Peer-Reviewed Journal Details
Mandatory Fields
Roy, NBA;Wilson, EA;Henderson, S;Wray, K;Babbs, C;Okoli, S;Atoyebi, W;Mixon, A;Cahill, MR;Carey, P;Cullis, J;Curtin, J;Dreau, H;Ferguson, DJP;Gibson, B;Hall, G;Mason, J;Morgan, M;Proven, M;Qureshi, A;Garcia, JS;Sirachainan, N;Teo, J;Tedgard, U;Higgs, D;Roberts, D;Roberts, I;Schuh, A
2016
October
British Journal of Haematology
A novel 33-Gene targeted resequencing panel provides accurate, clinical-grade diagnosis and improves patient management for rare inherited anaemias
Validated
WOS: 41 ()
Optional Fields
BONE-MARROW FAILURE DIAMOND-BLACKFAN ANEMIA HEMOLYTIC-ANEMIA WHOLE GENOME MUTATIONS DEFICIENCY PRECISION STANDARDS VARIANTS REVEALS
175
318
330
Accurate diagnosis of rare inherited anaemias is challenging, requiring a series of complex and expensive laboratory tests. Targeted next-generation-sequencing (NGS) has been used to investigate these disorders, but the selection of genes on individual panels has been narrow and the validation strategies used have fallen short of the standards required for clinical use. Clinical-grade validation of negative results requires the test to distinguish between lack of adequate sequencing reads at the locations of known mutations and a real absence of mutations. To achieve a clinically-reliable diagnostic test and minimize false-negative results we developed an open-source tool (CoverMi) to accurately determine base-coverage and the discoverability' of known mutations for every sample. We validated our 33-gene panel using Sanger sequencing and microarray. Our panel demonstrated 100% specificity and 997% sensitivity. We then analysed 57 clinical samples: molecular diagnoses were made in 22/57 (386%), corresponding to 32 mutations of which 16 were new. In all cases, accurate molecular diagnosis had a positive impact on clinical management. Using a validated NGS-based platform for routine molecular diagnosis of previously undiagnosed congenital anaemias is feasible in a clinical diagnostic setting, improves precise diagnosis and enhances management and counselling of the patient and their family.
HOBOKEN
0007-1048
10.1111/bjh.14221
Grant Details