Sperm ubiquitination in patients with dysplasia of the fibrous sheath

doi:10.1093/humrep/17.8.2119

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Human Reproduction, Vol. 17, No. 8, 2119-2127, August 2002
© 2002 European Society of Human Reproduction and Embryology

Sperm ubiquitination in patients with dysplasia of the fibrous sheath

V.Y. Rawe¹, S.Brugo Olmedo¹, A. Benmusa², S.M. Shiigi³, H.E. Chemes⁴ and P. Sutovsky²^,5

¹ Centro de Estudios en Ginecología y Reproducción, CEGyR, 1055-Buenos Aires, Argentina, ² Departments of Obstetrics and Gynecology and Animal Sciences, University of Missouri-Columbia, S141 ASRC, Columbia, MO 65211–5300, ³ Oregon Health and Science University, Oregon Regional Primate Research Center, 505 NW 185th Avenue, Beaverton, OR 97006, USA and ⁴ Laboratory of Testicular Physiology and Pathology, Endocrinology Division, Children's Hospital, Buenos Aires, Argentina

BACKGROUND: Human sperm with structural abnormalities displayan increased content of the cellular proteolytic marker peptide,ubiquitin. We investigated whether dysplasia of the fibroussheath (DFS), a severe structural anomaly found in the spermof some asthenozoospermic patients, is accompanied by (i) increasedubiquitination of the sperm surface and (ii) by increased ubiquitinationof the sperm mitochondria. METHODS AND RESULTS: Five DFS patientsand eight fertile donors were studied by immunocytochemistrywith anti-ubiquitin antibodies. Increased cross-reactivity ofthe ubiquitinated mitochondrial epitopes was seen in 32–50%of DFS sperm, but only 2–4.1% of sperm from fertile donors.Sperm surface ubiquitination assessed by sperm-ubiquitin tagimmunoassay (SUTI) and immunofluorescence demonstrated an increasedsperm ubiquitination in all DFS patients. The average medianvalue of ubiquitin-induced fluorescence in DFS patients was25.8 counts (range 19.8–37.9), as opposed to 13.4 countsrange (9.3–16.6) in fertile men. Sperm with `stump tails',coiled tails, twin and triplet sperm, and clusters of immaturespermatogenic cells were common. CONCLUSIONS: DFS sperm haveincreased cross-reactivity to anti-ubiquitin antibodies, a findingconsistent with the ubiquitination of defective sperm shownin animal models. These results justify the use of ubiquitin-basedassays for objective semen analysis in infertile men with heritabledefects.

Key words: asthenozoospermia/dysplasia of the fibrous sheath/male infertility/sperm mitochondria/ubiquitin

⁵ To whom correspondence should be addressed at: University ofMissouri-Columbia, S141 ASRC, 920 East Campus Drive, Columbia,MO 65211–5300, USA. E-mail: SutovskyP{at}missouri.edu

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