Your search keyword '"Pearson, Peter L."' showing total 3 results

1. A novel locus for split-hand/foot malformation associated with tibial hemimelia (SHFLD syndrome) maps to chromosome region 17p13.1–17p13.3.

Author

Lezirovitz, Karina, Maestrelli, Sylvia Regina Pedrosa, Cotrim, Nelson Henderson, Otto, Paulo A., Pearson, Peter L., and Mingroni-Netto, Regina Celia

Subjects

HUMAN abnormalities, HAND abnormalities, FOOT abnormalities, GENES, PHENOTYPES, GENETIC mutation

Abstract

Split-hand/foot malformation (SHFM) associated with aplasia of long bones, SHFLD syndrome or Tibial hemimelia-ectrodactyly syndrome is a rare condition with autosomal dominant inheritance, reduced penetrance and an incidence estimated to be about 1 in 1,000,000 liveborns. To date, three chromosomal regions have been reported as strong candidates for harboring SHFLD syndrome genes: 1q42.2–q43, 6q14.1 and 2q14.2. We characterized the phenotype of nine affected individuals from a large family with the aim of mapping the causative gene. Among the nine affected patients, four had only SHFM of the hands and no tibial defects, three had both defects and two had only unilateral tibial hemimelia. In keeping with previous publications of this and other families, there was clear evidence of both variable expression and incomplete penetrance, the latter bearing hallmarks of anticipation. Segregation analysis and multipoint Lod scores calculations (maximum Lod score of 5.03 using the LINKMAP software) using all potentially informative family members, both affected and unaffected, identified the chromosomal region 17p13.1–17p13.3 as the best and only candidate for harboring a novel mutated gene responsible for the syndrome in this family. The candidate gene CRK located within this region was sequenced but no pathogenic mutation was detected. [ABSTRACT FROM AUTHOR]

Published

2008

2. Haplotype study in Dutch SCA3 and SCA6 families: evidence for common founder mutations.

Author

Verbeek, Dineke S., Piersma, Systse J., Hennekam, Eric FAM, Ippel, Elly F., Pearson, Peter L., and Sinke, Richard J.

Subjects

ATAXIA, NEURODEGENERATION, GENETIC mutation, HUMAN genetics, HUMAN biology, GENETICS

Abstract

This pilot study was initiated to show the existence of founder effects in the Dutch autosomal dominant cerebellar ataxia (ADCA) population. The ADCAs comprise a clinically heterogeneous group of neurodegenerative disorders and the estimated prevalence in the Netherlands is approximately 3:100?000 individuals. Here, we focused on the SCA3 and SCA6 genes because mutations in these genes occur most frequently in the Netherlands. We were able to determine a common origin of the CAG repeat expansions in the majority of Dutch SCA3 and SCA6 families. Haplotype analysis and linkage disequilibrium studies with polymorphic markers revealed shared haplotypes surrounding the SCA3 and SCA6 genes. These results strongly suggest that ADCA families can be traced back to common ancestors in particular parts of the Netherlands.European Journal of Human Genetics (2004) 12, 441-446. doi:10.1038/sj.ejhg.5201167 Published online 17 March 2004 [ABSTRACT FROM AUTHOR]

Published

2004

3. Identification of a novel SCA locus (SCA19) in a Dutch autosomal dominant cerebellar ataxia family on chromosome region 1p21-q21.

Author

Verbeek, Dineke S., Schelhaas, Jurgen H., Ippel, Elly F., Beemer, Frits A., Pearson, Peter L., and Sinke, Richard J.

Subjects

CEREBELLAR ataxia, ATAXIA, FAMILIAL diseases, CHROMOSOMES, GENETIC mutation, NEUROLOGY, NEUROGENETICS

Abstract

We present a linkage study in a four-generation autosomal dominant cerebellar ataxia (ADCA) family of Dutch ancestry. The family shows a clinically and genetically distinct form of ADCA. This neurodegenerative disorder manifests in the family as a relatively mild ataxia syndrome with some additional characteristic symptoms. We have identified a SCA19 locus, approved by the Human Genome Nomenclature Committee that can be assigned to the chromosome region 1p21-q21. Our mutation analysis failed to identify any mutations in the known spinocerebellar ataxia (SCA) genes and linkage analysis excluded the remaining SCA loci. We therefore performed a genome-wide scan with 350 microsatellite markers to identify the location of the disease-causing gene in this family. Multi-point analysis was performed and exclusion maps were generated. Linkage and haplotype analysis revealed linkage to an interval located on chromosome 1. The estimated minimal prevalence of ADCA in the Netherlands is about 3:100,000. To date, sixteen different SCA loci have been identified in ADCA (SCA1–8 and SCA10–17). However, mutation analysis has been commercially available only for the SCA1, 2, 3, 6 and 7 genes. So far, a molecular analysis in these SCA genes cannot be made in about one-third of the ADCA families. Thus, the identification of this new, additional SCA19 locus will contribute to expanding the DNA diagnostic possibilities. [ABSTRACT FROM AUTHOR]

Published

2002