A novel mechanism of aberrant pre-mRNA splicing in humans

A novel mechanism of aberrant pre-mRNA splicing in humans

Eukaryotic pre-mRNA splicing is regulated by consensus sequences at the intron boundaries and branch site. Recently, Sirand-Pugnet at al. reported the importance of an additional intronic sequence, an (A/U)GGG repeat in chicken β-tropomyosin that is a binding site for a protein required for spliceos...

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Main Authors: Joy D. Cogan, Melissa A. Prince, Somsong Lekhakula, Sarah Bundey, Aree Futrakul, Eleanor M.S. McCarthy, John A. Phillips
Other Authors: Vanderbilt University
Format: Article
Published: 2018
Subjects:
Biochemistry, Genetics and Molecular Biology
Medicine
Online Access:https://repository.li.mahidol.ac.th/handle/123456789/17894
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spelling th-mahidol.178942018-07-04T14:50:06Z A novel mechanism of aberrant pre-mRNA splicing in humans Joy D. Cogan Melissa A. Prince Somsong Lekhakula Sarah Bundey Aree Futrakul Eleanor M.S. McCarthy John A. Phillips Vanderbilt University Mahidol University University of Birmingham Biochemistry, Genetics and Molecular Biology Medicine Eukaryotic pre-mRNA splicing is regulated by consensus sequences at the intron boundaries and branch site. Recently, Sirand-Pugnet at al. reported the importance of an additional intronic sequence, an (A/U)GGG repeat in chicken β-tropomyosin that is a binding site for a protein required for spliceosome assembly. Interestingly, we have detected mutations in IVS3 of the human growth hormone (GH) gene that affect a putative, homologous consensus sequence and which also perturb splicing. In a series of dominant-negative GH mutations that cause exon skipping, we found two mutations that do not occur within the 5' and 3' splice sites, or branch consensus sites. The first mutation is a G → A transition of the 28th base (+28G → A) of and the second deletes 18 bp (del+28-45) of IVS3 of the human GH gene. These mutations segregated with autosomal dominant GH deficiency in both kindreds and no other allelic GH gene changes were detected. RT-PCR amplification of transcripts from expression vectors containing the +28G → A or del+28-45 alleles yielded products showing a > 10-fold preferred use of alternative splicing, similar to findings previously reported for IVS3 donor site mutations. Both mutations are located 28 bp downstream from the 5' splice site and examination of the sequences perturbed revealed an intronic XGGG repeat similar to the repeat found to regulate mRNA splicing in chicken β-tropomyosin. Interestingly, the XGGG repeats involved in our mutations exhibit homologous spacing to those in a so-called 'winner' RNA sequence. Binding of A1 heterogeneous nuclear ribonucleoprotein (hnRNP) by 'winner' sequences in pre-mRNA transcripts is thought to play an important role in pre-mRNA packaging and transport as well as 5' splice site selection in pre-mRNAs that contain multiple 5' splice sites. Our findings suggest that (i) XGGG repeats may regulate alternative splicing in the human GH gene and (ii) mutations of these repeats cause GH deficiency by perturbing alternative splicing. Mutations of homologous intron sequences may underlie other human diseases. 2018-07-04T07:40:22Z 2018-07-04T07:40:22Z 1997-06-01 Article Human Molecular Genetics. Vol.6, No.6 (1997), 909-912 10.1093/hmg/6.6.909 09646906 2-s2.0-0031010287 https://repository.li.mahidol.ac.th/handle/123456789/17894 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=0031010287&origin=inward
institution Mahidol University
building Mahidol University Library
continent Asia
country Thailand
Thailand
content_provider Mahidol University Library
collection Mahidol University Institutional Repository
topic Biochemistry, Genetics and Molecular Biology
Medicine
spellingShingle Biochemistry, Genetics and Molecular Biology
Medicine
Joy D. Cogan
Melissa A. Prince
Somsong Lekhakula
Sarah Bundey
Aree Futrakul
Eleanor M.S. McCarthy
John A. Phillips
A novel mechanism of aberrant pre-mRNA splicing in humans
description Eukaryotic pre-mRNA splicing is regulated by consensus sequences at the intron boundaries and branch site. Recently, Sirand-Pugnet at al. reported the importance of an additional intronic sequence, an (A/U)GGG repeat in chicken β-tropomyosin that is a binding site for a protein required for spliceosome assembly. Interestingly, we have detected mutations in IVS3 of the human growth hormone (GH) gene that affect a putative, homologous consensus sequence and which also perturb splicing. In a series of dominant-negative GH mutations that cause exon skipping, we found two mutations that do not occur within the 5' and 3' splice sites, or branch consensus sites. The first mutation is a G → A transition of the 28th base (+28G → A) of and the second deletes 18 bp (del+28-45) of IVS3 of the human GH gene. These mutations segregated with autosomal dominant GH deficiency in both kindreds and no other allelic GH gene changes were detected. RT-PCR amplification of transcripts from expression vectors containing the +28G → A or del+28-45 alleles yielded products showing a > 10-fold preferred use of alternative splicing, similar to findings previously reported for IVS3 donor site mutations. Both mutations are located 28 bp downstream from the 5' splice site and examination of the sequences perturbed revealed an intronic XGGG repeat similar to the repeat found to regulate mRNA splicing in chicken β-tropomyosin. Interestingly, the XGGG repeats involved in our mutations exhibit homologous spacing to those in a so-called 'winner' RNA sequence. Binding of A1 heterogeneous nuclear ribonucleoprotein (hnRNP) by 'winner' sequences in pre-mRNA transcripts is thought to play an important role in pre-mRNA packaging and transport as well as 5' splice site selection in pre-mRNAs that contain multiple 5' splice sites. Our findings suggest that (i) XGGG repeats may regulate alternative splicing in the human GH gene and (ii) mutations of these repeats cause GH deficiency by perturbing alternative splicing. Mutations of homologous intron sequences may underlie other human diseases.
author2 Vanderbilt University
author_facet Vanderbilt University
Joy D. Cogan
Melissa A. Prince
Somsong Lekhakula
Sarah Bundey
Aree Futrakul
Eleanor M.S. McCarthy
John A. Phillips
format Article
author Joy D. Cogan
Melissa A. Prince
Somsong Lekhakula
Sarah Bundey
Aree Futrakul
Eleanor M.S. McCarthy
John A. Phillips
author_sort Joy D. Cogan
title A novel mechanism of aberrant pre-mRNA splicing in humans
title_short A novel mechanism of aberrant pre-mRNA splicing in humans
title_full A novel mechanism of aberrant pre-mRNA splicing in humans
title_fullStr A novel mechanism of aberrant pre-mRNA splicing in humans
title_full_unstemmed A novel mechanism of aberrant pre-mRNA splicing in humans
title_sort novel mechanism of aberrant pre-mrna splicing in humans
publishDate 2018
url https://repository.li.mahidol.ac.th/handle/123456789/17894
_version_ 1763490767590916096

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