Association of splicing defects in PTEN leading to exon skipping or partial intron retention in Cowden syndrome

Cowden syndrome (CS) and Bannayan Zonana syndrome (BZS) are two autosomal dominantly inherited conditions characterized by hamartomas. Mutations in PTEN, a tumor suppressor gene located on chromosome 10q23, have been identified in patients with phenotypic findings of both CS and BZS. These mutations...

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Published inHuman genetics Vol. 107; no. 3; pp. 234 - 238
Main Authors CELEBI, Julide Tok, WANNER, Molly, XIAO LI PING, HONG ZHANG, PEACOCKE, Monica
Format Journal Article
LanguageEnglish
Published Heidelberg Springer 01.09.2000
Berlin
New York, NY
Subjects
Biological and medical sciences
Child
Complex syndromes
Exons
Female
Genes, Tumor Suppressor
Germ-Line Mutation
Hamartoma Syndrome, Multiple - genetics
Humans
Introns
Male
Medical genetics
Medical sciences
Phosphoric Monoester Hydrolases - genetics
Point Mutation
PTEN Phosphohydrolase
RNA Splicing - genetics
Syndrome
Tumor Suppressor Proteins
Pseudotumor
Human
Skin disease
Splicing
Nucleotide sequence
Family study
Chromosome C10
Genetic disease
Hamartoma
Messenger RNA
Autosomal character
Benign neoplasm
Mutation
Tumor suppressor gene
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Summary:Cowden syndrome (CS) and Bannayan Zonana syndrome (BZS) are two autosomal dominantly inherited conditions characterized by hamartomas. Mutations in PTEN, a tumor suppressor gene located on chromosome 10q23, have been identified in patients with phenotypic findings of both CS and BZS. These mutations are found throughout the entire gene, with exon 5 being the most common site, and include point mutations, insertions and deletions. To date, 11 point mutations at the splice junctions of the PTEN gene have been reported, however, data on the alterations in the transcripts have been lacking. In this study, we have identified three novel splice site mutations in PTEN, in two families with CS and in one individual with BZS. One mutation affected the splice-acceptor site, which resulted in out-of-frame skipping of an entire exon. By contrast, the other two mutations affected the splice-donor sites, and both showed inclusion of partial intronic sequences in the transcript due to activation of cryptic splice sites. These data demonstrate mRNA alterations as a consequence of splice site mutations in the PTEN gene.
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ISSN:0340-6717
1432-1203
DOI:10.1007/s004390000362