Your search keyword '"J S Stiffler"' showing total 8 results

1. Sequence variations in CREB1 cosegregate with depressive disorders in women

Author

Mary L. Marazita, Wendy N. Zubenko, J S Stiffler, Brion S. Maher, George S. Zubenko, A Brechbiel, and Hugh B. Hughes

Subjects

Male, Genetic Linkage, behavioral disciplines and activities, Pathogenesis, Cellular and Molecular Neuroscience, Sex Factors, Genetic linkage, mental disorders, Cyclic AMP, medicine, Humans, Genetic Predisposition to Disease, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Depression (differential diagnoses), Sequence (medicine), Genetics, Depressive Disorder, Major, biology, Intron, medicine.disease, Introns, Pedigree, Psychiatry and Mental health, Mood disorders, biology.protein, Major depressive disorder, Female, Psychology, CREB1, Signal Transduction, Transcription Factors

Abstract

Major depressive disorder (MDD) constitutes a major public health problem worldwide and affects women twice as frequently as men. Previous linkage studies have identified a 451 kb region of 2q33-35 that exhibited significant evidence of linkage to Mood Disorders among women (but not men) from families with recurrent, early-onset MDD (RE-MDD), a severe and strongly familial subtype of MDD. This 451 kb region includes CREB1, an attractive susceptibility gene for MDD and related disorders. Sequence variations in the CREB1 promoter and intron 8 have been detected that cosegregate with Mood Disorders, or their absence, in women from these families, identifying CREB1 as a sex-limited susceptibility gene for unipolar Mood Disorders. These findings implicate the cAMP signaling pathway in the pathophysiology of Mood Disorders and related conditions.

Published

2003

2. D2S2944 identifies a likely susceptibility locus for recurrent, early-onset, major depression in women

Author

Barry B. Kaplan, Wendy N. Zubenko, J S Stiffler, George S. Zubenko, and Hugh B. Hughes

Subjects

Adult, Genetic Markers, Male, Proband, Candidate gene, Genotype, Physiology, behavioral disciplines and activities, White People, Genetic determinism, Cellular and Molecular Neuroscience, Recurrence, mental disorders, Ethnicity, medicine, Humans, Genetic Predisposition to Disease, Age of Onset, Family history, Allele, Molecular Biology, Alleles, Genetics, Depressive Disorder, Sex Characteristics, Odds ratio, medicine.disease, Psychiatry and Mental health, Major depressive disorder, Female, Age of onset, Psychology

Abstract

Recurrent, early-onset, major depressive disorder (RE-MDD) is a strongly familial condition whose malignant effects have a significant negative impact on the health and longevity of patients and their family members. Sixteen of the 19 candidate susceptibility loci identified by a recent genome survey revealed allelic associations with RE-MDD in men or women, but not in both sexes. The association of D2S2944 alleles and genotypes with RE-MDD and related disorders was evaluated using a case-control study design employing 100 adults with RE-MDD and 100 adult controls who had no personal or family history of mental disorders. The results of the case-control study were subsequently evaluated in a sample of 81 families ascertained through probands with RE-MDD using the transmission/disequilibrium test. The frequency of the D2S2944 124-bp allele among women with RE-MDD was approximately three times that for female controls (P = 0.0003). Women who carried the D2S2944 124-bp allele revealed a significantly elevated risk of developing RE-MDD, as indicated by an odds ratio of 4.5 compared to female controls (P

Published

2002

3. Clinical and neurobiological correlates of DXS1047 genotype in Alzheimer’s disease

Author

G S, Zubenko, H B, Hughes, and J S, Stiffler

Subjects

Male, Polymorphism, Genetic, X Chromosome, Genotype, Brain, Alzheimer Disease, Culture Techniques, Humans, Female, Genetic Predisposition to Disease, Longitudinal Studies, Alleles, Biological Psychiatry, Aged, Microsatellite Repeats

Abstract

The goal of the current study was to explore the clinical, neuropathological, and neurochemical correlates of the DXS1047 202 bp allele in a group of 50 autopsy-confirmed cases of Alzheimer's disease (AD) who lacked other concomitant brain diseases. We previously published the results of a genome survey for novel risk loci for typical-onset (or = 60 years) AD conducted at 10 cM resolution (Zubenko et al 1998a, b). This survey detected associations of alleles at six microsatellite loci with AD, including the 202 bp allele of the DXS1047 locus that resides within Xq25 on the human cytogenetic map.Clinical assessments were performed as part of a longitudinal study of AD and related disorders. Autopsies were performed using standardized methods and the resulting diagnoses were made according to established criteria. Genotyping, morphometry, and neurochemical analyses were performed using postmortem brain tissue.Patients with AD who carried the DXS1047 202 bp allele manifested cortical norepinephrine levels that ranged from 2.1 to 3.6 times the corresponding values for noncarriers (p = .002), controlling for the potential effects of gender, age at symptomatic onset or death, and postmortem interval. In contrast, carriers tended to have lower cortical levels of dopamine (p = .10).These findings support the results of our previous genome survey and suggest that the DXS1047 locus, or a locus in close proximity, modulates biological variables relevant to the pathophysiology of AD. In addition to providing insights into the clinical biology of AD, the characterization of biologically meaningful subtypes, including genotypic subtypes associated with particular neurobiological derangements, may be important to the advancement of experimental therapeutics in AD.

Published

1999

4. D10S1423 identifies a susceptibility locus for Alzheimer's disease in a prospective, longitudinal, double-blind study of asymptomatic individuals

Author

J S Stiffler, Hugh B. Hughes, and George S. Zubenko

Subjects

Apolipoprotein E, Adult, Genetic Markers, Male, medicine.medical_specialty, Pathology, Genotype, Disease, Asymptomatic, Central nervous system disease, Cohort Studies, Cellular and Molecular Neuroscience, Degenerative disease, Apolipoproteins E, Double-Blind Method, Alzheimer Disease, Risk Factors, Internal medicine, medicine, Humans, Family, Genetic Predisposition to Disease, Longitudinal Studies, Prospective Studies, Risk factor, Allele, Molecular Biology, Aged, Proportional Hazards Models, business.industry, Middle Aged, medicine.disease, Psychiatry and Mental health, Female, Alzheimer's disease, medicine.symptom, business, Mental Status Schedule

Abstract

Typical, later-onset forms of Alzheimer's disease (AD) appear to be influenced by multiple susceptibility loci, combinations of which contribute to the development of this disorder. We previously reported the results of a systematic survey of the human genome for the identification of highly informative DNA polymorphisms (SSTRPs) that target new AD risk genes. In addition to the APOE locus, our survey detected five new candidate susceptibility loci for AD, including D10S1423. An association of the D10S1423 234-bp allele with AD has been reported in three independent samples of AD cases and controls (Boston, Pittsburgh, Bonn). Data from our case-control studies suggest a strong synergistic interaction between the D10S1423 234-bp and APOE E4 risk alleles (234-bp carrier: OR = 2.5, 95% CI = 1.4--4.5; E4 carrier: OR = 8.3, 95% CI = 4.3--15.8; both alleles: OR = 23.1, 95% CI = 5.3--99.5). This report describes the prospective, longitudinal, double-blind assessment of the age-specific risk of AD encountered by 325 asymptomatic first-degree relatives of AD probands who carried the D10S1423 234-bp allele, the APOE E4 allele, or both, after 11.5 years of systematic follow-up. A total of 18 incident cases of AD were detected during the first 3379 subject-years of this longitudinal study. The effects of carrying either or both of the D10S1423 234-bp and APOE E4 alleles on the age-specific risk of developing AD were determined using Kaplan-Meier survival analysis. The age-specific risk of developing AD was the greatest for individuals who carried both alleles (Mantel--Cox statistic = 20.12, df = 3, P = 0.0002; Breslow statistic = 13.36, df = 3, P = 0.004). Cox proportional hazards models were developed to estimate the risk ratios for each genotype, controlling for the potential effects of age at recruitment, sex, and years of education. In the resulting best fitting model, only individuals who carried both risk alleles exhibited a risk ratio that differed significantly from 1 (risk ratio = 16.2, P = 0.008, 95% CI = 2.1--128.3). After controlling for these genotypes, female gender was also significantly associated with increased risk of developing AD (risk ratio = 5.1, P = 0.02, 95% CI = 1.2--21.1). Neither age at recruitment nor years of education made significant contributions to the model.

Published

2000

5. A genome survey for novel Alzheimer disease risk loci: results at 10-cM resolution

Author

J S Stiffler, Hugh B. Hughes, Barry B. Kaplan, Mark R. Hurtt, and George S. Zubenko

Subjects

Male, Linkage disequilibrium, Genotype, Minisatellite Repeat, Apolipoprotein E4, Minisatellite Repeats, Biology, Polymerase Chain Reaction, Linkage Disequilibrium, Apolipoproteins E, Gene Frequency, Polymorphism (computer science), Alzheimer Disease, Genetics, Humans, Genetic Predisposition to Disease, Allele, Age of Onset, Allele frequency, Genotyping, Alleles, Aged, Repetitive Sequences, Nucleic Acid, Aged, 80 and over, Polymorphism, Genetic, Middle Aged, Case-Control Studies, Microsatellite, Female

Abstract

We completed a systematic survey of the human genome, conducted at an average resolution of 10 cM, for the identification of simple sequence tandem repeat polymorphisms (SSTRPs) that target new risk genes for Alzheimer disease (AD) by virtue of linkage disequilibrium. The efficiency of our association study was enhanced by genotyping pools of DNA from autopsy-confirmed cases with AD and matched controls. Allelic associations with AD were observed for 6 of the 391 SSTRPs in the CHLC Human Screening Set/Weber Version 6 (Research Genetics, Inc., Huntsville, AL): D1S518, D1S547, D10S1423, D12S1045, D19S178, and DXS1047. These allelic associations were replicated in an independent sample of autopsied AD cases and controls recruited from a geographically disparate site. The association of the large D19S178 alleles with AD appeared to arise from linkage disequilibrium with the APOE epsilon 4 allele, whose effect on increasing the risk of AD has been established. None of the remaining SSTRPs was in close proximity to loci previously reported to influence the risk of developing AD. Instead, they may identify five novel AD susceptibility loci.

Published

1998

6. Initial results of a genome survey for novel Alzheimer's disease risk genes: association with a locus on the X chromosome

Author

G S, Zubenko, J S, Stiffler, H B, Hughes, M R, Hurtt, and B B, Kaplan

Subjects

Adult, Aged, 80 and over, Male, Polymorphism, Genetic, X Chromosome, Genotype, Middle Aged, Apolipoproteins E, Gene Frequency, Alzheimer Disease, Case-Control Studies, Humans, Female, Genetic Predisposition to Disease, Autopsy, Genetic Testing, Age of Onset, Alleles, Aged, Repetitive Sequences, Nucleic Acid

Abstract

As the initial step in a systematic genome survey, 16 simple sequence tandem repeat polymorphisms that span the X chromosome at an average spacing of 10 cM were examined for allelic associations with typical-onset Alzheimer's disease (AD). The efficiency of this survey was substantially enhanced by genotyping pools of genomic DNA from 50 autopsy-confirmed AD cases and 50 autopsied controls who were similar in sex ratio, race, and age at death. The frequency of the DXS1047 202-bp allele was twice as common among AD cases (0.45 +/- S.E. 0.06) than controls (0.22 +/- S.E. 0.05), a finding that was reproduced in an independent and geographically disparate sample. Consistent with Hardy-Weinberg equilibrium, the proportion of women with AD who carried the 202-bp allele, 73% was nearly double that observed for men with AD, 38%. However, the frequency of the 202-bp allele was similar for men and women and the presence of this allele did not affect the age at onset of dementia in either sex. Furthermore, the frequency of the DXS1047 202-bp allele in AD cases and controls was unaffected by the APOE genotype, indicating that these two loci modulate AD risk independently. Finally, the frequency of the 202-bp allele among 50 autopsy-confirmed cases of Parkinson's disease (0.29 +/- S.E. 0.06) was indistinguishable from the control value, reflecting relative specificity for this allelic association with AD.

Published

1998

7. Clinically-silent mutation in the putative iron-responsive element in exon 17 of the beta-amyloid precursor protein gene

Author

J S Stiffler, Hugh B. Hughes, George S. Zubenko, Joan E. Farr, and Barry B. Kaplan

Subjects

Silent mutation, Molecular Sequence Data, Biology, medicine.disease_cause, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, Exon, Amyloid beta-Protein Precursor, Alzheimer Disease, Genes, Regulator, medicine, Missense mutation, Humans, Genetics, Mutation, Base Sequence, Point mutation, Iron-Regulatory Proteins, RNA-Binding Proteins, General Medicine, Exons, Genetic code, Neurology, Point accepted mutation, Neurology (clinical), Synonymous substitution, Oligonucleotide Probes

Abstract

Three missense mutations in exon 17 of the beta-amyloid precursor protein (APP) gene have been reported to cosegregate in families with early onset Alzheimer's disease (AD). All three mutations result in amino acid substitutions at codon 717 and may produce AD by altering the structure of the transmembrane domain of APP. Alternatively, the mutations may destabilize the stem of a putative iron-responsive element (IRE) in which they lie and confer pathogenicity by inactivating this negative regulatory element. We have detected a clinically-silent mutation in codon 716 that would also be expected to disrupt the putative IRE but results in no amino acid substitution. This result strongly suggests that the missense mutations at codon 717 produce AD by altering the amino acid sequence of APP rather than the IRE. Furthermore, the identification of a clinically-silent mutation among four point mutations that span only three nucleotides of exon 17 suggests that this region may be a mutational "hot" spot.

Published

1992

8. 296. Identification and characteristics of six risk loci for Alzheimer's disease

Author

A.J. Martinez, Hugh B. Hughes, J S Stiffler, Mark R. Hurtt, Barry B. Kaplan, George S. Zubenko, and Ursula Kopp

Subjects

Genetics, Identification (biology), Disease, Biology, Biological Psychiatry

Published

1998