| Literature DB >> 27084890 |
Ilenia Simeoni1, Jonathan C Stephens2, Fengyuan Hu3, Sri V V Deevi1, Karyn Megy1, Tadbir K Bariana4, Claire Lentaigne5, Sol Schulman6, Suthesh Sivapalaratnam7, Minka J A Vries8, Sarah K Westbury9, Daniel Greene10, Sofia Papadia1, Marie-Christine Alessi11, Antony P Attwood2, Matthias Ballmaier12, Gareth Baynam13, Emilse Bermejo14, Marta Bertoli15, Paul F Bray16, Loredana Bury17, Marco Cattaneo18, Peter Collins19, Louise C Daugherty1, Rémi Favier20, Deborah L French21, Bruce Furie6, Michael Gattens22, Manuela Germeshausen12, Cedric Ghevaert23, Anne C Goodeve24, Jose A Guerrero25, Daniel J Hampshire24, Daniel P Hart26, Johan W M Heemskerk27, Yvonne M C Henskens8, Marian Hill28, Nancy Hogg29, Jennifer D Jolley30, Walter H Kahr31, Anne M Kelly32, Ron Kerr33, Myrto Kostadima1, Shinji Kunishima34, Michele P Lambert35, Ri Liesner33, José A López36, Rutendo P Mapeta1, Mary Mathias33, Carolyn M Millar5, Amit Nathwani37, Marguerite Neerman-Arbez38, Alan T Nurden39, Paquita Nurden39, Maha Othman40, Kathelijne Peerlinck41, David J Perry22, Pawan Poudel42, Pieter Reitsma43, Matthew T Rondina44, Peter A Smethurst45, William Stevenson46, Artur Szkotak47, Salih Tuna1, Christel van Geet42, Deborah Whitehorn1, David A Wilcox48, Bin Zhang49, Shoshana Revel-Vilk50, Paolo Gresele17, Daniel B Bellissimo51, Christopher J Penkett1, Michael A Laffan5, Andrew D Mumford52, Augusto Rendon53, Keith Gomez4, Kathleen Freson42, Willem H Ouwehand54, Ernest Turro55.
Abstract
Inherited bleeding, thrombotic, and platelet disorders (BPDs) are diseases that affect ∼300 individuals per million births. With the exception of hemophilia and von Willebrand disease patients, a molecular analysis for patients with a BPD is often unavailable. Many specialized tests are usually required to reach a putative diagnosis and they are typically performed in a step-wise manner to control costs. This approach causes delays and a conclusive molecular diagnosis is often never reached, which can compromise treatment and impede rapid identification of affected relatives. To address this unmet diagnostic need, we designed a high-throughput sequencing platform targeting 63 genes relevant for BPDs. The platform can call single nucleotide variants, short insertions/deletions, and large copy number variants (though not inversions) which are subjected to automated filtering for diagnostic prioritization, resulting in an average of 5.34 candidate variants per individual. We sequenced 159 and 137 samples, respectively, from cases with and without previously known causal variants. Among the latter group, 61 cases had clinical and laboratory phenotypes indicative of a particular molecular etiology, whereas the remainder had an a priori highly uncertain etiology. All previously detected variants were recapitulated and, when the etiology was suspected but unknown or uncertain, a molecular diagnosis was reached in 56 of 61 and only 8 of 76 cases, respectively. The latter category highlights the need for further research into novel causes of BPDs. The ThromboGenomics platform thus provides an affordable DNA-based test to diagnose patients suspected of having a known inherited BPD.Entities:
Mesh:
Year: 2016 PMID: 27084890 PMCID: PMC5016734 DOI: 10.1182/blood-2015-12-688267
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 25.476