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Deep Intronic Mutation in SERPING1 Caused Hereditary Angioedema Through Pseudoexon Activation
P. Hujová, P. Souček, L. Grodecká, H. Grombiříková, B. Ravčuková, P. Kuklínek, R. Hakl, J. Litzman, T. Freiberger
Language English Country Netherlands
Document type Journal Article, Research Support, Non-U.S. Gov't
Grant support
NV16-34414A
MZ0
CEP Register
Digital library NLK
Full text - Article
NLK
ProQuest Central
from 1997-01-01
Medline Complete (EBSCOhost)
from 2010-01-01 to 1 year ago
Health & Medicine (ProQuest)
from 1997-01-01
Public Health Database (ProQuest)
from 1997-01-01
Springer Nature OA/Free Journals
from 1981-01-01
- MeSH
- Child MeSH
- Adult MeSH
- Exons genetics MeSH
- Hereditary Angioedema Types I and II genetics MeSH
- Complement C1 Inhibitor Protein genetics MeSH
- Introns genetics MeSH
- Middle Aged MeSH
- Humans MeSH
- RNA Splice Sites genetics MeSH
- Adolescent MeSH
- Young Adult MeSH
- Mutation genetics MeSH
- DNA Mutational Analysis methods MeSH
- Pedigree MeSH
- Aged MeSH
- Protein Splicing genetics MeSH
- Check Tag
- Child MeSH
- Adult MeSH
- Middle Aged MeSH
- Humans MeSH
- Adolescent MeSH
- Young Adult MeSH
- Male MeSH
- Aged MeSH
- Female MeSH
- Publication type
- Journal Article MeSH
- Research Support, Non-U.S. Gov't MeSH
PURPOSE: Hereditary angioedema (HAE) is a rare autosomal dominant life-threatening disease characterized by low levels of C1 inhibitor (type I HAE) or normal levels of ineffective C1 inhibitor (type II HAE), typically occurring as a consequence of a SERPING1 mutation. In some cases, a causal mutation remains undetected after using a standard molecular genetic analysis. RESULTS: Here we show a long methodological way to the final discovery of c.1029 + 384A > G, a novel deep intronic mutation in intron 6 which is responsible for HAE type I in a large family and has not been identified by a conventional diagnostic approach. This mutation results in de novo donor splice site creation and subsequent pseudoexon inclusion, the mechanism firstly described to occur in SERPING1 in this study. We additionally discovered that the proximal part of intron 6 is a region potentially prone to pseudoexon-activating mutations, since natural alternative exons and additional cryptic sites occur therein. Indeed, we confirmed the existence of at least two different alternative exons in this region not described previously. CONCLUSIONS: In conclusion, our results suggest that detecting aberrant transcripts, which are often low abundant because of nonsense-mediated decay, requires a modified methodological approach. We suggest SERPING1 intron 6 sequencing and/or tailored mRNA analysis to be routinely used in HAE patients with no mutation identified in the coding sequence.
Central European Institute of Technology Masaryk University Brno Czech Republic
Centre for Cardiovascular Surgery and Transplantation Brno Czech Republic
References provided by Crossref.org
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