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The use of cloned Y chromosome-specific DNA probes for fetal sex determination in first trimester prenatal diagnosis
Authors:J. R. Gosden  C. M. Gosden  S. Christie  H. J. Cooke  J. M. Morsman  C. H. Rodock
Affiliation:(1) MRC Clinical and Population Cytogenetics Unit, Western General Hospital, Edinburgh, Scotland;(2) MRC Mammalian Genome Unit, Kings Buildings, Edinburgh, Scotland;(3) Dept. of Obstetrics and Gynaecology, King's College Hospital Medical School, London, UK
Abstract:Summary Prenatal diagnosis by chorion biopsy in the first trimester of pregnancy has advantages over second trimester amniocentesis because diagnosis can be achieved at 9–12 weeks gestation, reducing prenatal anxiety and avoiding the trauma of late abortion. DNA can be prepared from chorionic villus biopsies in sufficient quantity and purity for use in prenatal diagnosis systems using specific DNA probes hybridised to restriction endonuclease digests.DNA probes derived from the Y chromosome have been used to determine fetal sex. The use of such probes means that the chromosomal sex of the fetus can be identified more quickly than by chromosome preparation and more accurately than by sex chromatin staining, and has the additional advantage that the same DNA preparation can be used for other diagnostic tests. A dot hybridisation method has been successfully used to provide even more rapid results than conventional hybridisation to Southern blots of restriction endonuclease digests.There is a risk that Y chromosome-specific DNA probes for sex determination may be subject to error if the parents have extreme Y chromosome variants such as a small or non-fluorescent Y or a Y autosome chromosome translocation. The precise extent to which such chromosome variants may lead to error has been investigated. Even extreme Y chromosome variants totally lacking fluorescence were identified as male by the cloned probes used. However, Y autosome translocations carried by females could cause error if not identified in the parents. The value of the probes has been confirmed provided that parental chromosomes and DNA are examined in parallel with the chorionic biopsy material
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