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. 2014 Jan 23:15:14.
doi: 10.1186/1471-2350-15-14.

Diagnosis of Noonan syndrome and related disorders using target next generation sequencing

Francesca Romana Lepri  1 Rossana ScavelliMaria Cristina DigilioMaria GnazzoSimona GrottaMaria Lisa DenticiElisa PisaneschiPietro SirletoRossella CapolinoAnwar BabanSerena RussoTiziana FranchinAdriano AngioniBruno Dallapiccola
Affiliations

Diagnosis of Noonan syndrome and related disorders using target next generation sequencing

Francesca Romana Lepri et al. BMC Med Genet. .

Abstract

Background: Noonan syndrome is an autosomal dominant developmental disorder with a high phenotypic variability, which shares clinical features with other rare conditions, including LEOPARD syndrome, cardiofaciocutaneous syndrome, Noonan-like syndrome with loose anagen hair, and Costello syndrome. This group of related disorders, so-called RASopathies, is caused by germline mutations in distinct genes encoding for components of the RAS-MAPK signalling pathway. Due to high number of genes associated with these disorders, standard diagnostic testing requires expensive and time consuming approaches using Sanger sequencing. In this study we show how targeted Next Generation Sequencing (NGS) technique can enable accurate, faster and cost-effective diagnosis of RASopathies.

Methods: In this study we used a validation set of 10 patients (6 positive controls previously characterized by Sanger-sequencing and 4 negative controls) to assess the analytical sensitivity and specificity of the targeted NGS. As second step, a training set of 80 enrolled patients with a clinical suspect of RASopathies has been tested. Targeted NGS has been successfully applied over 92% of the regions of interest, including exons for the following genes: PTPN11, SOS1, RAF1, BRAF, HRAS, KRAS, NRAS, SHOC, MAP2K1, MAP2K2, CBL.

Results: All expected variants in patients belonging to the validation set have been identified by targeted NGS providing a detection rate of 100%. Furthermore, all the newly detected mutations in patients from the training set have been confirmed by Sanger sequencing. Absence of any false negative event has been excluded by testing some of the negative patients, randomly selected, with Sanger sequencing.

Conclusion: Here we show how molecular testing of RASopathies by targeted NGS could allow an early and accurate diagnosis for all enrolled patients, enabling a prompt diagnosis especially for those patients with mild, non-specific or atypical features, in whom the detection of the causative mutation usually requires prolonged diagnostic timings when using standard routine. This approach strongly improved genetic counselling and clinical management.

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Figures

Figure 1
Figure 1
Screenshots of the designed panel within DS software.
Figure 2
Figure 2
Flowchart of how the analysis was carried out.
Figure 3
Figure 3
An example of three different mutations (A. PTPN11 :Y63C; B. SOS1 : M269R; C. BRAF : K601I) identified by Miseq.
Figure 4
Figure 4
Performance of the same target (PTPN11_exon8) region through 3 different sequencing runs (A. first run; B. second run; C. third run).
Figure 5
Figure 5
Comparison of time (A) and cost (B) between NGS and Sanger sequencing.
See this image and copyright information in PMC

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