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Nature of DNA Damage in Ejaculated Human Spermatozoa and the Possible Involvement of Apoptosis
Numerous studies have shown the presence of DNA strand breaks in human ejaculated spermatozoa. The nature of this nuclear anomaly and its relationship to patient etiology is however poorly understood. The aim of this study was to investigate the relationship between nuclear DNA damage, assessed usin...
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Published in: | Biology of reproduction 2002-04, Vol.66 (4), p.1061-1067 |
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Main Authors: | , , , , , |
Format: | Article |
Language: | English |
Subjects: | |
Online Access: | Get full text |
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Summary: | Numerous studies have shown the presence of DNA strand breaks in human ejaculated spermatozoa. The nature of this nuclear
anomaly and its relationship to patient etiology is however poorly understood. The aim of this study was to investigate the
relationship between nuclear DNA damage, assessed using the TUNEL assay and a number of key apoptotic markers, including Fas,
Bcl-x, and p53, in ejaculated human spermatozoa from men with normal and abnormal semen parameters. We also determined the
nature of the DNA damage by examining the percentage of ejaculated spermatozoa exhibiting DNA damage using the comet assay
and by challenging sperm chromatin to attack by micrococcal nuclease S7 and DNase I. We show that TUNEL positivity and apoptotic
markers do not always exist in unison; however, semen samples that had a low sperm concentration and poor morphology were
more likely to show high levels of TUNEL positivity and Fas and p53 expression. In addition, the DNA damage in ejaculated
human sperm is represented by both single- and double-stranded DNA breaks, and access to the DNA is restricted by the compacted
nature of ejaculated spermatozoa. This DNA protection is poorer in men with abnormal semen parameters. We propose that the
presence of DNA damage is not directly linked to an apoptotic process occurring in spermatozoa and arises due to problems
in the nuclear remodeling process. Subsequently, the presence of apoptotic proteins in ejaculated spermatozoa may be linked
to defects in cytoplasmic remodeling during the later stages of spermatogenesis. |
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ISSN: | 0006-3363 1529-7268 |
DOI: | 10.1095/biolreprod66.4.1061 |