Y;autosome translocations and mosaicism in the aetiology of 45,X maleness: assignment of fertility factor to distal Yq11

Y;autosome translocations and mosaicism in the aetiology of 45,X maleness: assignment of fertility factor to distal Yq11

Three 45,X males have been studied with Y-DNA probes by Southern blotting and in situ hybridization. Southern blotting studies with a panel of mapped Y-DNA probes showed that in all three individuals contiguous portions of the Y chromosome including all of the short arm, the centromere, and part of...

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Bibliographic Details
Published in:Human genetics Vol. 79; no. 1; pp. 2 - 7
Main Authors: ANDERSSON, M, PAGE, D. C, PETTAY, D, SUBRT, I, TURLEAU, C, DE GROUCHY, J, DE LA CHAPELLE, A
Format: Journal Article
Language:English
Published: Heidelberg Springer 01-05-1988
Berlin
New York, NY
Subjects:
Adolescent
Adult
Biological and medical sciences
Chromosome aberrations
Chromosome Banding
Chromosome Mapping
Genetic Markers
Humans
Infertility, Male - genetics
Infertility, Male - physiopathology
Karyotyping
Male
Medical genetics
Medical sciences
Mosaicism
Noonan Syndrome - genetics
Noonan Syndrome - physiopathology
Nucleic Acid Hybridization
Sex Determination Analysis
Translocation, Genetic
Y Chromosome
Chromosomal aberration
Genetic mapping
Human
Molecular hybridization
In situ
Sex chromosome
Inheritance
Aneuploidy
Acrocentric chromosome
Gene
Y»-Chromosome
Fertility
Blotting assay
Breaking point
Abnormal Y chromosome
Abnormal chromosome
Mosaicism
Male sterility
Molecular probe
Abnormal autosome
Southern blotting
Chromosome translocation
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Summary:Three 45,X males have been studied with Y-DNA probes by Southern blotting and in situ hybridization. Southern blotting studies with a panel of mapped Y-DNA probes showed that in all three individuals contiguous portions of the Y chromosome including all of the short arm, the centromere, and part of the euchromatic portion of the long arm were present. The breakpoint was different in each case. The individual with the largest portion (intervals 1-6) is a fertile male belonging to a family in which the translocation is inherited in four generations. The second adult patient, who has intervals 1-5, is an azoospermic, sterile male. These phenotypic findings suggest the existence of a gene involved in spermatogenesis in interval 6 in distal Yq11. The third case, a boy with penoscrotal hypospadias, has intervals 1-4B. In situ hybridization with the pseudoautosomal probe pDP230 and the Y chromosome specific probe pDP105 showed that Y-derived DNA was translocated onto the short arm of a chromosome 15, 14, and 14, respectively. One of the patients was a mosaic for the 14p+ translocation chromosome. Our data and those reported by others suggest the following conclusions based on molecular studies in eight 45,X males: The predominant aetiological factor is Y;autosome translocation observed in seven of the eight cases. As the remaining case was a low-grade mosaic involving a normal Y chromosome, the maleness in all cases was due to the effect of the testis determining factor, TDF. There is preferential involvement of the short arm of an acrocentric chromosome (five out of seven translocations) but other autosomal regions can also be involved. The reason why one of the derivative translocation chromosomes becomes lost may be that it has no centromere.
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ISSN:0340-6717
1432-1203
DOI:10.1007/BF00291700