Your search keyword '"Michael W. Pauciulo"' showing total 4 results

1. Parkin dosage mutations have greater pathogenicity in familial PD than simple sequence mutations

Author

Tatiana Foroud, Karen Marder, William C. Nichols, Alice Rudolph, Ronald F. Pfeiffer, Michael W. Pauciulo, Diane Kissell, Cheryl Halter, and Nathan Pankratz

Subjects

Adult, Genetic Markers, Male, Adolescent, Genotype, Ubiquitin-Protein Ligases, DNA Mutational Analysis, Gene Dosage, Biology, Parkin, Young Adult, Exon, Gene Frequency, Risk Factors, Humans, Point Mutation, Genetic Predisposition to Disease, Genetic Testing, Age of Onset, Allele, Aged, Aged, 80 and over, Genetics, Base Sequence, Point mutation, Parkinson Disease, Articles, Middle Aged, nervous system diseases, Haplotypes, Mutation, Mutation (genetic algorithm), Female, Neurology (clinical), Age of onset, Haploinsufficiency, Gene Deletion

Abstract

Objective: Mutations in both alleles of parkin have been shown to result in Parkinson disease (PD). However, it is unclear whether haploinsufficiency (presence of a mutation in only 1 of the 2 parkin alleles) increases the risk for PD. Methods: We performed comprehensive dosage and sequence analysis of all 12 exons of parkin in a sample of 520 independent patients with familial PD and 263 controls. We evaluated whether presence of a single parkin mutation, either a sequence (point mutation or small insertion/deletion) or dosage (whole exon deletion or duplication) mutation, was found at increased frequency in cases as compared with controls. We then compared the clinical characteristics of cases with 0, 1, or 2 parkin mutations. Results: We identified 55 independent patients with PD with at least 1 parkin mutation and 9 controls with a single sequence mutation. Cases and controls had a similar frequency of single sequence mutations (3.1% vs 3.4%, p = 0.83); however, the cases had a significantly higher rate of dosage mutations (2.6% vs 0%, p = 0.009). Cases with a single dosage mutation were more likely to have an earlier age at onset (50% with onset at ≤45 years) compared with those with no parkin mutations (10%, p = 0.00002); this was not true for cases with only a single sequence mutation (25% with onset at ≤45 years, p = 0.06). Conclusions: Parkin haploinsufficiency, specifically for a dosage mutation rather than a point mutation or small insertion/deletion, is a risk factor for familial PD and may be associated with earlier age at onset.

Published

2009

2. Variation in GIGYF2 is not associated with Parkinson disease

Author

Diane Kissell, Kristi A. Clark, Tatiana Foroud, Ronald F. Pfeiffer, V. E. Elsaesser, Alice Rudolph, William C. Nichols, Joanne Wojcieszek, Cheryl Halter, Michael W. Pauciulo, and Nathan Pankratz

Subjects

Male, Parkinson's disease, Genotype, Genetic Linkage, DNA Mutational Analysis, Disease, Biology, Polymorphism, Single Nucleotide, Open Reading Frames, Degenerative disease, Genetic linkage, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Aged, Genetic testing, Genetics, Linkage (software), Base Sequence, medicine.diagnostic_test, Chromosome Mapping, Genetic Variation, Parkinson Disease, Middle Aged, medicine.disease, Pedigree, Chromosomes, Human, Pair 2, Mutation, Chromosomal region, Female, Neurology (clinical), Carrier Proteins

Abstract

Objective: A recent study reported that mutations in a gene on chromosome 2q36-37, GIGYF2 , result in Parkinson disease (PD). We have previously reported linkage to this chromosomal region in a sample of multiplex PD families, with the strongest evidence of linkage obtained using the subset of the sample having the strongest family history of disease and meeting the strictest diagnostic criteria. We have tested whether mutations in GIGYF2 may account for the previously observed linkage finding. Methods: We sequenced the GIGYF2 coding region in 96 unrelated patients with PD used in our original study that contributed to the chromosome 2q36-37 linkage signal. Subsequently, we genotyped the entire sample of 566 multiplex PD kindreds as well as 1,447 controls to test whether variants in GIGYF2 are causative or increase susceptibility for PD. Results: We detected three novel variants as well as one of the previously reported seven variants in a total of five multiple PD families; however, there was no consistent evidence that these variants segregated with PD in these families. We also did not find a significant increase in risk for PD among those inheriting variants in GIGYF2 ( p = 0.28). Conclusions: We believe that variation in a gene other than GIGYF2 accounts for the previously reported linkage finding on chromosome 2q36-37. GDS = Geriatric Depression Scale; MMSE = Mini-Mental State Examination; NCRAD = National Cell Repository for Alzheimer’s Disease; PD = Parkinson disease; PSG = Parkinson Study Group; UPDRS = Unified Parkinson’s Disease Rating Scale.

Published

2009

3. LRRK2 mutation analysis in Parkinson disease families with evidence of linkage to PARK8

Author

William C. Nichols, Diane K. Marek, Michael W. Pauciulo, Tatiana Foroud, V. E. Elsaesser, Cheryl Halter, Alice Rudolph, Nathan Pankratz, and Clifford W. Shults

Subjects

Nonsynonymous substitution, Genetics, Locus (genetics), Biology, medicine.disease, LRRK2, nervous system diseases, Exon, Genetic linkage, Mutation testing, medicine, Neurology (clinical), Alzheimer's disease, Gene

Abstract

Background: Pathogenic mutations in the leucine-rich repeat kinase 2 gene ( LRRK2 ) have been found to cause typical, later-onset Parkinson disease (PD). Although G2019S is the most common mutation, other mutations have also been reported. It is critical to catalog the types of mutations found in LRRK2 that can cause PD, so as to provide insight regarding disease susceptibility and potential novel treatments. Methods: We performed a comprehensive study of all 51 exons of the LRRK2 gene in one PD patient from each of 88 multiplex PD families who had the highest family-specific multipoint lod score at the LRRK2 locus from a cohort of 430 PD families without the G2019S mutation. Results: Five families (5.7%) harbored what seem to be novel, pathogenic mutations (L1795F, I1192V, E10K, E334K, Q1111H). Three of these apparent mutations were in known, functional domains of the LRRK2 protein, where other studies have also identified disease producing mutations. However, two of the novel variants were found in the N-terminal region of LRRK2, where no pathogenic substitutions have yet been reported. Similar to previous studies, all subjects with an LRRK2 mutation had classic symptoms of PD and typical, later age at onset. Conclusions: We have identified five novel variants in LRRK2, with two of these in the N-terminal region of LRRK2, where no pathogenic substitutions have been previously reported. If confirmed to be causative, these mutations would broaden the potential mechanisms whereby mutations in LRRK2 result in Parkinson disease. GLOSSARY: AD = Alzheimer disease; cDNA = complementary DNA; COR = C terminal of Ras; Hisp = Hispanic; LRR = leucine-rich repeat; LRRK2 = leucine-rich repeat kinase 2 gene; MMSE = Mini-Mental State Examination; NS = nonsynonymous variant that is potentially disease producing; PD = Parkinson disease; Roc = Ras of complex; S = synonymous variant that is not likely to be pathogenic; UPDRS = Unified Parkinson’s Disease Rating Scale.

Published

2007

4. A mutation in myotilin causes spheroid body myopathy

Author

B. Azzarelli, Ruben Vidal, Hans-Hilmar Goebel, L. J. Cushman, Martin R. Farlow, Tatiana Foroud, Nathan Pankratz, H. Horak, Michael W. Pauciulo, Leticia Miravalle, William C. Nichols, and A. P. Batchman

Subjects

Adult, Genetic Markers, Male, Candidate gene, Pathology, medicine.medical_specialty, DNA Mutational Analysis, Muscle Proteins, Chromosome Disorders, Biology, Exon, Muscular Diseases, medicine, Humans, Point Mutation, Myotilin, Connectin, Genetic Predisposition to Disease, Genetic Testing, Muscular dystrophy, Muscle, Skeletal, Myopathy, Aged, Genes, Dominant, Aged, 80 and over, Inclusion Bodies, Genetics, Muscle biopsy, medicine.diagnostic_test, Microfilament Proteins, Chromosome Mapping, Exons, Middle Aged, medicine.disease, Pedigree, Cytoskeletal Proteins, Mutation, Chromosomal region, biology.protein, Chromosomes, Human, Pair 5, Female, Titin, Neurology (clinical), medicine.symptom

Abstract

Background: Spheroid body myopathy (SBM) is a rare, autosomal dominant, neuromuscular disorder, which has only been previously reported in a single large kindred. Identification of the mutated gene in this disorder may provide insight regarding abnormal neuromuscular function. Methods: The authors completed a detailed clinical evaluation on an extensive kindred diagnosed with SBM. Genome-wide linkage analysis was performed to localize the disease gene to a specific chromosomal region. Further marker genotyping and screening of a positional, functional candidate gene were completed to detect the disease-causing mutation. Pathologic analysis of muscle biopsy was performed on three individuals. Biochemical studies were performed on one muscle biopsy specimen from an affected individual. Results: Linkage to chromosome 5q23-5q31 was detected with a lod score of 2.9. Genotyping of additional markers in a larger sample of family members produced a maximum lod score of 6.1 and narrowed the critical interval to 12.2 cM. Screening of the candidate gene titin immunoglobulin domain protein ( TTID , also known as MYOT ) detected a cytosine-to-thymine mutation in exon 2 of all clinically affected family members. Similar pathologic changes were present in all muscle biopsy specimens. Immunohistologic and biochemical analysis revealed that the TTID protein, also known as myotilin, is a component of the insoluble protein aggregate. Conclusions: A novel mutation in the TTID gene results in the clinical and pathologic phenotype termed “spheroid body myopathy.” Mutations in this gene also cause limb-girdle muscular dystrophy 1A and are associated with myofibrillar myopathy.

Published

2005