期刊文献+

Presence of c.3956del C mutation in familial adenomatous polyposis patients from Brazil 被引量:1

下载PDF
导出
摘要 AIM: To characterize APC gene mutations and correlate them with patient phenotypes in individuals diagnosed with familial adenomatous polyposis(FAP) in northern Brazil. METHODS: A total of 15 individuals diagnosed with FAP from 5 different families from the north of Brazil were analyzed in this study. In addition to patients with histopathological diagnosis of FAP,family members who had not developed the disease were also tested in order to identify mutations and for possible genetic counseling. All analyzed patients or their guardians signed a consent form approved by the Research Ethics Committee of the Jo?o de Barros Barreto University Hospital(Belem,Brazil). DNA extracted from the peripheral blood of a member of each of the affected families was subjected to direct sequencing. The proband of each family was sequenced to identify germline mutations using the Ion Torrent platform. To validate the detected mutations,Sanger sequencing was also performed. The samples from all patients were also tested for the identification of mutations by real-time quantitative polymerase chain reaction using the amplification refractory mutation system. RESULTS: Through interviews with relatives and a search of medical records,it was possible to construct genograms for three of the five families included in the study. All 15 patients from the five families with FAP exhibited mutations in the APC gene,and all mutations were detected in exon 15 of the APC gene. In addition to the patients with a histological diagnosis of FAP,family members without disease symptoms showed the mutation in the APC gene. In the present study,we detected two of the three most frequent germline mutations in the literature: the mutation at codon 1309 and the mutation at codon 1061. The presence of c.3956 del C mutation was found in all families from this study,and suggests that this mutation was introduced in the population of the State of Pará through ancestor immigration(i.e.,a de novo mutation that arose in one member belonging to this state from Brazil). CONCLUSION: Regardless of its origin,the c.3956 del C mutation is a strong candidate biomarker of this hereditary cancer syndrome in families of northern Brazil. AIM: To characterize APC gene mutations and correlate them with patient phenotypes in individuals diagnosed with familial adenomatous polyposis(FAP) in northern Brazil. METHODS: A total of 15 individuals diagnosed with FAP from 5 different families from the north of Brazil were analyzed in this study. In addition to patients with histopathological diagnosis of FAP,family members who had not developed the disease were also tested in order to identify mutations and for possible genetic counseling. All analyzed patients or their guardians signed a consent form approved by the Research Ethics Committee of the Jo?o de Barros Barreto University Hospital(Belem,Brazil). DNA extracted from the peripheral blood of a member of each of the affected families was subjected to direct sequencing. The proband of each family was sequenced to identify germline mutations using the Ion Torrent platform. To validate the detected mutations,Sanger sequencing was also performed. The samples from all patients were also tested for the identification of mutations by real-time quantitative polymerase chain reaction using the amplification refractory mutation system. RESULTS: Through interviews with relatives and a search of medical records,it was possible to construct genograms for three of the five families included in the study. All 15 patients from the five families with FAP exhibited mutations in the APC gene,and all mutations were detected in exon 15 of the APC gene. In addition to the patients with a histological diagnosis of FAP,family members without disease symptoms showed the mutation in the APC gene. In the present study,we detected two of the three most frequent germline mutations in the literature: the mutation at codon 1309 and the mutation at codon 1061. The presence of c.3956 del C mutation was found in all families from this study,and suggests that this mutation was introduced in the population of the State of Pará through ancestor immigration(i.e.,a de novo mutation that arose in one member belonging to this state from Brazil). CONCLUSION: Regardless of its origin,the c.3956 del C mutation is a strong candidate biomarker of this hereditary cancer syndrome in families of northern Brazil.
出处 《World Journal of Gastroenterology》 SCIE CAS 2015年第31期9413-9419,共7页 世界胃肠病学杂志(英文版)
基金 Supported by Grants from Conselho Nacional de Desenvolvimento Científico e Tecnológico(www.cnpq.br),No.401976/2010-6 and No.305220/2013-6(to Burbano RR) Coordenacao de Aperfeicoamento de Pessoal de Nível Superior(www.capes.gov.br),No.PNPD 2810/2011(to Moreira-Nunes CA)
  • 相关文献

参考文献20

  • 1Alyssa C. Lesko,Kathleen H. Goss,Jenifer R. Prosperi.Exploiting APC Function as a Novel Cancer Therapy[J]. Current Drug Targets . 2014 (1)
  • 2Lillian Rossanese,Fernando Marson,José Ribeiro,Claudio Coy,Carmen Bertuzzo.APC germline mutations in families with familial adenomatous polyposis[J]. Oncology Reports . 2013 (5)
  • 3Jonathan Jarry,Jean-Sébastien Brunet,Rachel Laframboise,Régen Drouin,Jean Latreille,Carole Richard,Jean Gekas,Bruno Maranda,Yury Monczak,Nora Wong,Carly Pouchet,Sonya Zaor,Lidia Kasprzak,Laura Palma,Mona Kay Wu,Marc Tischkowitz,William D. Foulkes,George Chong.A survey of APC mutations in Quebec[J]. Familial Cancer . 2011 (4)
  • 4Anne Munck,Lamia Gargouri,Corinne Alberti,Jerome Viala,Michel Peuchmaur,Catherine Lenaerts,Laurent Michaud,Thierry Lamireau,Jean Francois Mougenot,Alain Dabadie,Chantal Maurage,Alain Lachaux,Michele Scaillon,Jane Languepin,Claire Spyckerelle,Martine Meyer,Sylvianne Olschwang.Evaluation of Guidelines for Management of Familial Adenomatous Polyposis in a Multicenter Pediatric Cohort[J]. Journal of Pediatric Gastroenterology and Nutrition . 2011 (3)
  • 5M.H. Nieuwenhuis,H.F.A. Vasen.Correlations between mutation site in APC and phenotype of familial adenomatous polyposis (FAP): A review of the literature[J]. Critical Reviews in Oncology and Hematology . 2006 (2)
  • 6Molecular analysis of the APC and MYH genes in Czech families affected by FAP or multiple adenomas: 13 novel mutations[J]. Hum. Mutat. . 2004 (4)
  • 7Christopher Groves,Hanan Lamlum,Michael Crabtree,Jill Williamson,Claire Taylor,Sylvia Bass,Darren Cuthbert-Heavens,Shirley Hodgson,Robin Phillips,Ian Tomlinson.Mutation Cluster Region, Association Between Germline and Somatic Mutations and Genotype-Phenotype Correlation in Upper Gastrointestinal Familial Adenomatous Polyposis[J]. The American Journal of Pathology . 2002 (6)
  • 8JudithMulkens,JacquesPoncin,Jan WillemArends,Anton F. P. M.de Goeij.APC mutations in human colorectal adenomas: analysis of the mutation cluster region with temperature gradient gel electrophoresis and clinicopathological features[J]. J. Pathol. . 1999 (4)
  • 9Claudio Soravia,Terri Berk,Lisa Madlensky,Angela Mitri,Hong Cheng,Steven Gallinger,Zane Cohen,Bharati Bapat.Genotype-Phenotype Correlations in Attenuated Adenomatous Polyposis Coli[J]. The American Journal of Human Genetics . 1998 (6)
  • 10Paul Polakis.The adenomatous polyposis coli (APC) tumor suppressor[J]. BBA - Reviews on Cancer . 1997 (3)

共引文献1

同被引文献10

引证文献1

相关作者

内容加载中请稍等...

相关机构

内容加载中请稍等...

相关主题

内容加载中请稍等...

浏览历史

内容加载中请稍等...
;
使用帮助 返回顶部