[Prenatal genetic diagnosis of oculocutaneous albinism type II through mutation detection combined with SNPs linkage analysis].

[oculocutaneous albinism]

To provide prenatal diagnosis for two families affected with oculocutaneous albinism (OCA ), in both of which only 1 pathogenic allele has been identified .To determine the clinical classification of OCA through DNA sequencing for TYR , P , TYRP 1 and SLC 45 A 2 genes in combination with phenotype analysis . Prenatal diagnosis was carried out by direct sequencing and intragenic SNPs family-based linkage analysis .In the first family , only 1 heterozygous mutation c .1255 C >T was found in the proband , which was inherited from her mother . Together with its clinical phenotype , the proband was suspected to have OCA 2 Screening of amniotic fluid , however , has found no mutation . With family-based linkage analysis , the fetus was deemed to be an OCA 2 carrier . In the second family , again only one heterozygous mutation c .1920 _1949 del 30 bp and ins AACA was found in the proband , which was inherited from her father . Together with its clinical phenotype , the proband was suspected to have OCA 2 . Screening of amniotic fluid has revealed a heterozygous mutation c .1920 _1949 del 30 bp and ins AACA . By family-based linkage analysis , the fetus was deemed to be an OCA 2 carrier . Both fetuses had a normal phenotype at birth .Prenatal genetic diagnosis has been provided for the first time for two families affected with OCA , in which only 1 pathogenic mutant allele was detected . The combined mutation detection and SNPs linkage analysis has turned out to be successful .