| Literature DB >> 26581427 |
Virginia Andreotti1,2, Alessandra Bisio3, Brigitte Bressac-de Paillerets4, Mark Harland5, Odile Cabaret4, Julia Newton-Bishop5, Lorenza Pastorino1,2, William Bruno1,2, Roberto Bertorelli6, Veronica De Sanctis6, Alessandro Provenzani7, Chiara Menin8, Gilberto Fronza9, Paola Queirolo10, Robert C Spitale11, Giovanna Bianchi-Scarrà1,2, Alberto Inga3, Paola Ghiorzo1,2.
Abstract
Many variants of uncertain functional significance in cancer susceptibility genes lie in regulatory regions, and clarifying their association with disease risk poses significant challenges. We studied 17 germline variants (nine of which were novel) in the CDKN2A 5'UTR with independent approaches, which included mono and bicistronic reporter assays, Western blot of endogenous protein, and allelic representation after polysomal profiling to investigate their impact on CDKN2A mRNA translation regulation. Two of the novel variants (c.-27del23, c.-93-91delAGG) were classified as causal mutations (score ≥3), along with the c.-21C>T, c.-34G>T, and c.-56G>T, which had already been studied by a subset of assays. The novel c.-42T>A as well as the previously described c.-67G>C were classified as potential mutations (score 1 or 2). The remaining variants (c.-14C>T, c.-20A>G, c.-25C>T+c.-180G>A, c.-30G>A, c.-40C>T, c.-45G>A, c.-59C>G, c.-87T>A, c.-252A>T) were classified as neutral (score 0). In conclusion, we found evidence that nearly half of the variants found in this region had a negative impact on CDKN2A mRNA translation, supporting the hypothesis that 5'UTR can act as a cellular Internal Ribosome Entry Site (IRES) to modulate p16(INK) (4a) translation.Entities:
Keywords: 5′ untranslated region; CDKN2A; germline mutation; melanoma susceptibility; polysomal imbalance; reporter assays; variants with unknown functional significance
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Year: 2015 PMID: 26581427 DOI: 10.1111/pcmr.12444
Source DB: PubMed Journal: Pigment Cell Melanoma Res ISSN: 1755-1471 Impact factor: 4.693