Inactivation of the Fas gene by Alu insertion: retrotransposition in an intron causing splicing variation and autoimmune lymphoproliferative syndrome

Inactivation of the Fas gene by Alu insertion: retrotransposition in an intron causing splicing variation and autoimmune lymphoproliferative syndrome

Mutations in the Fas (apo-1, CD95) gene result in autoimmune lymphoproliferative syndrome (ALPS). These mutations are dominated by small deletions and point mutations that result in splicing errors or missense changes. We report here a novel mutation caused by retrotransposon insertion, which result...

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Bibliographic Details
Published in:Genes and immunity Vol. 3; no. S1; pp. S66 - S70
Main Authors: Tighe, P J, Stevens, S E, Dempsey, S, Le Deist, F, Rieux-Laucat, F, Edgar, J D M
Format: Journal Article
Language:English
Published: England Nature Publishing Group 01-10-2002
Subjects:
Alu Elements - genetics
Alu Elements - physiology
Apoptosis
Apoptosis - genetics
Apoptosis - immunology
Autoimmunity - genetics
Autoimmunity - immunology
Base Sequence
CD95 antigen
Disease
Exons
Fas antigen
fas Receptor - genetics
fas Receptor - physiology
Gene Silencing
Genes
Genomic analysis
Homeostasis
Homology
Humans
Immunology
Infant
Introns
Lymphadenopathy
Lymphocytes
Lymphoproliferative Disorders - genetics
Lymphoproliferative Disorders - immunology
Male
Molecular Sequence Data
mRNA
Mutation
Polymerase chain reaction
Proteins
Retrotransposition
Reverse Transcriptase Polymerase Chain Reaction
RNA, Messenger
Signal transduction
United Kingdom > UK
Northern Ireland
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Description
Summary:Mutations in the Fas (apo-1, CD95) gene result in autoimmune lymphoproliferative syndrome (ALPS). These mutations are dominated by small deletions and point mutations that result in splicing errors or missense changes. We report here a novel mutation caused by retrotransposon insertion, which results in loss of exon 8 and ALPS. A father and son suffering from recurrent lymphadenopathy were examined for resistance to Fas-mediated apoptosis. A functional defect was detected and RT-PCR analysis revealed two different copies of Fas mRNA, one normal and a second shorter version lacking exon 8. DNA analysis of the genomic region between exons seven and nine in the longer copy revealed two PCR products, one being 331 base pairs (bp) longer than expected. Sequencing revealed that intron 7 had undergone an insertion event with an Alu element (99.31% homology with Alu-Sb1) of 331 bp. This element included a 34-bp Poly A tract that was flanked on each side by a perfect 17 bp direct duplication of the target site. Both patients were heterozygous for the mutated allele that produced Fas mRNA lacking exon 8, although not due to loss of a splice junction. The structure of the insertion suggests that the Alu element may have integrated by retrotransposition, and represents the first report of a retrotransposon causing ALPS.
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ISSN:1466-4879
1476-5470
DOI:10.1038/sj.gene.6363864