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11. Cloning of a novel gene bearing missense mutations in early-onset Alzheimer's disease

Author

Sherrington, R, Rogaev, Ei, Liang, Y, Rogaeva, Ea, Levesque, G, Ikeda, M, Chi, H, Lin, C, Li, G, Holman, K, Tsuda, T, Mar, L, Foncin, Jf, Bruni, Ac, Montesi, Mp, Sorbi, S, Rainero, Innocenzo, Pinessi, Lorenzo, Nee, L, Chumak, I, Pollen, D, Brookes, A, Sanseau, P, Polinski, Rj, and Wasco

Subjects
Alzheimer disease, gene mutation
Published
1995

12. Alzheimer's disease associated with mutations in presenilin 2 is rare and variably penetrant

Author

Maire E. Percy, Alexis Brice, M. Ikeda, Benedetta Nacmias, Chih-Ping Lin, P. St. George-Hyslop, Johanna M. Rommens, Luigi Amaducci, Dominique Campion, Silvia Piacentini, Yan Liang, L. Mar, R. Sherrington, G. Levesque, Sandro Sorbi, Ekaterina Rogaeva, Yves Agid, Thierry Frebourg, Evgeny I. Rogaev, Susanne Froelich, Gabriella Marcon, Françoise Clerget-Darpoux, Lars Lannfelt, H. Chi, Sherrington, R, Froelich, S, Sorbi, S, Campion, D, Chi, H, Rogaeva, Ea, Levesque, G, Rogaev, Ei, Lin, C, Liang, Y, Ikeda, M, Mar, L, Brice, A, Agid, Y, Percy, Me, CLERGET DARPOUX, F, Piacentini, S, Marcon, Gabriella, Nacmias, B, Amaducci, L, Frebourg, T, Lannfelt, L, Rommens, Jm, and ST GEORGE HYSLOP, Ph

Subjects
Male, DNA Mutational Analysis, Molecular Sequence Data, Gene mutation, Biology, medicine.disease_cause, Presenilin, Apolipoproteins E, Alzheimer Disease, Genotype, Presenilin-2, Genetics, medicine, Missense mutation, Humans, Point Mutation, Age of Onset, Molecular Biology, Gene, Genetics (clinical), Aged, Aged, 80 and over, Mutation, Alternative splicing, Membrane Proteins, General Medicine, Middle Aged, Penetrance, Pedigree, Female
Abstract

Missense mutations in the presenilin 2 (PS-2) gene on chromosome 1 were sought by direct nucleotide sequence analysis of the open reading frame of 60 pedigrees with familial Alzheimer's disease (FAD). In the majority of these pedigrees, PS-1 and beta-amyloid precursor protein (beta APP) gene mutations had been excluded. While no additional PS-2 pathogenic mutations were detected, four silent nucleotide substitutions and alternative splicing of nucleotides 1338-1340 (Glu325) were observed. Analysis of additional members of a pedigree known to segregate a Met239Val mutation in PS-2 revealed that the age of onset of symptoms is highly variable (range 45-88 years). This variability is not attributable to differences in ApoE genotypes. These results suggest (i) that, in contrast to mutations in PS-1, mutations in PS-2 are a relatively rare cause of FAD; (ii) that other genetic or environmental factor modify the AD phenotype associated with PS-2 mutations; and (iii) that still other FAD susceptibility genes remain to be identified.

Published
1996

13. Association of Body Mass Index and Parkinson Disease: A Bidirectional Mendelian Randomization Study.

Author

Domenighetti C, Sugier PE, Ashok Kumar Sreelatha A, Schulte C, Grover S, Portugal B, Lee PC, May P, Bobbili D, Radivojkov Blagojevic M, Lichtner P, Singleton AB, Hernandez D, Edsall C, Mellick GD, Zimprich AA, Pirker W, Rogaeva EA, Lang AE, Koks S, Taba P, Lesage S, Brice A, Corvol JC, Chartier-Harlin MC, Mutez E, Brockmann K, Deutschlander AB, Hadjigeorgiou GM, Dardiotis E, Stefanis L, Simitsi AM, Valente EM, Petrucci S, Straniero L, Zecchinelli AL, Pezzoli G, Brighina L, Ferrarese C, Annesi G, Quattrone A, Gagliardi M, Matsuo H, Nakayama A, Hattori N, Nishioka K, Chung SJ, Kim YJ, Kolber P, Van De Warrenburg BPC, Bloem BR, Toft M, Pihlstrøm L, Correia Guedes L, Ferreira JJ, Bardien S, Carr J, Tolosa E, Ezquerra M, Pastor P, Diez-Fairen M, Wirdefeldt K, Pedersen NL, Ran C, Belin AC, Puschmann A, Hellberg C, Clarke CE, Morrison KE, Tan MM, Krainc D, Burbulla LF, Farrer M, Kruger R, Gasser T, Sharma M, and Elbaz A

Subjects
Humans, Female, Male, Middle Aged, Aged, Risk Factors, Mendelian Randomization Analysis, Parkinson Disease genetics, Parkinson Disease epidemiology, Body Mass Index, Polymorphism, Single Nucleotide genetics, Genome-Wide Association Study
Abstract

Background and Objectives: The role of body mass index (BMI) in Parkinson disease (PD) is unclear. Based on the Comprehensive Unbiased Risk Factor Assessment for Genetics and Environment in PD (Courage-PD) consortium, we used 2-sample Mendelian randomization (MR) to replicate a previously reported inverse association of genetically predicted BMI with PD and investigated whether findings were robust in analyses addressing the potential for survival and incidence-prevalence biases. We also examined whether the BMI-PD relation is bidirectional by performing a reverse MR., Methods: We used summary statistics from a genome-wide association study (GWAS) to extract the association of 501 single-nucleotide polymorphisms (SNPs) with BMI and from the Courage-PD and international Parkinson Disease Genomics Consortium (iPDGC) to estimate their association with PD. Analyses are based on participants of European ancestry. We used the inverse-weighted method to compute odds ratios (OR IVW per 4.8 kg/m 2 [95% CI]) of PD and additional pleiotropy robust methods. We performed analyses stratified by age, disease duration, and sex. For reverse MR, we used SNPs associated with PD from 2 iPDGC GWAS to assess the effect of genetic liability toward PD on BMI., Results: Summary statistics for BMI are based on 806,834 participants (54% women). Summary statistics for PD are based on 8,919 (40% women) cases and 7,600 (55% women) controls from Courage-PD, and 19,438 (38% women) cases and 24,388 (51% women) controls from iPDGC. In Courage-PD, we found an inverse association between genetically predicted BMI and PD (OR IVW 0.82 [0.70-0.97], p = 0.012) without evidence for pleiotropy. This association tended to be stronger in younger participants (≤67 years, OR IVW 0.71 [0.55-0.92]) and cases with shorter disease duration (≤7 years, OR IVW 0.75 [0.62-0.91]). In pooled Courage-PD + iPDGC analyses, the association was stronger in women (OR IVW 0.85 [0.74-0.99], p = 0.032) than men (OR IVW 0.92 [0.80-1.04], p = 0.18), but the interaction was not statistically significant ( p -interaction = 0.48). In reverse MR, there was evidence for pleiotropy, but pleiotropy robust methods showed a significant inverse association., Discussion: Using an independent data set (Courage-PD), we replicate an inverse association of genetically predicted BMI with PD, not explained by survival or incidence-prevalence biases. Moreover, reverse MR analyses support an inverse association between genetic liability toward PD and BMI, in favor of a bidirectional relation.

Published
2024
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14. Occurrence of Amyotrophic Lateral Sclerosis in Type 1 Gaucher Disease.

Author

Oliveira LM, Rastin T, Nimmo GAM, Ross JP, Dion PA, Zhang M, Nevay DL, Arkadir D, Gotkine M, Barnett C, Shoesmith CL, Zimran A, Rogaeva EA, Zinman L, Rouleau GA, Gan-Or Z, Amato D, and Kalia LV

Abstract

Objective: To report the association between type 1 Gaucher disease (GD1) and amyotrophic lateral sclerosis (ALS) in 3 unrelated families and to explore whether GBA variants influence the risk of ALS., Methods: We conducted retrospective chart reviews of patients with GD1 or their family members diagnosed with ALS. To further investigate whether there is an association between ALS and GD, we performed exploratory analyses for the presence of GBA variants in 3 ALS cohorts from Toronto (Canada), Montreal (Canada), and Project MinE (international), totaling 4,653 patients with ALS and 1,832 controls., Results: We describe 2 patients with GD1 and 1 obligate GBA mutation carrier (mother of GD1 patient) with ALS. We identified 0 and 8 GBA carriers in the Toronto and Montreal cohorts, respectively. The frequencies of GBA variants in patients with ALS in the Montreal and Project MinE cohorts were similar to those of Project MinE controls or Genome Aggregation Database population controls., Conclusions: The occurrence of ALS in biallelic or monoallelic GBA mutation carriers described here, in addition to common pathogenic pathways shared by GD1 and ALS, suggests that GBA variants could influence ALS risk. However, analyses of GBA variants in ALS cohorts did not reveal a meaningful association. Examination of larger cohorts and neuropathologic studies will be required to elucidate whether patients with GD1 are indeed at increased risk for ALS., (Copyright © 2021 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published
2021
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15. SPATACSIN mutations cause autosomal recessive juvenile amyotrophic lateral sclerosis.

Author

Orlacchio A, Babalini C, Borreca A, Patrono C, Massa R, Basaran S, Munhoz RP, Rogaeva EA, St George-Hyslop PH, Bernardi G, and Kawarai T

Subjects
Adult, Age Factors, Amyotrophic Lateral Sclerosis diagnosis, Female, Genes, Recessive genetics, Humans, Male, Middle Aged, Pedigree, Amyotrophic Lateral Sclerosis genetics, Mutation genetics, Proteins genetics
Abstract

The mutation of the spatacsin gene is the single most common cause of autosomal recessive hereditary spastic paraplegia with thin corpus callosum. Common clinical, pathological and genetic features between amyotrophic lateral sclerosis and hereditary spastic paraplegia motivated us to investigate 25 families with autosomal recessive juvenile amyotrophic lateral sclerosis and long-term survival for mutations in the spatascin gene. The inclusion criterion was a diagnosis of clinically definite amyotrophic lateral sclerosis according to the revised El Escorial criteria. The exclusion criterion was a diagnosis of hereditary spastic paraplegia with thin corpus callosum in line with an established protocol. Additional pathological and genetic evaluations were also performed. Surprisingly, 12 sequence alterations in the spatacsin gene (one of which is novel, IVS30 + 1 G > A) were identified in 10 unrelated pedigrees with autosomal recessive juvenile amyotrophic lateral sclerosis and long-term survival. The countries of origin of these families were Italy, Brazil, Canada, Japan and Turkey. The variants seemed to be pathogenic since they co-segregated with the disease in all pedigrees, were absent in controls and were associated with amyotrophic lateral sclerosis neuropathology in one member of one of these families for whom central nervous system tissue was available. Our study indicates that mutations in the spatascin gene could cause a much wider spectrum of clinical features than previously recognized, including autosomal recessive juvenile amyotrophic lateral sclerosis.

Published
2010
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16. Mutations in the open reading frame of the beta-site APP cleaving enzyme (BACE) locus are not a common cause of Alzheimer's disease.

Author

Nicolaou M, Song YQ, Sato CA, Orlacchio A, Kawarai T, Medeiros H, Liang Y, Sorbi S, Richard E, Rogaev EI, Moliaka Y, Bruni AC, Jorge R, Percy M, Duara R, Farrer LA, St Georg-Hyslop P, and Rogaeva EA

Subjects
Aged, Aged, 80 and over, Amyloid Precursor Protein Secretases, DNA Mutational Analysis, Endopeptidases, Genetic Linkage, Genetic Markers, Genotype, Humans, Middle Aged, Mutation, Alzheimer Disease genetics, Aspartic Acid Endopeptidases genetics, Open Reading Frames genetics
Abstract

Amyloid beta-peptide (Abeta) plays a central role in the pathogenesis of Alzheimer's disease (AD). The gene encoding the beta-site APP cleaving enzyme (BACE), one of two enzymes that sequentially cleave the beta-amyloid precursor protein to generate Abeta, has recently been cloned. We tested the hypothesis that BACE might be genetically associated with AD by linkage analysis (56 pedigrees), by direct nucleotide sequencing of the entire open reading frame (20 subjects with familial AD, and 10 subjects with sporadic AD) and by allelic association analysis (155 AD cases and 173 non-demented controls). Our results revealed no evidence for either genetic linkage or allelic association between BACE and AD, and no coding sequence mutations were detected in the open reading frame of the BACE gene. These data suggest that while BACE protein plays an important role in the pathogenesis of AD, and may be a robust therapeutic target, it is unlikely to be a major AD susceptibility locus.

Published
2001
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17. Screening for PS1 mutations in a referral-based series of AD cases: 21 novel mutations.

Author

Rogaeva EA, Fafel KC, Song YQ, Medeiros H, Sato C, Liang Y, Richard E, Rogaev EI, Frommelt P, Sadovnick AD, Meschino W, Rockwood K, Boss MA, Mayeux R, and St George-Hyslop P

Subjects
Adult, Aged, Aged, 80 and over, Alzheimer Disease diagnosis, Humans, Middle Aged, Presenilin-1, Referral and Consultation, Survival Analysis, Alzheimer Disease genetics, Genetic Testing methods, Membrane Proteins genetics, Mutation genetics
Abstract

Background: Mutations in the presenilin-1 gene (PS1) account for a majority of patients with early-onset familial AD. However, the clinical indications and algorithms for genetic testing in dementia are still evolving., Methods: The entire open reading frame of the PS1 gene was sequenced in a series of 414 consecutive patients referred for diagnostic testing, including 372 patients with AD and 42 asymptomatic persons with a strong family history of AD., Results: Forty-eight independent patients screened had a PS1 mutation including 21 novel mutations. In addition, 3% of subjects (11/413) had a known polymorphism, the Glu318Gly substitution. The majority of the mutations were missense substitutions but there were three insertions and Delta exon 10 mutation. With six exceptions (codons 35, 178, 352, 354, 358, and 365) most of the mutations occurred at residues conserved in the homologous PS2 gene or in PS1 of other species., Conclusions: Eleven percent of a referral-based series of patients with AD can be explained by coding sequence mutations in the PS1 gene. The high frequency of PS1 mutations in this study indicates that screening for PS1 mutations in AD is likely to be successful, especially when directed at patients with a positive family history with onset before 60 years (90% of those with PS1 mutations were affected by age 60 years). This will also have significance for the secondary identification of at-risk relatives who might be candidates for future prophylactic therapies for AD.

Published
2001
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18. Association between angiotensin-converting enzyme and Alzheimer disease.

Author

Farrer LA, Sherbatich T, Keryanov SA, Korovaitseva GI, Rogaeva EA, Petruk S, Premkumar S, Moliaka Y, Song YQ, Pei Y, Sato C, Selezneva ND, Voskresenskaya S, Golimbet V, Sorbi S, Duara R, Gavrilova S, St George-Hyslop PH, and Rogaev EI

Subjects
Aged, Alleles, Alzheimer Disease epidemiology, Alzheimer Disease genetics, Apolipoproteins E genetics, Apolipoproteins E metabolism, DNA analysis, DNA genetics, DNA Primers, Female, Gene Frequency, Genotype, Humans, Male, Moscow epidemiology, Ontario epidemiology, Peptidyl-Dipeptidase A genetics, Risk Factors, Alzheimer Disease enzymology, Peptidyl-Dipeptidase A metabolism
Abstract

Background: Angiotensin-converting enzyme has been reported to show altered activity in patients with neurologic diseases. An insertion-deletion polymorphism in ACE has recently been linked to heart disease, cerebrovascular disease, and AD., Objective: To determine whether the angiotensin-converting enzyme (ACE) is associated with risk of Alzheimer disease (AD)., Methods: We investigated the ACE polymorphism as a potential risk factor for AD in 151 patients with AD and 206 ethnically matched controls from Russia and in 236 patients with AD and 169 controls from North America by means of allele association methods and logistic regression., Results: None of the ACE genotypes was associated with increased susceptibility to AD in the total sample or in subsets stratified by apolipoprotein E gene (APOE) epsilon4 status. However, the D allele was more frequent among AD cases between ages 66 and 70 years compared with controls in both the Russian (P = .02) and North American (P = .001) datasets. In this age group, the effect of D (odds ratio, 11.2; 95% confidence interval, 2.9-44.0) appeared to be independent of and equal or greater in magnitude to the effect of APOE epsilon4 (odds ratio, 7.8; 95% confidence interval, 3.5-7.4)., Conclusions: Our results suggest that APOE and ACE genotypes may be independent risk factors for late-onset AD, but the ACE association needs to be confirmed in independent samples in which the time and extent of vascular cofactors can be assessed.

Published
2000
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19. Aberrant splicing in the presenilin-1 intron 4 mutation causes presenile Alzheimer's disease by increased Abeta42 secretion.

Author

De Jonghe C, Cruts M, Rogaeva EA, Tysoe C, Singleton A, Vanderstichele H, Meschino W, Dermaut B, Vanderhoeven I, Backhovens H, Vanmechelen E, Morris CM, Hardy J, Rubinsztein DC, St George-Hyslop PH, and Van Broeckhoven C

Subjects
Age of Onset, Alzheimer Disease metabolism, Amino Acid Sequence, Animals, Base Sequence, CHO Cells, Cell Line, Cricetinae, DNA chemistry, DNA genetics, DNA Mutational Analysis, DNA, Complementary genetics, Family Health, Female, Gene Expression, Humans, Male, Molecular Sequence Data, Mutagenesis, Site-Directed, Mutation, Pedigree, Presenilin-1, Transfection, Tumor Cells, Cultured, Alternative Splicing, Alzheimer Disease genetics, Amyloid beta-Peptides metabolism, Introns genetics, Membrane Proteins genetics, Peptide Fragments metabolism
Abstract

We previously described a splice donor site mutation in intron 4 of presenilin-1 (PSEN1) in two patients with autopsy-confirmed early-onset Alzheimer's disease (AD). Here we provide evidence that the intron 4 mutation is present in four additional unrelated early-onset AD cases, that the mutation segregates in an autosomal dominant manner and that all cases have one common ancestor. We demonstrate that the intron 4 mutation produces three different transcripts, two deletion transcripts (Delta4 and Delta4cryptic) and one insertion transcript (insTAC), by aberrant splicing. The deletion transcripts result in the formation of C-truncated (approximately 7 kDa) PSEN1 proteins while the insertion transcript produces a full-length PSEN1 with one extra amino acid (Thr) inserted between codons 113 and 114 (PSEN1 T113-114ins). The truncated proteins were not detectable in vivo in brain homogenates or lymphoblast lysates of mutation carriers. In vitro HEK-293 cells overexpressing Delta4, Delta4cryptic or insTACPSEN1 cDNAs showed increased Abeta42 secretion (approximately 3.4 times) only for the insertion cDNA construct. Increased Abeta42 production was also observed in brain homogenates. Our data indicate that in the case of intron 4 mutation, the AD pathophysiology results from the presence of the PSEN1 T113-114ins protein comparable with cases carrying dominant PSEN1 missense mutations.

Published
1999
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20. An alpha-2-macroglobulin insertion-deletion polymorphism in Alzheimer disease.

Author

Rogaeva EA, Premkumar S, Grubber J, Serneels L, Scott WK, Kawarai T, Song Y, Hill DL, Abou-Donia SM, Martin ER, Vance JJ, Yu G, Orlacchio A, Pei Y, Nishimura M, Supala A, Roberge B, Saunders AM, Roses AD, Schmechel D, Crane-Gatherum A, Sorbi S, Bruni A, Small GW, Conneally PM, Haines JL, Van Leuven F, St George-Hyslop PH, Farrer LA, and Pericak-Vance MA

Subjects
Alleles, Alzheimer Disease blood, Gene Deletion, Gene Frequency, Genotype, Humans, Mutagenesis, Insertional, Polymorphism, Genetic, alpha-Macroglobulins metabolism, Alzheimer Disease genetics, alpha-Macroglobulins genetics
Published
1999
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21. Association between bleomycin hydrolase and Alzheimer's disease in caucasians.

Author

Farrer LA, Abraham CR, Haines JL, Rogaeva EA, Song Y, McGraw WT, Brindle N, Premkumar S, Scott WK, Yamaoka LH, Saunders AM, Roses AD, Auerbach SA, Sorbi S, Duara R, Pericak-Vance MA, and St George-Hyslop PH

Subjects
Aged, Alleles, Apolipoproteins E genetics, Boston, Female, Gene Frequency, Genotype, Humans, Male, North Carolina, Reference Values, Alzheimer Disease genetics, Cysteine Endopeptidases genetics, Polymorphism, Genetic, White People genetics
Abstract

A recent study showed modest evidence for an increased frequency of the bleomycin hydrolase (BH) V/V genotype in Alzheimer's disease (AD) patients compared with non-demented controls. To test this hypothesis, we examined this polymorphism in 621 rigorously evaluated patients and 502 control subjects (all caucasian) but were unable to detect an association between BH and AD even after controlling for age, gender, and apolipoprotein E (ApoE) genotype. We conclude that this polymorphism does not account for inherited susceptibility to AD in the populations represented in this sample.

Published
1998
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22. A novel Leu171Pro mutation in presenilin-1 gene in a Mexican family with early onset Alzheimer disease.

Author

Ramirez-Dueñas MG, Rogaeva EA, Leal CA, Lin C, Ramirez-Casillas GA, Hernandez-Romo JA, St George-Hyslop PH, and Cantu JM

Subjects
Adult, Age of Onset, Amino Acid Substitution, Humans, Leucine, Mexico, Pedigree, Polymerase Chain Reaction, Presenilin-1, Proline, Alzheimer Disease genetics, Membrane Proteins genetics, Mutation, Missense
Abstract

A search for mutations in exons 6, 7, 9 and 12 of the PS1 gene in four Mexican families with Early-Onset (36-40 years) Alzheimer Disease yielded the discovery in one family of a T-->C mismatch in exon 7 which correspond to nucleotide 760 of cDNA, leading to a Leu171Pro mutation. The pedigree analysis and the literature data strongly suggest an etiopathogenic relationship of the mutation with the disorder.

Published
1998

23. Analysis of the 5' sequence, genomic structure, and alternative splicing of the presenilin-1 gene (PSEN1) associated with early onset Alzheimer disease.

Author

Rogaev EI, Sherrington R, Wu C, Levesque G, Liang Y, Rogaeva EA, Ikeda M, Holman K, Lin C, Lukiw WJ, de Jong PJ, Fraser PE, Rommens JM, and St George-Hyslop P

Subjects
Alternative Splicing, Amino Acid Sequence, Base Sequence, Humans, Molecular Sequence Data, Presenilin-1, Sequence Analysis, DNA, Alzheimer Disease genetics, Genome, Human, Membrane Proteins genetics
Abstract

Mutations in the human presenilin genes (PSEN1 and PSEN2) are associated with early onset familial Alzheimer disease. The presenilin genes encode integral membrane proteins with similar structures, which suggests that they may have closely related, but as yet unknown functions. Analysis of the 5' upstream sequence and the structure of the PSEN1 gene reveals that the 5' sequence contains multiple putative transcription regulatory elements including clusters of STAT elements involved in transcriptional activation in response to signal transduction. The first four exons contain untranslated sequences, with Exons 1 and 2 representing alternate initial transcription sites. The function of these alternate initial exons is unclear. Exon 4 bears the first ATG sequence. The last 12 bp of Exon 4 is used as an alternative splice donor site. Exon 9 is alternately spliced in leukocytes, but not in most other tissues. Splicing of Exon 9 is predicted to cause significant structural changes to the protein. The majority of transcripts expressed in most tissues are polyadenylated 1127 bp from the TAG stop codon in Exon 13. A small proportion of transcripts contain the same 5'UTR and ORF but are polyadenylated 4435 bp from the stop codon. The longer polyadenylated transcripts contain three additional palindromes and at least one additional stem-loop structure with stabilities greater than -16 kcal/mol.

Published
1997
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24. Interfamilial and intrafamilial phenotypic heterogeneity in familial Alzheimer's disease.

Author

Lopez-Alberola RF, Barker WW, Harwood DG, Loewenstein DA, George-Hyslop PH, Tsuda T, Rogaeva EA, and Duara R

Subjects
Aged, Aged, 80 and over, Alzheimer Disease diagnosis, Alzheimer Disease psychology, Apolipoproteins E genetics, Atrophy, Cerebral Cortex pathology, Female, Genetic Heterogeneity, Genotype, Humans, Male, Middle Aged, Neuropsychological Tests, Alzheimer Disease genetics, Family, Phenotype
Abstract

The features of Alzheimer's disease (AD) are very heterogenous, and some component of the variability of AD is likely to be related to genetic factors. To investigate this question, we evaluated 19 clinical neuropsychiatric and brain imaging features in 32 familial Alzheimer's disease (FAD) kindred, primarily of late onset. Within families, patients displayed a high degree of phenotypic heterogeneity (PH), which occurred irrespective of gender, ethnicity, or apolipoprotein E genotype. Overall, an equivalent amount of PH was observed in both the between- (37%) and within-family (31%) groups. However, for onset age and rate of decline between families, there was greater PH than within families (P = .002 and P = .01, respectively). A similar trend was found for severity of cortical atrophy (P = .05). These observations suggest a weak genetic influence, and possibly strong nongenetic influences, on the degree of phenotypic heterogeneity in late-onset FAD. In early-onset AD kindred, a much smaller degree of phenotypic heterogeneity may be expected within families, because genetic influences in phenotypic expression tend to be more prominent in early-onset cases.

Published
1997
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25. [Comparison of mitochondrial DNA sequences of T.N. Kulikovskiĭ-Romanov, the nephew of Tsar Nikolaĭ II Romanov, with DNA from the putative remains of the Tsar].

Author

Rogaev EI, Ovchinnikov IV, Dzhorzh-Khislop P, and Rogaeva EA

Subjects
Humans, Male, Pedigree, Polymerase Chain Reaction, DNA, Mitochondrial genetics, Forensic Anthropology methods, Sequence Homology, Nucleic Acid
Abstract

Analysis of two polymorphic regions of mitochondrial DNA obtained from T. N. Kulikovskii-Romanov, the nephew of the last Tsar of the Russian Empire Nikolai II Romanov, was performed. The mitochondrial DNA sequences of T. N. Kulikovskii-Romanov and earlier reported DNA sequences obtained from the putative remains of Nikolai II showed almost complete coincidence except for a single nucleotide at the position 16169. At this position, C was found in mitochondrial DNA of T. N. Kulikovskii-Romanov, C/T in that from the putative remains of Nikolai II Romanov, and T in mitochondrial DNA from great great grandson and great great grand-daughter of Louise Hesse-Cassel. These data suggest independent mutations in the maternal lineage of Louise Hesse-Cassel's descendants and/or a mutation leading to a heteroplasmia in the lineage of Louise Hesse-Cassel.

Published
1996

26. The clinical phenotype of two missense mutations in the presenilin I gene in Japanese patients.

Author

Ikeda M, Sharma V, Sumi SM, Rogaeva EA, Poorkaj P, Sherrington R, Nee L, Tsuda T, Oda N, Watanabe M, Aoki M, Shoji M, Abe K, Itoyama Y, Hirai S, Schellenberg GD, Bird TD, and St George-Hyslop PH

Subjects
Adult, Alzheimer Disease pathology, Base Sequence, Brain pathology, Female, Hippocampus pathology, Humans, Male, Membrane Proteins genetics, Middle Aged, Molecular Sequence Data, Neurofibrillary Tangles pathology, Pedigree, Phenotype, Presenilin-1, Alzheimer Disease genetics, Mutation
Abstract

We report the clinical and neuropathologic phenotypes associated with two different missense mutations in the presenilin 1 (PS-1) gene in Japanese patients with early-onset familial Alzheimer's disease (FAD). In the AM/JPN1 pedigree a missense mutation (C-->T) was found at nucleotide 1102, which is predicted to cause an alanine-to-valine missense substitution at codon 260. In this family, the disease had a mean age of onset of 40.3 years and an indolent course (range, 8-19 years). Neuropathologic studies in 3 members of this pedigree showed widespread senile plaques, neurofibrillary tangles, and neuronal loss, as well as abundant perivascular subpial amyloid deposits in the Virchow-Robin spaces and the presence of Pick-like intraneuronal inclusions in the dentate gyrus. In the second pedigree, transmitting a C-->T nucleotide substitution at position 1027, leading to the missense mutation of alanine to valine at codon 285, the disease had a later onset (mean, 51 years) but a more rapid course. Comparison of the disease phenotypes associated with other missense mutations in exon 9 of PS-1 reveals no clinical or pathological phenotype, which uniquely distinguishes Alzheimer's disease associated with PS-1 mutations from other forms of early-onset FAD, implying that direct mutation screening is required to identify these cases.

Published
1996
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27. Intergenerational instability of the CAG repeat of the gene for Machado-Joseph disease (MJD1) is affected by the genotype of the normal chromosome: implications for the molecular mechanisms of the instability of the CAG repeat.

Author

Igarashi S, Takiyama Y, Cancel G, Rogaeva EA, Sasaki H, Wakisaka A, Zhou YX, Takano H, Endo K, Sanpei K, Oyake M, Tanaka H, Stevanin G, Abbas N, Dürr A, Rogaev EI, Sherrington R, Tsuda T, Ikeda M, Cassa E, Nishizawa M, Benomar A, Julien J, Weissenbach J, Wang GX, Agid Y, St George-Hyslop PH, Brice A, and Tsuji S

Subjects
Female, Gene Frequency, Humans, Machado-Joseph Disease ethnology, Male, Risk, Sex Factors, Chromosomes, Human, Pair 14 genetics, Genotype, Machado-Joseph Disease genetics, Polymorphism, Genetic, Trinucleotide Repeats genetics
Abstract

Machado-Joseph disease (MJD) is an autosomal dominant neurodegenerative disorder caused by unstable expansion of a CAG repeat in the MJD1 gene at 14q32.1. To identify elements affecting the intergenerational instability of the CAG repeat, we investigated whether the CGG/GGG polymorphism at the 3' end of the CAG repeat affects intergenerational instability of the CAG repeat. The [expanded (CAG)n-CGG]/[normal (CAG)n-GGG] haplotypes were found to result in significantly greater instability of the CAG repeat compared to the [expanded (CAG)n-CGG]/[normal (CAG)n-CGG] or [expanded (CAG)nGGG]/[normal (CAG)n-GGG] haplotypes. Multiple stepwise logistic regression analysis revealed that the relative risk for a large intergenerational change in the number of CAG repeat units (< -2 or > 2) is 7.7-fold (95% CI: 2.5-23.9) higher in the case of paternal transmission than in that of maternal transmission and 7.4-fold (95% CI: 2.4-23.3) higher in the case of transmission from a parent with the [expanded (CAG)n-CGG]/[normal (CAG)n-GGG] haplotypes than in that of transmission from a parent with the [expanded (CAG)n-CGG]/[normal (CAG)n-CGG] or [expanded (CAG)n-GGG]/[normal (CAG)n-GGG] haplotypes. The combination of paternal transmission and the [expanded (CAG)n-CGG]/[normal (CAG)n-GGG] haplotypes resulted in a 75.2-fold (95% CI: 9.0-625.0) increase in the relative risk compared with that of maternal transmission and the [expanded (CAG)n-CGG]/[normal (CAG)n-CGG] or [expanded (CAG)n-GGG]/[normal (CAG)n-GGG] haplotypes. The results suggest that an inter-allelic interaction is involved in the intergenerational instability of the expanded CAG repeat.

Published
1996
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28. Alzheimer's disease associated with mutations in presenilin 2 is rare and variably penetrant.

Author

Sherrington R, Froelich S, Sorbi S, Campion D, Chi H, Rogaeva EA, Levesque G, Rogaev EI, Lin C, Liang Y, Ikeda M, Mar L, Brice A, Agid Y, Percy ME, Clerget-Darpoux F, Piacentini S, Marcon G, Nacmias B, Amaducci L, Frebourg T, Lannfelt L, Rommens JM, and St George-Hyslop PH

Subjects
Age of Onset, Aged, Aged, 80 and over, Apolipoproteins E genetics, DNA Mutational Analysis, Female, Humans, Male, Middle Aged, Molecular Sequence Data, Pedigree, Presenilin-2, Alzheimer Disease genetics, Membrane Proteins genetics, Point Mutation genetics
Abstract

Missense mutations in the presenilin 2 (PS-2) gene on chromosome 1 were sought by direct nucleotide sequence analysis of the open reading frame of 60 pedigrees with familial Alzheimer's disease (FAD). In the majority of these pedigrees, PS-1 and beta-amyloid precursor protein (beta APP) gene mutations had been excluded. While no additional PS-2 pathogenic mutations were detected, four silent nucleotide substitutions and alternative splicing of nucleotides 1338-1340 (Glu325) were observed. Analysis of additional members of a pedigree known to segregate a Met239Val mutation in PS-2 revealed that the age of onset of symptoms is highly variable (range 45-88 years). This variability is not attributable to differences in ApoE genotypes. These results suggest (i) that, in contrast to mutations in PS-1, mutations in PS-2 are a relatively rare cause of FAD; (ii) that other genetic or environmental factor modify the AD phenotype associated with PS-2 mutations; and (iii) that still other FAD susceptibility genes remain to be identified.

Published
1996
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29. Linkage of polymorphic congenital cataract to the gamma-crystallin gene locus on human chromosome 2q33-35.

Author

Rogaev EI, Rogaeva EA, Korovaitseva GI, Farrer LA, Petrin AN, Keryanov SA, Turaeva S, Chumakov I, St George-Hyslop P, and Ginter EK

Subjects
Cataract genetics, Databases, Factual, Female, Genes, Dominant, Humans, Male, Pedigree, Phenotype, Point Mutation, Cataract congenital, Chromosomes, Human, Pair 2, Crystallins genetics, Genetic Linkage, Polymorphism, Genetic
Abstract

Cataract is one of the major causes of blindness in humans. We describe here an autosomal dominant polymorphic congenital cataract (PCC) which is characterised by wide variations in phenotype of non-nuclear lens opacities, even among affected members of the same family. PCC families included a large, unique pedigree (254 members, 103 affected individuals), and genetic linkage was conducted using a variety of polymorphic markers. Evidence for linkage was found for chromosome 2q33-35 with PCC mapping near D2S72 and TNP1. A tri-nucleotide microsatellite marker for gamma-crystallin B gene (CRYG1) was found to co-segregate with PCC and yielded a maximum lod score of 10.62 at (theta = 0). A multipoint analysis demonstrated that the most probable location of the PCC gene was within an 8 cM genetic interval containing the gamma-crystallin gene cluster. These data provide strong evidence of the existence of an autosomal dominant mutation for PCC in or near the gamma-crystallin gene cluster. This defect is characterised by complete penetrance but variable expression of the cataract phenotype. Our study also suggests that non-nuclear human cataracts might be caused by some abnormality in gamma-crystallin genes.

Published
1996
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30. Failure to detect missense mutations in the S182 gene in a series of late-onset Alzheimer's disease cases.

Author

Tsuda T, Chi H, Liang Y, Rogaeva EA, Sherrington R, Levesque G, Ikeda M, Rogaev EI, Pollen D, and Freedman M

Subjects
Aged, Base Sequence, Cloning, Molecular, DNA Primers, Genes, Humans, Molecular Sequence Data, Mutation physiology, Polymerase Chain Reaction, Presenilin-1, Alzheimer Disease genetics, Membrane Proteins genetics, Mutation genetics
Abstract

The possibility of an interaction of multiple genes has been speculated in pathogenesis of Alzheimer's disease (AD). Because we have recently cloned a novel gene S182 bearing five different missense mutations which segregate with early-onset familial AD, we sought the frequency of these mutations in familial and sporadic late-onset AD to clarify the incidence of these mutations in the disease. The current study showed lack of these mutations in 118 independent subjects affected with late-onset Alzheimer's disease.

Published
1995
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31. Dopa-responsive parkinsonism phenotype of Machado-Joseph disease: confirmation of 14q CAG expansion.

Author

Tuite PJ, Rogaeva EA, St George-Hyslop PH, and Lang AE

Subjects
DNA analysis, Female, Humans, Male, Middle Aged, Parkinson Disease drug therapy, Chromosomes, Human, Pair 14, Dihydroxyphenylalanine therapeutic use, Machado-Joseph Disease genetics, Parkinson Disease genetics, Repetitive Sequences, Nucleic Acid
Abstract

The subtype IV of Machado-Joseph disease (MJD), characterized by parkinsonism variably combined with ataxia, distal atrophy, and sensory loss, has been all but ignored in recent reports of MJD, including those describing the molecular biologic substrate of the disease. We have demonstrated expansion of the CAG trinucleotide repeat of the MJD1 gene located on chromosome 14q32.1 in 2 patients of Azorean descent who presented with levodopa-responsive atypical parkinsonism. Previous publications have documented the presence of this expanded repeat in the other more common MJD phenotypes (I-III). To our knowledge, this is the first molecular biologic confirmation of the presence of the MJD1 gene in the subtype IV phenotype. Patients presenting with parkinsonism and peripheral neuropathy should be screened for this genetic defect.

Published
1995
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32. Familial Alzheimer's disease in kindreds with missense mutations in a gene on chromosome 1 related to the Alzheimer's disease type 3 gene.

Author

Rogaev EI, Sherrington R, Rogaeva EA, Levesque G, Ikeda M, Liang Y, Chi H, Lin C, Holman K, and Tsuda T

Subjects
Alzheimer Disease classification, Amino Acid Sequence, Base Sequence, DNA, Humans, Membrane Proteins physiology, Molecular Sequence Data, Presenilin-1, Presenilin-2, Sequence Homology, Amino Acid, Alzheimer Disease genetics, Chromosomes, Human, Pair 1, Membrane Proteins genetics, Mutation
Abstract

We report the cloning of a novel gene (E5-1) encoded on chromosome 1 which has substantial nucleotide and amino-acid sequence similarity to the S182 gene on chromosome 14q24.3. Mutations, including three new missense mutations in the S182 gene, are associated with the AD3 subtype of early-onset familial Alzheimer's disease (AD). Both the E5-1 and the S182 proteins are predicted to be integral membrane proteins with seven membrane-spanning domains, and a large exposed loop between the sixth and seventh transmembrane domains. Analysis of the nucleotide sequence of the open reading frame (ORF) of the E5-1 gene led to the discovery of two missense substitutions at conserved amino-acid residues in affected members of pedigrees with a form of familial AD that has a later age of onset than the AD3 subtype (50-70 years versus 30-60 years for AD3). These observations imply that the E5-1 gene on chromosome 1 and the S182 gene on chromosome 14q24.3 are members of a family of genes (presenilins) with related functions, and indicates that mutations in conserved residues of E5-1 could also play a role in the genesis of AD. Our results also indicate that still other AD susceptibility genes exist.

Published
1995
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33. Evidence for inter-generational instability in the CAG repeat in the MJD1 gene and for conserved haplotypes at flanking markers amongst Japanese and Caucasian subjects with Machado-Joseph disease.

Author

Takiyama Y, Igarashi S, Rogaeva EA, Endo K, Rogaev EI, Tanaka H, Sherrington R, Sanpei K, Liang Y, and Saito M

Subjects
Age of Onset, Alleles, Ataxin-3, Base Sequence, Conserved Sequence, Female, Genetics, Population, Homozygote, Humans, Japan epidemiology, Machado-Joseph Disease epidemiology, Male, Meiosis, Molecular Sequence Data, Nuclear Proteins, Pedigree, Phenotype, Polymorphism, Genetic, Proteins genetics, Repressor Proteins, Asian People genetics, Haplotypes genetics, Machado-Joseph Disease genetics, Nerve Tissue Proteins, Repetitive Sequences, Nucleic Acid genetics, White People genetics
Abstract

The size of the (CAG)n repeat array in the 3' end of the MJD1 gene and the haplotype at a series of microsatellite markers surrounding the MJD1 gene were examined in a large cohort of Japanese and Caucasian subjects affected with Machado-Joseph disease (MJD). Our data provide five novel observations. First, MJD is associated with expansion fo the array from the normal range of 14-37 repeats to 68-84 repeats in most Japanese and Caucasian subjects, but no subjects were observed with expansions intermediate in size between those of the normal and MJD affected groups. Second, the expanded allele associated with MJD displays inter-generational instability, particularly in male meioses, and this instability was associated with the clinical phenomenon of anticipation. Third, the size of the expanded allele is not only inversely correlated with the age-of-onset of MJD (r = -0.738, p < 0.001), but is also correlated with the frequency of other clinical features [e.g. pseudoexophthalmos and pyramidal signs were more frequent in subjects with large repeats (p < 0.001 and p < 0.05 respectively)]. Fourth, the disease phenotype is significantly more severe and had an early age of onset (16 years) in a subject homozygous for the expanded allele, which contrasts with Huntington disease and suggests that the expanded allele in the MJD1 gene could exert its effect either by a dominant negative effect (putatively excluded in HD) or by a gain of function effect as proposed for HD. Finally, Japanese and Caucasian subjects affected with MJD share haplotypes at several markers surrounding the MJD1 gene, which are uncommon in the normal Japanese and Caucasian population, and which suggests the existence either of common founders in these populations or of chromosomes susceptible to pathologic expansion of the CAG repeat in the MJD1 gene.

Published
1995
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34. Cloning of a gene bearing missense mutations in early-onset familial Alzheimer's disease.

Author

Sherrington R, Rogaev EI, Liang Y, Rogaeva EA, Levesque G, Ikeda M, Chi H, Lin C, Li G, Holman K, Tsuda T, Mar L, Foncin JF, Bruni AC, Montesi MP, Sorbi S, Rainero I, Pinessi L, Nee L, Chumakov I, Pollen D, Brookes A, Sanseau P, Polinsky RJ, Wasco W, Da Silva HA, Haines JL, Perkicak-Vance MA, Tanzi RE, Roses AD, Fraser PE, Rommens JM, and St George-Hyslop PH

Subjects
Amino Acid Sequence, Animals, Base Sequence, Chromosome Mapping, Female, Humans, Male, Membrane Proteins chemistry, Mice, Molecular Sequence Data, Open Reading Frames, Pedigree, Presenilin-1, Protein Structure, Secondary, Transcription, Genetic, Alzheimer Disease genetics, Chromosomes, Human, Pair 14, Cloning, Molecular, Membrane Proteins genetics, Mutation
Abstract

Some cases of Alzheimer's disease are inherited as an autosomal dominant trait. Genetic linkage studies have mapped a locus (AD3) associated with susceptibility to a very aggressive form of Alzheimer's disease to chromosome 14q24.3. We have defined a minimal cosegregating region containing the AD3 gene, and isolated at least 19 different transcripts encoded within this region. One of these transcripts (S182) corresponds to a novel gene whose product is predicted to contain multiple transmembrane domains and resembles an integral membrane protein. Five different missense mutations have been found that cosegregate with early-onset familial Alzheimer's disease. Because these changes occurred in conserved domains of this gene, and are not present in normal controls, they are likely to be causative of AD3.

Published
1995
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35. [Direct detection of loci with pathologic trinucleotide repeats in diseases with anticipation].

Author

Rogaev EI, Rogaeva EA, and Dzhordzh-Khislop P

Subjects
Alleles, Humans, Molecular Weight, Nucleic Acid Hybridization, Repetitive Sequences, Nucleic Acid, Chromosome Mapping methods, Genome, Human, Oligonucleotides genetics
Abstract

We describe a simple method for the identification of pathologically expanded (CCG)n and (CTG)n three nucleotides repeat arrays in the human genome and for the recovery of flanking sequences. We were able to detect the presence of novel high-molecular-weight alleles in at least two of three subjects known to have expanded (CCG)n tracts at the FRAXA locus. The above method may be used for testing of small families or even single affected individuals with disease thought to display clinical evidence of anticipation. The (CCG)n > 200 and (CTG)n > 250 probes may also be useful for individual "DNA fingerprint" identifications.

Published
1995

36. Homozygous inheritance of the Machado-Joseph disease gene.

Author

Lang AE, Rogaeva EA, Tsuda T, Hutterer J, and St George-Hyslop P

Subjects
Adult, Aged, Chromosome Mapping, Female, Genes, Dominant, Genetic Linkage, Genotype, Homozygote, Humans, Male, Middle Aged, Machado-Joseph Disease genetics
Abstract

We report a patient presenting at age 16 years with postural instability and falls who developed severe generalized dystonia by the age of 20 years. He was the product of a consanguineous marriage. Maternal grandfather and paternal grandmother (brother and sister) living in the Azores were both affected by Machado-Joseph disease (MJD) beginning late in life. To date neither of the patient's parents are clinically affected. Linkage studies in this family and others of Azorean descent have confirmed the recent mapping of the MJD gene to chromosome 14q. Genotyping of the members of this pedigree provides strong genetic evidence that our patient is homozygous for the MJD gene. Our results combined with experience in 2 putative homozygotes previously reported in the literature suggest that gene dosage is an important determinant of age of onset and clinical phenotype in MJD. Other possible influencing factors are discussed.

Published
1994
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37. The upstream promoter of the beta-amyloid precursor protein gene (APP) shows differential patterns of methylation in human brain.

Author

Rogaev EI, Lukiw WJ, Lavrushina O, Rogaeva EA, and St George-Hyslop PH

Subjects
5-Methylcytosine, Animals, Cytosine analysis, DNA-Binding Proteins metabolism, Deoxyribonuclease HpaII, Deoxyribonucleases, Type II Site-Specific, Gene Expression Regulation, Humans, Mammals genetics, Methylation, Organ Specificity, Polymorphism, Restriction Fragment Length, Primates genetics, Sequence Homology, Nucleic Acid, Species Specificity, Amyloid beta-Protein Precursor genetics, Brain Chemistry, Cytosine analogs & derivatives, Genes, Promoter Regions, Genetic
Abstract

The human beta-amyloid protein precursor (beta-APP) gene (symbol APP) shows variable levels of expression in different human tissues, including brain. Because at least a moderate level of beta-APP expression is probably a necessary, although not sufficient, condition for diseases associated with pathologic deposition of beta-APP proteolytic products (such as the A beta peptide), we sought to identify factors in the 5' promoter of the human APP gene that may regulate tissue-specific expression of the APP gene. We report that sequences upstream from -500 bp in the APP promoter display complex, tissue-specific patterns of methylation. Furthermore, different patterns of methylation were observed even in DNA from different regions of brain. These differentially methylated sequences are able to bind nuclear proteins expressed in brain and HeLa cells and are also methylated in neocortex of nonhuman primates. Because these methylation patterns crudely reflect differences in APP expression, they may represent one mechanism for the tissue-specific regulation of APP expression.

Published
1994
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38. Are the associations between Alzheimer's disease and polymorphisms in the apolipoprotein E and the apolipoprotein CII genes due to linkage disequilibrium?

Author

Tsuda T, Lopez R, Rogaeva EA, Freedman M, Rogaev E, Drachman D, Pollen D, Haines J, Liang Y, and McLachlan DR

Subjects
Aged, Alleles, Apolipoprotein C-II, Female, Gene Frequency, Humans, Jews genetics, Male, Alzheimer Disease genetics, Apolipoproteins C genetics, Apolipoproteins E genetics, Linkage Disequilibrium, Polymorphism, Genetic
Abstract

Allele frequencies for polymorphisms in the apolipoprotein E and the apolipoprotein CII genes were determined in subjects of Ashkenazi Jewish origin with late-onset Alzheimer's disease and in unaffected control subjects from the same ethnic group. A significant association was observed between late-onset Alzheimer's disease and the epsilon 4 (112Cys-->Arg) allele of apolipoprotein E; however, no association was detected with apolipoprotein CII. These results suggest that the association with epsilon 4 is probably not due to linkage disequilibrium.

Published
1994
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39. [Mapping the gene for palmoplantar hyperkeratosis (thylosis) to chromosome 17 in the 17q12-q24 region].

Author

Rogaev EI, Rogaeva EA, Ginter EK, Korovaĭtseva GI, Farrer L, Shlenskiĭ AB, Prytkov AN, St George-Hyslop P, and Mordovtsev VN

Subjects
Chromosome Mapping, Genetic Linkage, Genetic Markers, Humans, Keratins genetics, Recombination, Genetic, Chromosomes, Human, Pair 17, Genes, Dominant, Keratoderma, Palmoplantar genetics
Abstract

Mapping of the genetic defect causing dominant palmoplantaris hyperkeratosis (PPHK) was continued based on the material of an extended Uzbek pedigree. No linkage between the PPHK gene and hypervariable DNA markers from 8p, 12p, 14q, and 22q were revealed. The study of PPHK gene linkage with DNA markers covering the entire length of 17th chromosome mapped the PPHK gene to 17q12-q24 and revealed close linkage with KRT10 and D17S800 loci (zero recombination frequency at a lod score > 7). The possible location of a PPHK mutation in one of the keratin genes mapped to the same region on the 17th chromosome is discussed.

Published
1994

40. Analysis of the c-FOS gene on chromosome 14 and the promoter of the amyloid precursor protein gene in familial Alzheimer's disease.

Author

Rogaev EI, Lukiw WJ, Vaula G, Haines JL, Rogaeva EA, Tsuda T, Alexandrova N, Liang Y, Mortilla M, Amaducci L, Bergamini L, Bruni AC, Foncin JF, Macciardi F, Montesi M, Sorbi S, Rainero I, Pinessi L, Polinsky RJ, Frommelt P, Duara R, Lopez R, Pollen D, Gusella JF, Tanzi R, MacLachlan D, Crapper D, and St George-Hyslop PH

Subjects
Adult, Genetic Linkage, Humans, Middle Aged, Pedigree, Polymorphism, Genetic, Restriction Mapping, Alzheimer Disease genetics, Amyloid beta-Protein Precursor genetics, Chromosomes, Human, Pair 14, Genes, fos genetics, Promoter Regions, Genetic genetics
Abstract

The c-FOS gene product, a putative transacting transcriptional regulator of the amyloid precursor protein (APP) gene, is a candidate locus for the familial Alzheimer's disease (FAD) mutation on chromosome 14 (FAD14). In light of this functional relationship, we investigated the nucleotide sequence and segregation of c-FOS and the nucleotide sequence of the 5' APP promoter. Single-stranded conformational polymorphisms (SSCPs) in the c-FOS gene revealed that c-FOS closely cosegregates with the FAD14 gene but does not show allelic association with FAD. A conservative third-position T-->C mutation was demonstrated in exon 2 (codon 84) of c-FOS, and a C-->G substitution was detected at -209 bp in the 5' promoter of APP. Neither were unique to FAD and are unlikely to be pathogenic or secondary modifiers of the FAD phenotype. We conclude that the c-FOS open reading frame is probably not the site of the FAD14 locus, but we cannot exclude the existence of modifier loci on chromosome 21.

Published
1993
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41. Identification of the genetic locus for keratosis palmaris et plantaris on chromosome 17 near the RARA and keratin type I genes.

Author

Rogaev EI, Rogaeva EA, Ginter EK, Korovaitseva GI, Farrer LA, Shlensky AB, Pritkov AN, Mordovtsev VN, and St George-Hyslop PH

Subjects
Base Sequence, Chromosome Mapping, DNA, DNA Mutational Analysis, Female, Genotype, Homozygote, Humans, Male, Molecular Sequence Data, Pedigree, Phenotype, Retinoic Acid Receptor alpha, Chromosomes, Human, Pair 17, Keratins genetics, Keratoderma, Palmoplantar genetics, Receptors, Retinoic Acid genetics
Abstract

Familial keratosis palmaris et plantaris (KPPF) is characterized by extreme keratinization and desquamation of the skin of the palmar and plantar surfaces of the hands and feet. We have mapped the causative genetic defect to an 8 cM interval on 17q12-24 in or close to the acidic keratin (type I) gene cluster. We show that KPPF co-segregates with a rare, high molecular weight allele of an insertion-deletion polymorphism in the C-terminal coding region of the keratin 10 gene (Z = 8.36 at theta = 0.00) and segrates as a true autosomal dominant trait. Some pedigrees with familial hyperkeratosis of the palms and soles have co-inherited diseases such as congenital malformations and familial cancers. Our analysis provide a region which should be investigated for contiguous gene syndromes in such pedigrees.

Published
1993
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42. [Obtaining monoclonal antibodies to paired tangled filaments from the brain of patients with Alzheimer's disease].

Author

Chumakova MM, Vostrikov VM, Dergunova NN, and Rogaeva EA

Subjects
Alzheimer Disease immunology, Animals, Antibodies, Monoclonal immunology, Cerebral Cortex immunology, Humans, Hybridomas immunology, Immunization, Immunoglobulin G immunology, Lymphocytes immunology, Mice, Mice, Inbred BALB C, Multiple Myeloma pathology, Spleen cytology, Alzheimer Disease pathology, Antibodies, Monoclonal biosynthesis, Cerebral Cortex ultrastructure, Immunoglobulin G biosynthesis, Neurofibrillary Tangles immunology
Abstract

Hybridoma technique was used to obtain a clone producing IgG antibodies. Paired helical neurofilaments isolated from the brain of patients suffering from Alzheimer's disease were used as an antigen during preparation of the clone. Antibodies recognize neurons with neurofibrillary changes. Specificity of the obtained antibodies to paired helical filaments was proved immunohistochemically. Monoclonal antibodies obtained are likely to be useful in the determination of the role played by pathological proteins in mutually twisted filaments formation.

Published
1991

43. [Anti-somatostatin autoantibodies in the blood serum of patients with schizophrenia].

Author

Rogaeva EA, Chumakova MM, Dergunova NN, Pozharitskaia DA, Kopeĭko GI, Tsutsul'kovskaia MIa, and Tsibezov VV

Subjects
Adolescent, Adult, Autoimmune Diseases etiology, Chronic Disease, Humans, Schizophrenia etiology, Schizophrenia, Paranoid etiology, Schizophrenia, Paranoid immunology, Autoantibodies analysis, Autoimmune Diseases immunology, Schizophrenia immunology, Somatostatin immunology
Abstract

Solid-phase IEA was used to measure the level of autoantibodies to somatostatin in the blood serum of 44 schizophrenics and 24 healthy donors. The patients suffering from schizophrenia manifested a higher (p less than 0.01) level of immune responsiveness of the blood serum to somatostatin (0.665 +/- 0.03) as compared to the control group (0.509 +/- 0.05). The main contribution to the differences between the groups as regards the parameter measured is made by patients with malignant (0.810 +/- 0.10) and paranoid (0.773 +/- 0.08) schizophrenia whereas the patients' subgroup with slow-progressive schizophrenia did not differ from normal regarding the level of autoantibodies to somatostatin in the serum (0.504 +/- 0.03). These tentative data agree with a hypothesis of the involvement of autoimmune processes into the development of schizophrenia.

Published
1990

44. A biochemical approach to essential hypertension.

Author

Rogaeva EA, Boldyrev AA, Lopina OD, Rubtsov AM, Perova NV, Zhigareva NN, and Oganov RG

Subjects
Adolescent, Adult, Humans, Hypertension blood, Middle Aged, Molecular Weight, Probability, Blood Proteins analysis, Hypertension diagnosis, Sodium-Potassium-Exchanging ATPase antagonists & inhibitors
Abstract

Using multivariate statistical analysis, an attempt has been made to select hypertensive and normotensive sub-groups of subjects on the basis of certain parameters of their blood serum, such as the inhibition of purified Na,K-ATPase by serum and the content of two proteins with molecular masses of 12 and 15 kDa. An analysis of 20 human beings (10 hypertensive and 10 normotensive individuals) revealed that the best division into sub-groups is achieved only through the use of a combination of these three parameters.

Published
1989

45. [Endogenous Na, K-ATPase inhibitors and biochemical markers of hypertension].

Author

Boldyrev AA and Rogaeva EA

Subjects
Animals, Biological Transport, Blood Cells enzymology, Blood Pressure, Blood Proteins metabolism, Cell Membrane Permeability, Humans, Hypertension diagnosis, Hypertension etiology, Ion Channels drug effects, Ion Channels metabolism, Kidney enzymology, Kidney physiopathology, Potassium metabolism, Rats, Rats, Inbred SHR, Sodium metabolism, Sodium-Potassium-Exchanging ATPase metabolism, Stress, Physiological physiopathology, Hypertension metabolism, Sodium-Potassium-Exchanging ATPase antagonists & inhibitors
Abstract

Molecular mechanisms of disturbances in the system responsible for ion transport taking place in the development of the initial hypertension in linear animals have been analysed in this review. On the basis of own and literary data the diagnostic significance of the biochemical parameters which characterize the membrane ion transport state at given disease is estimated. Using the results of correlation analysis of facts which characterize the connection between the human hypertension and specific blood factors, a probability of hypertension development depending on the degree of the given factors expression is determined.

Published
1985

46. [Is there a relation between the presence in the serum of patients with arterial hypertension of a protein component with molecular weight of 15 kD and the inhibitory effect of the serum on Na,K-ATPase?].

Author

Rogaeva EA, Perova NV, Aleksandrov AA, Oganov RG, and Lopina OD

Subjects
Adult, Cardenolides, Female, Humans, Male, Middle Aged, Molecular Weight, Sodium-Potassium-Exchanging ATPase blood, Blood Proteins isolation & purification, Digoxin, Hypertension blood, Saponins, Sodium-Potassium-Exchanging ATPase antagonists & inhibitors
Abstract

Blood sera from patients with arterial hypertension exhibited more distinct inhibitory effect on purified Na+,K+-ATPase as compared with blood sera of healthy persons. Moreover, the fraction of 12-15 kDa protein components was usually increased in blood sera of the patients. At the same time, strong inhibition of the enzyme occurred after addition of blood sera which did not contain the protein fraction. The data obtained suggest that both these patterns--the degree of blood sera inhibitory effect on Na+,K+-ATPase activity and content of 12-15 kDa protein components in blood serum--should be considered as diagnostically valuable at early steps of development of hypertension.

Published
1987

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