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Molecular Human Reproduction, Vol. 6, No. 9, 861-866, September 2000
© 2000 European Society of Human Reproduction and Embryology


Genetic diagnosis

CAG trinucleotide repeats in the androgen receptor gene of infertile men exhibit stable inheritance in female offspring conceived after ICSI

D.S. Cram1,2,4, B. Song2, R.I. McLachlan1,3 and A.O. Trounson2

1 Monash IVF, Australia, 2 Monash Institute of Reproduction and Development, Clayton 3168, Australia, and 3 Prince Henry's Institute of Medical Research

Abstract

The androgen receptor (AR) gene is located on the X chromosome and contains a polymorphic CAG tract. CAG repeat expansions in the AR have been associated with male infertility and the neuromuscular disease, spinal bulbar muscular atrophy (SBMA). Based on Mendelian inheritance patterns, moderate CAG expansions in infertile men treated by intracytoplasmic sperm injection (ICSI) would be vertically transmitted to female offspring. Should further elongation of the repeat region occur in the male germline, it is conceivable that longer expansions could also be transmitted by ICSI and may lead to an increased incidence of male infertility and SBMA in succeeding generations. To determine the degree of stability of the paternal AR CAG tract following ICSI, we compared the CAG repeat number in the AR alleles of 92 men presenting for ICSI and their 99 ICSI-conceived daughters. CAG repeat lengths in the AR alleles were determined by fluorescent polymerase chain reaction and Genescan analysis of amplification products separated on DNA sequencing gels. In the vast majority of cases (95 out of 99), we found that the AR CAG tracts ranging in size from 15–28 repeats exhibited stable inheritance in female offspring. However, in the remaining father–daughter pairs, there was a discordance in the expected inheritance pattern with evidence for both CAG expansion (20->24; 22->23) and contraction (26->18 or 22) of the paternal AR allele. The detection of a low frequency of CAG mutation in paternal AR alleles following ICSI would be consistent with gonadal mosaicism originating from meiotic DNA replication errors. These findings in a typical group of infertile men undergoing ICSI for a variety of indications tend to alleviate concerns that ICSI may promote the transmission of AR alleles with expanded CAG tracts and suggest that the risk of SBMA in second generation sons would be extremely low.

androgen receptor/CAG repeat/ICSI/male infertility/spinal bulbar muscular atrophy

Notes

4 To whom correspondence should be addressed at: Monash Institute of Reproduction and Development, Clayton 3168, Australia. E-mail: david.cram{at}med.monash.edu.au


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