| Literature DB >> 31573083 |
Elisabeth Castellanos1, Inma Rosas1, Alex Negro1, Bernat Gel1, Andreu Alibés2, Neus Baena3, Mercè Pineda4, Graciela Pi5, Guillem Pintos6, Hector Salvador7, Conxi Lázaro8,9, Ignacio Blanco10, Lluïsa Vilageliu11, Hilde Brems12, Daniel Grinberg11, Eric Legius12, Eduard Serra1,9.
Abstract
Children with neurofibromatosis type 1 (NF1) may exhibit an incomplete clinical presentation, making difficult to reach a clinical diagnosis. A phenotypic overlap may exist in children with other RASopathies or with other genetic conditions if only multiple café-au-lait macules (CALMs) are present. The syndromes that can converge in these inconclusive phenotypes have different clinical courses. In this context, an early genetic testing has been proposed to be clinically useful to manage these patients. We present the validation and implementation into diagnostics of a custom NGS panel (I2HCP, ICO-IMPPC Hereditary Cancer Panel) for testing patients with a clinical suspicion of a RASopathy (n = 48) and children presenting multiple CALMs (n = 102). We describe the mutational spectrum and the detection rates identified in these two groups of individuals. We identified pathogenic variants in 21 out of 48 patients with clinical suspicion of RASopathy, with mutations in NF1 accounting for 10% of cases. Furthermore, we identified pathogenic mutations mainly in the NF1 gene, but also in SPRED1, in more than 50% of children with multiple CALMs, exhibiting an NF1 mutational spectrum different from a group of clinically diagnosed NF1 patients (n = 80). An NGS panel strategy for the genetic testing of these two phenotype-defined groups outperforms previous strategies.Entities:
Keywords: NGS panel; RASopathies; genetic testing; multiple CALMs; neurofibromatosis type 1
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Year: 2019 PMID: 31573083 DOI: 10.1111/cge.13649
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438