Mutational analysis of FANCL, FANCM and the recently identified FANCI suggests that among the 13 known Fanconi Anemia genes, only FANCD1/BRCA2 plays a major role in high-risk breast cancer predisposition

doi:10.1093/carcin/bgp218

Carcinogenesis Advance Access originally published online on September 8, 2009
Carcinogenesis 2009 30(11):1898-1902; doi:10.1093/carcin/bgp218

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Mutational analysis of FANCL, FANCM and the recently identified FANCI suggests that among the 13 known Fanconi Anemia genes, only FANCD1/BRCA2 plays a major role in high-risk breast cancer predisposition

María J. García¹^,2^,*, Victoria Fernández¹^,2, Ana Osorio¹^,2, Alicia Barroso¹^,2, Fernando Fernández¹^,2, Miguel Urioste¹^,2 and Javier Benítez¹^,2

¹ Group of Human Genetics, Human Cancer Genetics Program, Spanish National Cancer Centre (CNIO), C/ Melchor Fernández Almagro 3, 28029 Madrid, Spain
² Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), Instituto de Salud Carlos III, Madrid, Spain

^* To whom correspondence should be addressed. Tel: +34 917328000; Fax: +34 912246911; Email: mjgarcia{at}cnio.es

Fanconi Anemia (FA) is a rare recessive syndrome characterizedby cellular hypersensitivity to DNA-cross-linking agents. Todate, 13 FA complementation groups have been described and all13 genes associated to each of these groups have been currentlyidentified. Three of the known FA genes are also high-risk (FANCD1/BRCA2)or moderate-risk (FANCN/PALB2 and FANCJ/BRIP1) breast cancersusceptibility genes, which makes all members of the FA pathwayparticularly attractive breast cancer candidate genes. MostFA genes have been screened for mutations in breast cancer familiesnegative for BRCA1/2 mutations but the role of FANCL, FANCMand the recently identified FANCI has not been evaluated todate. This fact and novel data sustaining greater functionalrelevance of the three genes within the FA pathway promptedus to scrutinize all coding sequences and splicing sites ofFANCI, FANCL and FANCM in 95 BRCA1/2-negative index cases fromSpanish high-risk breast cancer families. We identified 68 sequencevariants of which 24 were coding and 44 non-coding. Six exonicand 26 non-coding variants had not been described previously.None of the coding changes caused clearly pathogenic changesand computational analysis of all non-described intronic variantsdid not revealed major impact in splicing. With the presentstudy, all known FA genes have been evaluated within the contextof breast cancer high-risk predisposition. Our results ruleout a major role of FANCI, FANCL and FANCM in familial breastcancer susceptibility, suggesting that among the 13 known FAgenes, only FANCD1/BRCA2 plays a major role in high-risk breastcancer predisposition.

Abbreviations: FA, Fanconi Anemia; PCR, polymerase chain reaction

Received May 24, 2009; revised August 18, 2009; accepted August 31, 2009.

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