Hereditary haemorrhagic telangiectasia: mutation detection, test sensitivity and novel mutations

NL Prigoda, S Savas, SA Abdalla, B Piovesan… - Journal of medical …, 2006 - jmg.bmj.com
NL Prigoda, S Savas, SA Abdalla, B Piovesan, D Rushlow, K Vandezande, E Zhang…
Journal of medical genetics, 2006jmg.bmj.com
Background: Hereditary haemorrhagic telangiectasia (HHT) is a genetic disorder present in
1 in 8000 people and associated with arteriovenous malformations. Genetic testing can
identify individuals at risk of developing the disease and is a useful diagnostic tool.
Objective: To present a strategy for mutation detection in families clinically diagnosed with
HHT. Methods: An optimised strategy for detecting mutations that predispose to HHT is
presented. The strategy includes quantitative multiplex polymerase chain reaction …
Background: Hereditary haemorrhagic telangiectasia (HHT) is a genetic disorder present in 1 in 8000 people and associated with arteriovenous malformations. Genetic testing can identify individuals at risk of developing the disease and is a useful diagnostic tool.
Objective: To present a strategy for mutation detection in families clinically diagnosed with HHT.
Methods: An optimised strategy for detecting mutations that predispose to HHT is presented. The strategy includes quantitative multiplex polymerase chain reaction, sequence analysis, RNA analysis, validation of missense mutations by amino acid conservation analysis for the ENG (endoglin) and ACVRL1 (ALK1) genes, and analysis of an ACVRL1 protein structural model. If no causative ENG or ACVRL1 mutation is found, proband samples are referred for sequence analysis of MADH4 (associated with a combined syndrome of juvenile polyposis and HHT).
Results: Data obtained over the past eight years were summarised and 16 novel mutations described. Mutations were identified in 155 of 194 families with a confirmed clinical diagnosis (80% sensitivity). Of 155 mutations identified, 94 were in ENG (61%), 58 in ACVRL1 (37%), and three in MADH4 (2%).
Conclusions: For most missense variants of ENG and ACVRL1 reported to date, study of amino acid conservation showed good concordance between prediction of altered protein function and disease occurrence. The 39 families (20%) yet to be resolved may carry ENG, ACVRL1, or MADH4 mutations too complex or difficult to detect, or mutations in genes yet to be identified.
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