Anemia / 2012 / Article / Tab 2 / Research Article
Diagnosis of Fanconi Anemia: Mutation Analysis by Multiplex Ligation-Dependent Probe Amplification and PCR-Based Sanger Sequencing Table 2 Major recurrent mutations in FA.
Gene Mutation* Geographic/ethnic background Comment References FANCA c.3788_3790del (p.Phe1263del) European, Brazilian Relatively mild [14 , 15 ] c.1115_1118delTTGG (p.Val372fs) European Relatively mild [16 ] Exon 12–17del South-African Relatively common in Afrikaners [17 ] c.295C>T (p.Gln99X) Spanish Gypsy population Worldwide highest prevalence of mutant FANCA allele [18 ] FANCC c.711+4A>T (originally reported as IVS4+4A>T) Homozygous in 80% of Ashkenazi Jewish FA; relatively common in Japan. Severe phenotype in Jews, milder in Japanese. [19 –22 ] c.67delG (originally reported as 322delG) Homozygous in approx. 50% of Dutch FA patients Like other exon 1 mutations, relatively mild phenotype. [19 , 23 –25 ] FANCD2 c.1948-16T>G Turkish Founder mutation [26 ] FANCG c.313G>T (p.Glu105X) European 44% of mutated FANCG alleles in Germany. [27 ] c.1077-2A>G Portuguese/Brazilian Founder mutation [27 , 28 ] c.1480+1G>C French-Canadian Founder mutation [28 ] c.307+1G>C Japanese Founder mutation [28 , 29 ] c.1794_1803del (p.Trp599fs) European [28 ] c.637_643del (p.Tyr213fs) Sub-Saharan Africa 82% of all black FA patients [30 ] FANCJ c.2392C>T (p.Arg798X) Found in ca. 50% of FA-J patients of diverse ancestry; ancient mutation or hot spot. [11 , 12 ]
Nucleotide numbering based on A TG = +1.http://www.rockefeller.edu/fanconi/ .
