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Rene H Martin*. Constitutional chromosome abnormalities are seen frequently in infertile men. The consequences of these abnormalities in sperm are outlined. Infertile men with a normal chromosome karyotype also have an increased frequency of chromosome abnormalities in their sperm and a review of these studies is presented. New research methods such as single sperm PCR and immunocytogenetic analysis of the synaptonemal complex have presented exciting new ways to study the etiology of chromosome abnormalities in humans and may provide prognostic information that assists in the management of infertile patients.
Introduction
Chromosome abnormalities are surprisingly common in humans, with an incidence of approximately 0.6% present in newborns, 6% in stillbirths and more than 60% in spontaneous abortions. Most chromosome abnormalities are lethal and are lost early in embryologic development, manifesting as infertility or spontaneous abortions. Some chromosomal abnormalities survive to term, for example trisomy 13, 18, 21 and aneuploidy for the sex chromosomes as well as certain chromosomal rearrangements such as translocations and inversions. Individuals with these chromosome anomalies can have mental and physical disabilities, infertility, behavioural problems and/or impaired sexual development. Most chromosome abnormalities have their origin during meiosis, thus information on the causes of chromosome abnormalities and factors affecting their frequency are best studied in human gametes. During the past two decades there has been an explosion of information on the chromosome complement of human spermatozoa. This has been stimulated by the advent of new techniques: human sperm karyotyping using the hamster oocyte system, fluorescence in situ hybridization (FISH) analysis, single sperm polymerase chain reaction (PCR) analysis, and synaptonemal complex (SC) analysis. Rudak et al1 first reported the use of hamster ova to reactivate human sperm allowing the analysis of pronuclear chromosomes. Other laboratories followed with the fist publications on the frequency and type of chromosome abnormalities in human sperm.2 - 5 Human sperm karyotyping, using the hamster system, provides detailed information about each individual chromosome, permitting analysis of both numerical and structural abnormalities. However, there are significant disadvantages of this approach: sperm must be capable of fertilizing hamster oocytes, the technique is very difficult, time-consuming, expensive and the data yield is small. In fact, only 12 laboratories world-wide have had success with this technique despite many efforts. Fluorescent in situ hybridization analysis with chromosome-specific DNA probes provides a faster, cheaper, easier alternative for detecting numerical abnormalities
(aneuploidy) in human sperm.6 - 8 Also, sperm with defects in fertilization ability and/or motility can be assessed using FISH analysis.9 - 11 Single sperm PCR is a difficult, timeconsuming technique but it can be used in a very powerful manner for specific studies on recombination and the etiology of chromosome abnormalities.12 , 13 Finally, a new immunocytogenetic technique allows assessment of early meiosis including the fidelity of chromosome pairing and recombination. 14 - 16 Some of the studies on infertile men, using these various techniques, will be summarized in this review.
FISH studies are assessed, the frequency of 24,YY or 24,XY sperm was 1%.25 There has been no compelling evidence for an interchromosomal effect in these men. Men with Klinefelter syndrome (47,XXY) or mosaic variants (e.g., 47,XXY/46,XY) generally have severe oligozoospermia or azoospermia and sperm can sometimes be obtained by a testicular biopsy. FISH analysis has demonstrated that the frequency of aneuploidy for the sex chromosomes varies from 1.5%26 to 7%27 in sperm from Klinefelter mosaics and 2%28 to 25%29 in the sperm of men who appear to have a nonmosaic 47,XXY karyotype (for review see ref. 17). Chromosomally normal offspring as well as conceptions with a 47,XXY karyotype have been reported in Klinefelter Syndrome males who have fathered a pregnancy through intracytoplasmic sperm injection (ICSI).17
Translocations
Robertsonian translocation carriers have a fusion of the long arms of two acrocentric chromosomes resulting in a balanced state with 45 chromosomes. Pairing of the chromosomes at meiosis can lead to chromosomally balanced and unbalanced gametes. Sperm karyotyping studies have demonstrated that 3-27% of the spermatozoa are unbalanced.30 FISH studies in 13 Robertsonian translocation heterozygotes have shown similar frequencies of imbalance varying from 7%31 to 26%.20 Interchromosomal effects were reported in 4 studies (e.g., see refs. 32, 33) but none of the increased disomy frequencies were higher than 1%. Reciprocal translocations occur when there are exchanges of chromosome material between any chromosomes. During meiosis, 4 chromosomes must pair in reciprocal translocation heterozygotes and the resulting segregations have a higher frequency of unbalanced chromosomes than Robertsonian translocations. Sperm karyotyping studies of over 30 reciprocal translocation heterozygotes have shown that 19-77% of spermatozoa are unbalanced.18 FISH analyses of chromosome segregations in over 30 carriers have reported frequencies of unbalanced chromosomes ranging from 49%-81%.34 , 35 In one interesting study, 4 male family members of a kindred segregating a chromosome 15; 17 translocation, were studied by FISH analysis.36 The segregation patterns were very similar in all 4 men with approximately 50% of sperm chromosomally unbalanced. This demonstrates the reproducibility of the method. Because the frequency of chromosome abnormality is very high, some men carrying reciprocal translocations have undergone preimplantation genetic diagnosis (PGD) in order to implant only chromosomally normal or balanced embryos. Studies comparing the frequency of chromosome abnormalities in sperm and embryos from reciprocal translocation carriers show a very close agreement in the abnormality frequencies.20 Indeed, it has been shown that the incidence of abnormal sperm from translocation carriers is predictive of the proportion of aneuploid embryos they will produce during a PGD cycle. This in turn has a direct influence on the patient's chances of becoming pregnant. Many FISH studies have assessed the possibility of an interchromosomal effect in reciprocal translocation heterozygotes. An increased frequency for at least one type of disomy was reported in 58% of carriers.17 Disomy frequencies were 1.5 to 6.6 times those observed in control
donors. However, preliminary evidence from studies of preimplantation genetic diagnosis suggests an interchromosomal effect for Robertsonian translocations, but not for reciprocal translocation.37
If the frequency of recombination is reduced or absent for these chromosomes, they may be particularly susceptible to nondisjunction. Indeed, it has been shown that 47,XXY of paternal origin is associated with a decreased recombination frequency.52 For a direct test of whether recombination is associated with nondisjunction in human sperm, we performed single sperm PCR analysis for a sex specific locus (STS/STS pseudogene) and a pseudoautosomal locus (DXY515).12 Individual unisomic sperm (23,X or Y) were isolated using a FACStarPlus flow cytometer into PCR tubes. To identify disomic 24,XY sperm, 3-colour FISH analysis was performed with probes for chromosomes X, Y and 1. The 24,XY cells were identified using fluorescence microscopy, each disomic sperm was scraped off the slide using a glass needle attached to a micromanipulator and then put into a PCR tube. Heminested PCR analysis of the two markers was performed to determine the frequency of recombination. The frequency of recombination between the two DNA markers was 38% for the normal unisomic sperm compared to 25% for the 24,XY disomic sperm that had undergone nondisjunction. This difference was highly significant and demonstrates that lack of recombination in the pseudoautosomal region is associated with XY nondisjunction and the production of aneuploid sperm.
Conclusions
Cytogenetic analysis of somatic cells, sperm cells and testicular tissue are all important in the diagnosis of male infertility and in determining the etiology of chromosome abnormalities.
Acknowledgements
Rene H. Martin holds the Canada Research Chair in Genetics and her research is supported by grant MA-7961 from the Canadian Institutes of Health Research.
References
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Figures
Figure 1
Example of human spermatocyte in pachytene stage. Chromosome bivalents are paired with 22 mature autosomal synaptonemal complexes (red) and sex chromosomes (marked
X and Y). Centromeres are shown in blue (CREST). The MLH1 foci (yellow) indicate recombination sites. A color version of this figure may be viewed at http://www.Eurekah.com. Copyright 2000-2011, Landes Bioscience and Springer Science+Business Media.