A Splicing Defect Due to an Exon-intron Junctional Mutation Results in Abnormal Beta-hexosaminidase Alpha Chain MRNAs in Ashkenazi Jewish Patients with Tay-Sachs Disease

Overview

Journal Biochem Biophys Res Commun

Publisher Elsevier

Specialty Biochemistry

Date 1988 May 31

PMID 2837213

Citations 30

Authors

K Ohno

K Suzuki

Affiliations

Soon will be listed here.

Abstract

Abnormal beta-hexosaminidase alpha chain mRNAs from an Ashkenazi Jewish patient with the classical infantile Tay-Sachs disease contained intact or truncated intron 12 sequences. Sequence analysis showed a single nucleotide transversion at the 5' donor site of intron 12 from the normal G to C. This provides the first evidence that this junctional mutation, also found independently in two other laboratories by analysis of genomic clones, results in functional abnormality. Analysis with normal and mutant oligonucleotides as probes indicated that our patient was a compound heterozygote with only one allele having the transversion. The patient studied in the other two laboratories was also a compound heterozygote. Another Ashkenazi Jewish patient was normal in this region in both alleles. Thus, the splicing defect is the underlying genetic cause in some but not all Ashkenazi Jewish patients with Tay-Sachs disease.

Citing Articles

EHMT2 as a Candidate Gene for an Autosomal Recessive Neurodevelopmental Syndrome.

Carvalho L, Rzasa J, Kerkhof J, McConkey H, Fishman V, Koksharova G Mol Neurobiol. 2024; .

PMID: 39674972 DOI: 10.1007/s12035-024-04655-x.

Tay-Sachs disease: current perspectives from Australia.

Lew R, Burnett L, Proos A, Delatycki M Appl Clin Genet. 2015; 8:19-25.

PMID: 25653550 PMC: 4309774. DOI: 10.2147/TACG.S49628.

Tay-Sachs disease preconception screening in Australia: self-knowledge of being an Ashkenazi Jew predicts carrier state better than does ancestral origin, although there is an increased risk for c.1421 + 1G > C mutation in individuals with South....

Lew R, Burnett L, Proos A J Community Genet. 2011; 2(4):201-9.

PMID: 22109873 PMC: 3215783. DOI: 10.1007/s12687-011-0057-x.

Different attenuated phenotypes of GM2 gangliosidosis variant B in Japanese patients with HEXA mutations at codon 499, and five novel mutations responsible for infantile acute form.

Tanaka A, Hoang L, Nishi Y, Maniwa S, Oka M, Yamano T J Hum Genet. 2003; 48(11):571-4.

PMID: 14566483 DOI: 10.1007/s10038-003-0080-9.

The frequency of Tay-Sachs disease causing mutations in the Brazilian Jewish population justifies a carrier screening program.

Rozenberg R, Pereira L Sao Paulo Med J. 2001; 119(4):146-9.

PMID: 11500789 PMC: 11164463. DOI: 10.1590/s1516-31802001000400007.