Please use this identifier to cite or link to this item: https://ninho.inca.gov.br/jspui/handle/123456789/6906
Title: Identification of three novel RB1 mutations in Brazilian patients with retinoblastoma by “exon by exon” PCR mediated SSCP analysis
Authors: Braggio, Esteban
Bonvicino, Cibele Rodrigues
Vargas, Fernando Regla
Ferman, Sima Esther
Eisenberg, Ana Lucia Amaral
Abreu, Hector Nicolas Seuánez
Keywords: Brasil
Brazil
Aconselhamento Genético
Genetic Counseling
Triagem
Triage
Mutação
Mutation
Ceras
Waxes
Parafina
Paraffin
Tecidos
Tissues
Retinoblastoma
Proteína do Retinoblastoma
Retinoblastoma Protein
Reação em Cadeia da Polimerase
Polymerase Chain Reaction
Polimorfismo Conformacional de Fita Simples
Polymorphism Single-Stranded Conformational
Issue Date: 2004
Publisher: Journal of Clinical Pathology
Citation: BRAGGIO, Esteban et al. Identification of three novel RB1 mutations in Brazilian patients with retinoblastoma by “exon by exon” PCR mediated SSCP analysis. Journal of Clinical Pathology, v. 57, n. 6, p. 585–590, jun. 2004.
Abstract: To carry out a retrospective study, screening for mutations of the entire coding region of RB1 and adjacent intronic regions in patients with retinoblastoma. Methods: Mutation screening in DNA extracts of formalin fixed, paraffin wax embedded tissues of 28 patients using combined ‘‘exon by exon’’ polymerase chain reaction mediated single strand conformational polymorphism analysis, followed by DNA sequencing. Results: Eleven mutations were found in 10 patients. Ten mutations consisted of single base substitutions; 10 were localised in exonic regions (eight nonsense, one missense, and one frameshift) and another one in the intron–exon splicing region. Three novel mutations were identified: a 2 bp insertion in exon 2 (g.5506–5507insAG, R73fsX77), a G to A transition affecting the last invariant nucleotide of intron 13 (g.76429G.A), and a T to C transition in exon 20 (g.156795T.C, L688P). In addition, eight C to T transitions, resulting in stop codons, were found in five different CGA codons (g.64348C.T, g.76430C.T, g.78238C.T, g.78250C.T, and g.150037C.T). Although specific mutation hotspots have not been identified in the literature, eight of the 11 mutations occurred in CGA codons and seven fell within the E1A binding domains (codons 393–572 and 646–772), whereas five were of both types—in CGA codons within E1A binding domains. Conclusions: CGA codons and E1A binding domains are apparently more frequent mutational targets and should be initially screened in patients with retinoblastoma. Paraffin wax embedded samples proved to be valuable sources of DNA for retrospective studies, providing useful information for genetic counselling.
Description: p. 585–590.: il. p&b.
URI: http://sr-vmlxaph03:8080/jspui/handle/123456789/6906
ISSN: 1472-4146
Appears in Collections:Artigos de Periódicos da área de Pediatria



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