Fine mapping of the hereditary haemorrhagic telangiectasia (HHT)3 locus on chromosome 5 excludes VE-Cadherin-2, Sprouty4 and other interval genes
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Abstract
Background
There is significant interest in new loci for the inherited condition hereditary haemorrhagic telangiectasia (HHT) because the known disease genes encode proteins involved in vascular transforming growth factor (TGF)-β signalling pathways, and the disease phenotype appears to be unmasked or provoked by angiogenesis in man and animal models. In a previous study, we mapped a new locus for HHT ( HHT3) to a 5.7 Mb region of chromosome 5. Some of the polymorphic markers used had been uninformative in key recombinant individuals, leaving two potentially excludable regions, one of which contained loci for attractive candidate genes encoding VE Cadherin-2, Sprouty4 and FGF1, proteins involved in angiogenesis.
Methods
Extended analyses in the interval-defining pedigree were performed using informative genomic sequence variants identified during candidate gene sequencing. These variants were amplified by polymerase chain reaction; sequenced on an ABI 3730xl, and analysed using FinchTV V1.4.0 software.Results
Informative genomic sequence variants were used to construct haplotypes permitting more precise citing of recombination breakpoints. These reduced the uninformative centromeric region from 141.2-144 Mb to between 141.9-142.6 Mb, and the uninformative telomeric region from 145.2-146.9 Mb to between 146.1-146.4 Mb.Conclusions
The HHT3interval on chromosome 5 was reduced to 4.5 Mb excluding 30% of the coding genes in the original HHT3interval. Strong candidates VE-cadherin-2 and Sprouty4 cannot be HHT3.
Article Details
How to Cite
GOVANI, Fatima S; SHOVLIN, Claire L.
Fine mapping of the hereditary haemorrhagic telangiectasia (HHT)3 locus on chromosome 5 excludes VE-Cadherin-2, Sprouty4 and other interval genes.
Vascular Cell, [S.l.], v. 2, n. 1, p. 15, aug. 2010.
ISSN 2045-824X.
Available at: <https://vascularcell.com/index.php/vc/article/view/10.1186-2040-2384-2-15>. Date accessed: 18 dec. 2024.
doi: http://dx.doi.org/10.1186/2040-2384-2-15.
Section
Original Research