MAPT (microtubule-associated protein tau), fused in sarcoma (FUS), granulin (GRN) and TAR DNA-binding protein 43 (TDP-43)) to PD and PD plus dementia (PD+D) in a discovery sample of 376 individuals with PD and followed by the genotyping of 25 out of the 27 identified variants with a minor allele frequency <5% in 975 individuals with PD, 93 cases with Lewy body disease on neuropathological examination, 613 individuals with Alzheimer's disease (AD), 182 cases with frontotemporal dementia and 1014 general population controls. Variants identified in APP were functionally followed up by Aβ mass spectrometry in transiently transfected HEK293 cells. PD+D cases harbored more rare variants across all the seven genes than PD individuals without dementia, and rare variants in APP were more common in PD cases overall than in either the AD cases or controls. When additional controls from publically available databases were added, one rare variant in APP (c.1795G>A(p.(E599K))) was significantly associated with the PD phenotype but was not found in either the PD cases or controls of an independent replication sample. One of the identified rare variants (c.2125G>A (p.(G709S))) shifted the Aβ spectrum from Aβ40 to Aβ39 and Aβ37. Although the precise mechanism remains to be elucidated, our data suggest a possible role for APP in modifying the PD phenotype as well as a general contribution of genetic factors to the development of dementia in individuals with PD.

Published
2015
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24. The coexistence of dynamin 2 mutation and multiple mitochondrial DNA (mtDNA) deletions in the background of severe cardiomyopathy and centronuclear myopathy.

Author

Gal A, Inczedy-Farkas G, Pal E, Remenyi V, Bereznai B, Geller L, Szelid Z, Merkely B, and Molnar MJ

Subjects
Blotting, Southern, Cardiomyopathies physiopathology, Dynamin II, Electrophysiology, Female, Humans, Middle Aged, Myopathies, Structural, Congenital physiopathology, Polymerase Chain Reaction, Sequence Deletion, Cardiomyopathies genetics, DNA, Mitochondrial genetics, Dynamins genetics, Mutation, Myopathies, Structural, Congenital genetics
Abstract

Dynamin2 (DNM2) gene mutations may result in Charcot-Marie-Tooth disease and centronuclear myopathy. Here, we present a patient suffering from cardiomyopathy and centronuclear myopathy with repetitive discharges and mild axonal neuropathy due to DNM2 mutation. Detailed cardiological and neurological examinations, electrophysiological tests, muscle biopsy, and molecular genetic analysis were performed. The patient developed left bundle branch block at age 40 and was fitted with a pacemaker at the age of 43. The patient has severe heart failure, ptosis, strabism, facial and proximal muscle weakness. Electrophysiological investigations found myopathy, complex repetitive discharges, and axonal neuropathy. Skeletal muscle biopsy detected centronuclear myopathy and cytochrome C oxidase (COX) negative fibers. Genetic analysis detected a pathogenic c.1105C>T (p.R369W) DNM2 gene mutation and heteroplasmic multiple mitochondrial DNA (mtDNA) deletion. Our data broadens the phenotypic spectrum of DNM2 mutations. The presence of the multiple mtDNA deletions may provide new aspects to understanding the pathogenesis of multisystemic symptoms in patients with DNM2 mutations.

Published
2015
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25. The modifying effect a PMP22 deletion in a family with Charcot-Marie-Tooth type 1 neuropathy due to an EGR2 mutation.

Author

Reményi V, Inczédy-Farkas G, Gál A, Bereznai B, Pál Z, Karcagi V, Mechler F, and Molnár MJ

Subjects
Adult, Age of Onset, Arginine, Charcot-Marie-Tooth Disease pathology, Histidine, Humans, Male, Median Nerve physiopathology, Middle Aged, Peroneal Nerve physiopathology, Sural Nerve pathology, Sural Nerve physiopathology, Ulnar Nerve physiopathology, Amino Acid Substitution, Charcot-Marie-Tooth Disease genetics, Charcot-Marie-Tooth Disease physiopathology, Early Growth Response Protein 2 genetics, Gene Deletion, Myelin Proteins genetics, Neural Conduction
Abstract

Background: Mutations of both the PMP22 and EGR2 genes cause Charcot-Marie-Tooth (CMT) disease type 1. Deletion of the PMP22 gene, results in hereditary neuropathy with liability to pressure palsies. More publications exist about the interaction of PMP22 duplication and other CMT-causing gene mutations. In these cases the intrafamiliar discordant phenotypes draw the attention to the possible role of modifying genes. The gene-gene interactions between the PMP22 and EGR2 genes are not well understood., Case Report: We report two brothers with late onset CMT1 due to a c. 1142 G>A (Arg381His) heterozygous substitution in the EGR2 gene. Additionally, the older brother with the less severe symptoms harbored the PMP22 gene deletion also., Conclusion: The coexistence of the two genetic alterations did not aggravate the clinical symptoms. Moreover, the PMP22 deletion appeared to have a beneficial modifying effect, thus implying potential gene-gene interaction of PMP22 and EGR2. PMP22 deletion may increase Schwann cells proliferation and compensate the dominant-negative effect of the Arg381 His substitution in the EGR2 gene.

Published
2014

26. Mitochondrial DNA mutations and cognition: a case-series report.

Author

Inczedy-Farkas G, Trampush JW, Perczel Forintos D, Beech D, Andrejkovics M, Varga Z, Remenyi V, Bereznai B, Gal A, and Molnar MJ

Subjects
Adolescent, Adult, Cognition Disorders diagnosis, Cohort Studies, Female, Genotype, Humans, Male, Mental Recall physiology, Middle Aged, Neuropsychological Tests, Verbal Learning, Young Adult, Cognition Disorders genetics, DNA, Mitochondrial genetics, Mutation genetics
Abstract

Mutations in the mitochondrial genome can impair normal metabolic function in the central nervous system (CNS) where cellular energy demand is high. Primary mitochondrial DNA (mtDNA) mutations have been linked to several mitochondrial disorders that have comorbid psychiatric, neurologic, and cognitive sequelae. Here, we present a series of cases with primary mtDNA mutations who were genotyped and evaluated across a common neuropsychological battery. Nineteen patients with mtDNA mutations were genotyped and clinically and cognitively evaluated. Pronounced deficits in nonverbal/visuoperceptual reasoning, verbal recall, semantic word generativity, and processing speed were evident and consistent with a "mitochondrial dementia" that has been posited. However, variation in cognitive performance was noteworthy, suggesting that the phenotypic landscape of cognition linked to primary mtDNA mutations is heterogeneous. Our patients with mtDNA mutations evidenced cognitive deficits quite similar to those commonly seen in Alzheimer's disease and could have clinical relevance to the evaluation of dementia., (© The Author 2014. Published by Oxford University Press. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published
2014
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27. Different patterns of nerve enlargement in polyneuropathy subtypes as detected by ultrasonography.

Author

Scheidl E, Böhm J, Simó M, Bereznai B, Bereczki D, and Arányi Z

Subjects
Aged, Case-Control Studies, Female, Humans, Male, Middle Aged, Polyneuropathies pathology, Prospective Studies, Spinal Nerve Roots pathology, Transducers, Ultrasonography, Arm innervation, Leg innervation, Polyneuropathies diagnostic imaging, Spinal Nerve Roots diagnostic imaging
Abstract

The purpose of our study was to examine how the pathologic type of polyneuropathy affects nerve size as assessed by high-resolution ultrasonography with a 15 MHz transducer. Cross-sectional area (CSA) of the C5-C7 nerve roots and several upper and lower limb nerves at multiple sites was measured in 38 patients with acquired diffuse sensorimotor demyelinating or axonal polyneuropathy and in 34 healthy control subjects. Significant differences were found among the groups for all nerve and root segments: Both types of polyneuropathy are characterized by nerve enlargement in comparison to controls, but in different patterns. In demyelinating polyneuropathies, an additional degree of nerve thickening appears in proximal upper limb nerves and cervical nerve roots compared with axonal polyneuropathies. With respect to the other nerves, a similar degree of nerve enlargement was observed in both patient groups. These results highlight that ultrasonography may be a complementary tool in differentiating polyneuropathies., (Copyright © 2014 World Federation for Ultrasound in Medicine & Biology. Published by Elsevier Inc. All rights reserved.)

Published
2014
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28. Rare variants in PLXNA4 and Parkinson's disease.

Author

Schulte EC, Stahl I, Czamara D, Ellwanger DC, Eck S, Graf E, Mollenhauer B, Zimprich A, Lichtner P, Haubenberger D, Pirker W, Brücke T, Bereznai B, Molnar MJ, Peters A, Gieger C, Müller-Myhsok B, Trenkwalder C, and Winkelmann J

Subjects
Case-Control Studies, Family, Female, Genetic Linkage, Humans, Male, Genetic Variation, Parkinson Disease genetics, Penetrance, Receptors, Cell Surface genetics
Abstract

Approximately 20% of individuals with Parkinson's disease (PD) report a positive family history. Yet, a large portion of causal and disease-modifying variants is still unknown. We used exome sequencing in two affected individuals from a family with late-onset familial PD followed by frequency assessment in 975 PD cases and 1014 ethnically-matched controls and linkage analysis to identify potentially causal variants. Based on the predicted penetrance and the frequencies, a variant in PLXNA4 proved to be the best candidate and PLXNA4 was screened for additional variants in 862 PD cases and 940 controls, revealing an excess of rare non-synonymous coding variants in PLXNA4 in individuals with PD. Although we cannot conclude that the variant in PLXNA4 is indeed the causative variant, these findings are interesting in the light of a surfacing role of axonal guidance mechanisms in neurodegenerative disorders but, at the same time, highlight the difficulties encountered in the study of rare variants identified by next-generation sequencing in diseases with autosomal dominant or complex patterns of inheritance.

Published
2013
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29. The role of SCARB2 as susceptibility factor in Parkinson's disease.

Author

Hopfner F, Schulte EC, Mollenhauer B, Bereznai B, Knauf F, Lichtner P, Zimprich A, Haubenberger D, Pirker W, Brücke T, Peters A, Gieger C, Kuhlenbäumer G, Trenkwalder C, and Winkelmann J

Subjects
Aged, Aged, 80 and over, Female, Genetic Variation genetics, Genotype, Glucosylceramidase genetics, Humans, Male, Middle Aged, Mutation genetics, Risk Factors, Genetic Predisposition to Disease, Lysosomal Membrane Proteins genetics, Parkinson Disease genetics, Polymorphism, Single Nucleotide genetics, Receptors, Scavenger genetics
Abstract

Background: Genetic variation in the glucocerebrosidase (GBA) gene is strongly associated with Parkinson's disease (PD). Transport of glucocerebrosidase to the lysosome involves the protein encoded by the SCARB2 gene. An association between the common SNP rs6812193, upstream of SCARB2, and PD has been reported previously. The role of exonic variants in the SCARB2 gene in PD has not been examined., Methods: We studied the role of exonic variants in SCARB2 and tried to replicate the association between the SNP rs6812193 and PD in a German and Austrian sample. Screening of all SCARB2 exons by high-resolution melting curve analysis was performed in 376 German PD patients. The SNP rs6812193 was analyzed in 984 PD patients and 1014 general population controls., Results: We identified no novel exonic variants in SCARB2 but confirmed the association between SNP rs6812193 and PD (OR, 0.86; P=.02)., (Copyright © 2013 Movement Disorder Society.)

Published
2013
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30. Variants in eukaryotic translation initiation factor 4G1 in sporadic Parkinson's disease.

Author

Schulte EC, Mollenhauer B, Zimprich A, Bereznai B, Lichtner P, Haubenberger D, Pirker W, Brücke T, Molnar MJ, Peters A, Gieger C, Trenkwalder C, and Winkelmann J

Subjects
Aged, Cohort Studies, Exons, Female, Genetic Linkage, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Haplotypes, Humans, Male, Middle Aged, Models, Genetic, Molecular Sequence Data, Eukaryotic Initiation Factor-4G genetics, Parkinson Disease genetics
Abstract

Recently, mutations in eukaryotic translation initiation factor 4G1 (EIF4G1) were reported as a rare cause of familial Parkinson's disease (PD). We screened the 33 exons of EIF4G1 by high-resolution melting curve analysis for variants in our Central European cohort of 376 PD cases. Variant frequency was assessed in a total of 975 PD cases and 1,014 general population controls. Eight novel nonsynonymous and four synonymous variants were identified. In our cohort, novel and previously identified nonsynonymous variants were very rare. Although it is possible that our general population controls also comprise individuals who have or could develop PD in the future, the presence of the original mutation (EIF4G1 p.Arg1205 His) in three controls only, raises questions about the causality of this variant with regard to PD.

Published
2012
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31. [The absence of the common LRRK2 G2019S mutation in 120 young onset Hungarian Parkinon's disease patients].

Author

Balicza P, Bereznai B, Takáts A, Klivényi P, Dibó G, Hidasi E, Balogh I, and Molnár MJ

Subjects
Adult, Age of Onset, Aged, Female, Gene Frequency, Genetic Predisposition to Disease, Genetic Testing, Glycine, Humans, Hungary epidemiology, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Male, Middle Aged, Serine, Parkinson Disease epidemiology, Parkinson Disease genetics, Point Mutation, Protein Serine-Threonine Kinases genetics
Abstract

Parkinson's disease is a promising target of applying personalized medicine. For this purpose it is crucial to reveal the genetic and environmental factors, which contribute to the disease, also to collect epidemiologic data and to preserve the patients samples and data in a proper biobank. In our investigation we examined the prevalence of the most frequent Parkinson's disease causing LRRK2 G2019S mutation in a Hungarian Parkinson-patient group. From 120 patients, we haven't detected this substitution in anyone. Our investigation suggest that the mutation LRRK2 G2019S may be a rare cause of Parkinson disease in the Hungarian population.

Published
2012

32. Ultrasonography of MADSAM neuropathy: focal nerve enlargements at sites of existing and resolved conduction blocks.

Author

Scheidl E, Böhm J, Simó M, Rózsa C, Bereznai B, Kovács T, and Arányi Z

Subjects
Adult, Demyelinating Diseases complications, Electric Stimulation, Facial Nerve physiopathology, Female, Humans, Male, Middle Aged, Polyneuropathies complications, Demyelinating Diseases pathology, Facial Nerve diagnostic imaging, Neural Conduction physiology, Polyneuropathies pathology, Ultrasonography
Abstract

Using the emerging technique of peripheral nerve ultrasonography, multiple focal nerve swellings corresponding to sites of existing conduction blocks have been described in demyelinating polyneuropathies. We report two cases of multifocal acquired demyelinating sensory and motor neuropathy (MADSAM). In the first, multiple focal nerve enlargements were detected by ultrasound at sites of previous conduction blocks, well after complete clinical and electrophysiological resolution. In the second case, existing proximal conduction blocks could be localized by ultrasound. Our cases highlight the importance of nerve ultrasound in identifying conduction blocks and demonstrate that ultrasonographic morphological changes may outlast functional recovery in demyelinating neuropathies., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published
2012
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33. Psychiatric symptoms of patients with primary mitochondrial DNA disorders.

Author

Inczedy-Farkas G, Remenyi V, Gal A, Varga Z, Balla P, Udvardy-Meszaros A, Bereznai B, and Molnar MJ

Subjects
Adolescent, Adult, Cohort Studies, Data Interpretation, Statistical, Female, Genotype, Hereditary Sensory and Motor Neuropathy genetics, Hereditary Sensory and Motor Neuropathy psychology, Humans, Male, Mental Disorders genetics, Mental Disorders psychology, Middle Aged, Mitochondrial Diseases genetics, Mitochondrial Diseases psychology, Mood Disorders genetics, Mood Disorders psychology, Mutation physiology, Neuropsychological Tests, Personality Disorders genetics, Personality Disorders psychology, Polymerase Chain Reaction, Psychiatric Status Rating Scales, Serotonin Plasma Membrane Transport Proteins genetics, Severity of Illness Index, Young Adult, DNA, Mitochondrial genetics, Mental Disorders etiology, Mitochondrial Diseases complications
Abstract

Background: The aim of our study was to assess psychiatric symptoms in patients with genetically proven primary mutation of the mitochondrial DNA., Methods: 19 adults with known mitochondrial mutation (MT) have been assessed with the Stanford Health Assessment Questionnaire 20-item Disability Index (HAQ-DI), the Symptom Check List-90-Revised (SCL-90-R), the Beck Depression Inventory-Short Form (BDI-SF), the Hamilton Depression Rating Scale (HDRS) and the clinical version of the Structured Clinical Interview for the the DSM-IV (SCID-I and SCID-II) As control, 10 patients with hereditary sensorimotor neuropathy (HN), harboring the peripheral myelin protein-22 (PMP22) mutation were examined with the same tools., Results: The two groups did not differ significantly in gender, age or education. Mean HAQ-DI score was 0.82 in the MT (range: 0-1.625) and 0.71 in the HN group (range: 0-1.625). Level of disability between the two groups did not differ significantly (p = 0.6076). MT patients scored significantly higher on the BDI-SF and HDRS than HN patients (12.85 versus 4.40, p = 0.031, and 15.62 vs 7.30, p = 0.043, respectively). The Global Severity Index (GSI) of SCL-90-R also showed significant difference (1.44 vs 0.46, p = 0.013) as well as the subscales except for somatization. SCID-I interview yielded a variety of mood disorders in both groups. Eight MT patient (42%) had past, 6 (31%) had current, 5 (26%) had both past and current psychiatric diagnosis, yielding a lifetime prevalence of 9/19 (47%) in the MT group. In the HN group, 3 patients had both past and current diagnosis showing a lifetime prevalence of 3/10 (30%) in this group. SCID-II detected personality disorder in 8 MT cases (42%), yielding 3 avoidant, 2 obsessive-compulsive and 3 personality disorder not otherwise specified (NOS) diagnosis. No personality disorder was identified in the HN group., Conclusions: Clinicians should be aware of the high prevalence of psychiatric symptoms in patients with mitochondrial mutation which has both etiologic and therapeutic relevance.

Published
2012
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34. [Therapy for anti-MuSK antibody positive myasthenia gravis].

Author

Pál Z, Boczán J, Bereznai B, Lovas G, and Molnár MJ

Subjects
Adult, Azathioprine administration & dosage, Female, Humans, Methotrexate administration & dosage, Myasthenia Gravis drug therapy, Treatment Failure, Treatment Outcome, Autoantibodies blood, Immunosuppressive Agents therapeutic use, Myasthenia Gravis immunology, Myasthenia Gravis therapy, Plasma Exchange, Receptor Protein-Tyrosine Kinases immunology, Receptors, Cholinergic immunology
Abstract

The authors report the case of a 27-year-old woman with muscle-specific receptor tyrosine kinase antibody positive myasthenia with predominantly ocular and bulbar symptoms. Both edrophonium and low dose (4×30 mg/day) pyridostigmin resulted in cholinergic side effects including fasciculation mainly in the facial and neck muscles, and excessive salivation. The patient responded well to a relatively high dose of chronic corticosteroid treatment (methyprednisolone 64mg/day), but the decrease of the corticosteroid dose below 16 mg/day induced exacerbation of the clinical symptoms. Immunosuppression with azathioprine and methotrexate failed to maintain the clinical improvement. However, plasma exchange was always very effective, and all clinical symptoms improved significantly. The authors conclude that patients with muscle-specific receptor tyrosine kinase antibody positive myasthenia gravis should have an individual treatment protocol differing from those used in patients who do not have this antibody but are positive for acetylcholine-receptor antibody. Identification of the pathogenic antibody in the early stage of myasthenia gravis may help to develop the optimal, individualized treatment strategy, to avoid severe side effects, and to achieve fast improvement.

Published
2011
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35. [Clinical manifestations, course and outcome of enzyme replacement therapy in Hungarian patients with Pompe's disease].

Author

Bereznai B, Trauninger A, György I, Szakszon K, Almássy Z, Pál E, Herczegfalvi A, Várdi Visy K, Illés Z, and Molnár MJ

Subjects
Adult, Age of Onset, Carbon Dioxide metabolism, Child, Child, Preschool, Disease Progression, Female, Forced Expiratory Volume, Glycogen Storage Disease Type II drug therapy, Glycogen Storage Disease Type II physiopathology, Humans, Hungary, Male, Middle Aged, Oxygen metabolism, Phenotype, Respiratory Insufficiency enzymology, Respiratory Insufficiency physiopathology, Time Factors, alpha-Glucosidases genetics, Enzyme Replacement Therapy methods, Glycogen Storage Disease Type II enzymology, Glycogen Storage Disease Type II genetics, Respiratory Insufficiency etiology, alpha-Glucosidases deficiency, alpha-Glucosidases therapeutic use
Abstract

Unlabelled: Pompe's disease is an autosomal recessive disease caused by deficiency of acid-alpha-glucosidase., Aims and Methods: Authors analyzed the phenotype of 11 Hungarian patients with Pompe's disease and evaluated clinical parameters and response to enzyme replacement therapy during a long-term follow-up in 8 patients., Results: One patient with atypical infantile form presented with cardiomyopathy and a very slow progression of motor deficits; after 2 years of enzyme replacement therapy no disability was present at the age 6 years. Another patient was asymptomatic at the age of 2.5 years. The adult onset form was characterized by slight to prominent limb-girdle myopathy with an age of onset between 20 and 50 years. In 3 of such cases respiratory insufficiency was also present., Conclusions: Hungarian patients with Pompe's disease presented with a wide phenotypic variability ranging from atypical early childhood form with slowly progressive course to late-onset limb-girdle myopathy with variable courses. Enzyme replacement therapy resulted in significant improvement in motor and respiratory functions in most of the patients.

Published
2011
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36. Coexisting huntingtin and SCA8 repeat expansion: case report of a severe complex neurodegenerative syndrome.

Author

Bereznai B, Lovas G, Pentelenyi K, Rudas G, and Molnar MJ

Subjects
Adult, Brain pathology, DNA Mutational Analysis methods, Female, Humans, Huntingtin Protein, Magnetic Resonance Imaging methods, RNA, Long Noncoding, RNA, Untranslated, Nerve Tissue Proteins genetics, Neurodegenerative Diseases genetics, Nuclear Proteins genetics, Trinucleotide Repeat Expansion genetics
Abstract

We report the case of a 29 year old woman with a complex movement disorder syndrome due to the combination of coexisting pathological triplet repeat expansions of huntingtin and ATXN8 genes. The disease course was characterized by mental disturbances including cognitive decline and changes in personality starting at the age of 12 years, followed by twisting motions, intentional tremor and gait ataxia. Later Parkinsonian symptoms of micrographia, bradykinesia, muscle rigidity and mental decline became dominant. Brain MRI showed hypoplasia of the nucleus caudatus and generalized atrophy; MR spectroscopy revealed a decrease of all typical metabolites except for an increased level of lactate and acetate. Therapeutic trials with pramipexole, ropinirole and tetrabenazine showed no benefit, while levetiracetam caused agitation and hallucinations. We discuss phenotype-genotype correlation and the rule of triplet repeat expansions of gene ATXN8., (Copyright 2010 Elsevier B.V. All rights reserved.)

Published
2010
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37. [Genetics and present therapy options in Parkinson's disease: a review].

Author

Bereznai B and Molnar MJ

Subjects
Combined Modality Therapy methods, Dance Therapy, Genetic Predisposition to Disease, Genetic Testing, Genetic Therapy, Humans, Intracellular Signaling Peptides and Proteins genetics, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Music Therapy, Oncogene Proteins genetics, Parkinson Disease diagnosis, Parkinson Disease drug therapy, Physical Therapy Modalities, Protein Deglycase DJ-1, Protein Kinases genetics, Protein Serine-Threonine Kinases genetics, Psychotherapy, Relaxation Therapy, Ubiquitin-Protein Ligases genetics, alpha-Synuclein genetics, Antiparkinson Agents therapeutic use, Deep Brain Stimulation, Parkinson Disease genetics, Parkinson Disease therapy
Abstract

In the past years, six monogenic forms of Parkinson disease have clearly been associated with this movement disorder. The most frequent forms are LRRK2- and Parkin-associated Parkinson disease. Currently, a genetic diagnosis does not change the therapy, the genes involved in genetic Parkinson disease help to understand the underlying pathophysiologic mechanisms of Parkinson disease. Beside the overview of the molecular-genetic basis, we give a review about genetic testing, pharmacological and other multidisciplinary treatment options.

Published
2009

38. [DYT1 positive generalised dystonia: a case study of two siblings].

Author

Bereznai B, Baraczka K, Nagy Z, and Molnár MJ

Subjects
Adolescent, Adult, Child, Dystonia classification, Gene Deletion, Handwriting, Humans, Male, Mutation, Polymerase Chain Reaction, Walking, Dystonia metabolism, Dystonic Disorders genetics, Dystonic Disorders metabolism, Molecular Chaperones genetics, Molecular Chaperones metabolism, Siblings
Abstract

The early-onset generalised dystonia is a dyskinetic movement disorder with a wide variety in phenotype and poor response to pharmacological treatment. A mutation on the DYT1 gene is responsible for the disease in more than 50% of cases with typical early-onset dystonia beginning in a limb. We describe the medical history of two brothers with first signs of focal dystonia at age 12 starting with right side lower limb dystonia of the older brother and writers cramp of the younger one. In both over a period of 6 and 10 years dystonia generalised. The negative results of MRI, electrophysiological testing and muscle biopsy corroborate the diagnosis of primary dystonia. The DNA from the older patient was tested for the 3 bp deletion in exon 5 of the DYT1 gene by restriction enzyme. The positive result confirmed the diagnosis of early-onset primary dystonia. A short synopsis of routine molecular genetic tests indications and treatment options is outlined.

Published
2007

39. Point mutations in exon 1 of the NR4A2 gene are not a major cause of familial Parkinson's disease.

Author

Zimprich A, Asmus F, Leitner P, Castro M, Bereznai B, Homann N, Ott E, Rutgers AW, Wieditz G, Trenkwalder C, and Gasser T

Subjects
DNA-Binding Proteins metabolism, Dopamine metabolism, Exons, Family Health, Humans, Nuclear Receptor Subfamily 4, Group A, Member 2, Transcription Factors metabolism, DNA-Binding Proteins genetics, Parkinson Disease genetics, Point Mutation, Transcription Factors genetics
Published
2003
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40. Chronic high-frequency globus pallidus internus stimulation in different types of dystonia: a clinical, video, and MRI report of six patients presenting with segmental, cervical, and generalized dystonia.

Author

Bereznai B, Steude U, Seelos K, and Bötzel K

Subjects
Adult, Aged, Chronic Disease, Female, Humans, Male, Middle Aged, Severity of Illness Index, Videotape Recording, Brain pathology, Dystonia diagnosis, Dystonia therapy, Electric Stimulation Therapy methods, Globus Pallidus pathology, Magnetic Resonance Imaging
Abstract

The results of deep brain stimulation (DBS) of the globus pallidus internus (Gpi) in six patients with generalized, focal, and segmental dystonia are presented. Pre- and postoperative assessments are given for one patient with generalized inherited dystonia and for five patients with idiopathic segmental or cervical dystonia. Clinical symptoms were evaluated before and 3-12 months after surgery using the Burke-Fahn-Marsden (BFM) dystonia rating scale for primary torsion dystonia and the Tsui scale for cervical dystonia. The Short-Form Health Survey (SF-36) was completed by each patient to document preoperative and postoperative health status. Also, neurological status was documented by video before and during chronic stimulation. Magnetic resonance imaging studies were performed to show the anatomical localization of the electrode leads. Five patients showed a progressive improvement within 7 days. One patient with cervical dystonia and Meige's syndrome showed no improvement for 3 months, but beneficial effects were observed after 12 months. On average, the BFM movement scale scores decreased by 72.5% and Tsui scale scores by 63%. SF-36 showed an improvement in health status by an average of 36% according to eight different health categories. We conclude that chronic high-frequency Gpi stimulation in different types of dystonia is a very effective and safe treatment., (Copyright 2002 Movement Disorder Society.)

Published
2002
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41. The Ile93Met mutation in the ubiquitin carboxy-terminal-hydrolase-L1 gene is not observed in European cases with familial Parkinson's disease.

Author

Harhangi BS, Farrer MJ, Lincoln S, Bonifati V, Meco G, De Michele G, Brice A, Dürr A, Martinez M, Gasser T, Bereznai B, Vaughan JR, Wood NW, Hardy J, Oostra BA, and Breteler MM

Subjects
Aged, DNA Primers, Exons, Female, France, Germany, Humans, Italy, Male, Middle Aged, Nerve Tissue Proteins genetics, Netherlands, Nuclear Family, Parkinson Disease enzymology, Polymerase Chain Reaction, Thiolester Hydrolases chemistry, Ubiquitin Thiolesterase, Amino Acid Substitution, Parkinson Disease genetics, Point Mutation, Thiolester Hydrolases genetics, White People genetics
Abstract

Recently an Ile93Met mutation in the ubiquitin-carboxy-terminal-hydrolase-L1 gene (UCH-L1) has been described in a German family with Parkinson's disease (PD). The authors showed that this mutation is responsible for an impaired proteolytic activity of the UCH-L1 protein and may lead to an abnormal aggregation of proteins in the brain. In order to determine the importance of this or any other mutation in the coding region of the UCH-L1 gene in PD, we performed mutation analysis on Caucasian families with at least two affected sibs. We did not detect any mutations in the UCH-L1 gene, however, we cannot exclude mutations in the regulatory or intronic regions of the UCH-L1 gene since these regions were not sequenced. We conclude that the UCH-L1 gene is not a major gene responsible for familial PD.

Published
1999
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42. [Therapy of multiple sclerosis].

Author

Bereznai B, Goebels N, Dang T, Voltz R, Walther E, Zimmermann C, and Hohlfeld R

Subjects
Adrenal Cortex Hormones therapeutic use, Humans, Immunosuppressive Agents therapeutic use, Immunotherapy, Multiple Sclerosis therapy
Published
1999
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43. The alpha-synuclein Ala53Thr mutation is not a common cause of familial Parkinson's disease: a study of 230 European cases. European Consortium on Genetic Susceptibility in Parkinson's Disease.

Author

Vaughan J, Durr A, Tassin J, Bereznai B, Gasser T, Bonifati V, De Michele G, Fabrizio E, Volpe G, Bandmann O, Johnson WG, Golbe LI, Breteler M, Meco G, Agid Y, Brice A, Marsden CD, and Wood NW

Subjects
Adult, Aged, Aged, 80 and over, DNA analysis, Europe, Female, Genetic Testing, Humans, Male, Middle Aged, Mutation, Polymerase Chain Reaction, Synucleins, alpha-Synuclein, Nerve Tissue Proteins genetics, Parkinson Disease genetics, Phosphoproteins genetics, White People genetics
Abstract

We report the results of a screen of 230 European familial index cases of Parkinson's disease for the recently described Ala53Thr mutation in the alpha-synuclein gene in an autosomal dominant Parkinson's disease kindred. No mutations were found from this broad white population, and we therefore conclude that although of great interest, this mutation is a very rare cause of familial Parkinson's disease.

Published
1998
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44. A susceptibility locus for Parkinson's disease maps to chromosome 2p13.

Author

Gasser T, Müller-Myhsok B, Wszolek ZK, Oehlmann R, Calne DB, Bonifati V, Bereznai B, Fabrizio E, Vieregge P, and Horstmann RD

Subjects
Adult, Age of Onset, Aged, Aged, 80 and over, Disease Susceptibility, Female, Genes, Dominant, Genetic Markers, Haplotypes, Humans, Lod Score, Male, Middle Aged, Pedigree, Chromosomes, Human, Pair 2, Genetic Linkage, Parkinson Disease genetics
Abstract

Parkinson's disease (PD) is a common degenerative neurologic disorder, which is pathologically characterized by a selective degeneration of dopaminergic neurons of the substantia nigra pars compacta, and the presence of characteristic eosinophilic inclusions, known as Lewy-bodies in affected brain areas. The cause of PD is unknown but, in recent years, genetic factors have been implicated in the aetiology of the disease. Firstly, clinico-genetic, epidemiologic and twin studies revealed inheritable effects and questioned earlier studies which had denied such influences. Secondly, several family studies suggested autosomal-dominant inheritance of syndromes which, to variable degrees, resembled sporadic PD clinically and in some cases also neuropathologically. Recently, a disease locus has been mapped to chromosome 4q21-22 in a large Mediterranean pedigree, in which disease expression is clinically and pathologically within the spectrum of sporadic PD; being atypical only for a relatively young mean age at onset of 46 years and rapid course of 10 years from onset to death. In affected individuals of this family and of three unrelated Greek kindreds, a putative disease-causing mutation has been identified in the gene encoding alpha-synuclein. With the first variant being defined, genetic heterogeneity has become apparent, as in other families parkinsonism was not linked to the 4q-locus and was not associated with the alpha-synuclein mutation (unpublished data). We describe a different genetic locus that appears to be involved in the development of parkinsonism closely resembling sporadic PD including a similar mean age of onset (59 years in the families, 59.7 years in sporadic PD; ref. 12). This locus was detected in a group of families of European origin. In two of these families, there is genetic evidence for a common founder. The penetrance of the mutation appears to be low, most likely below 40%. This is compatible with a possible role of this locus not only in familial, but also in typical (sporadic) PD.

Published
1998
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45. Genetic complexity and Parkinson's disease.

Author

Gasser T, Müller-Myhsok B, Wszolek ZK, Dürr A, Vaughan JR, Bonifati V, Meco G, Bereznai B, Oehlmann R, Agid Y, Brice A, and Wood N

Subjects
Adult, Age of Onset, Humans, Lod Score, Microsatellite Repeats, Middle Aged, Mutation, Chromosomes, Human, Pair 4 genetics, Genetic Linkage, Parkinson Disease genetics
Published
1997

46. (3H)dipyridamole and (3H)nitrobenzylthioinosine binding sites at the human parietal cortex and erythrocyte adenosine transporter: a comparison.

Author

Deckert J, Hennemann A, Bereznai B, Fritze J, Vock R, Marangos PJ, and Riederer P

Subjects
Binding Sites, Binding, Competitive, Biological Transport, Humans, Thioinosine metabolism, Adenosine metabolism, Dipyridamole metabolism, Erythrocytes metabolism, Parietal Lobe metabolism, Thioinosine analogs & derivatives
Abstract

We compared the binding sites of the adenosine transport inhibitors (3H)dipyridamole (DPR) and (3H)nitrobenzylthioinosine (NBI) in human parietal cortex and erythrocytes. In comparison with guinea pig (3H)DPR marked only slightly more binding sites than (3H)NBI with a Bmax of 1080 +/- 29 and 780 +/- 7 fmol/mg protein respectively in parietal cortex and 24288 +/- 2725 and 20875 +/- 1905 fmol/mg protein respectively in erythrocytes. NBI displaced (3H)DPR binding completely from its binding sites at about KD/2 concentrations in parietal cortex as well as erythrocytes with inhibition constants comparable to its dissociation constants. Lineweaver-Burke analysis in erythrocytes indicated a competitive inhibition of (3H)DPR binding by NBI. Pharmacological characterization of (3H)DPR binding sites in human erythrocytes is consistent with their localization on adenosine transporters. These findings provide evidence that as opposed to guinea pig (3H)DPR and (3H)NBI largely label binding sites to the same adenosine transporter in human erythrocytes and parietal cortex.

Published
1994
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47. Nimodipine inhibits [3H]nitrobenzylthioinosine binding to the adenosine transporter in human brain.

Author

Deckert J, Bereznai B, Hennemann A, Gsell W, Götz M, Fritze J, and Riederer P

Subjects
Dihydropyridines metabolism, Dihydropyridines pharmacology, Humans, In Vitro Techniques, Parietal Lobe metabolism, Thioinosine metabolism, Nimodipine pharmacology, Parietal Lobe drug effects, Receptors, Purinergic P1 metabolism, Thioinosine analogs & derivatives
Abstract

The inhibition of [3H]nitrobenzylthioinosine ([3H]NBI) binding to human parietal cortex membranes by adenosine transport inhibitors, adenosine receptor agonists and antagonists and dihydropyridines was investigated. While the adenosine transport inhibitors inhibited [3H]NBI binding with Ki values in the low nanomolar range and the adenosine A1 receptor agonist, cyclopentyladenosine, with a Ki in the low micromolar range, no IC50 values could be obtained for the adenosine receptor antagonists at concentrations up to 100,000 nM. Among the dihydropyridines (+)-nimodipine was the most potent with a Ki of 201 +/- 55 nM. Inhibition of adenosine transport thus may contribute to the clinical effects of nimodipine in the central nervous system.

Published
1993
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