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Molecular Human Reproduction, Vol. 5, No. 6, 498-506, June 1999
© 1999 European Society of Human Reproduction and Embryology

The neoglycoprotein mannose–bovine serum albumin, but not progesterone, activates T-type calcium channels in human spermatozoa*

Peter F. Blackmore1 and Stefan Eisoldt

Department of Physiological Sciences, Eastern Virginia Medical School, P.O. Box 1980, Norfolk, VA 23501, USA

The neoglycoproteins {alpha}-D-mannose–bovine serum albumin (mannose–BSA) and N-acetyl-{alpha}-D-glucosamine–BSA (glucNAc–BSA) were shown to rapidly increase intracellular free calcium ([Ca2+]i) in human spermatozoa. The increase in [Ca2+]i induced by these neoglycoproteins accounts for the known ability of these compounds to induce the acrosome reaction in human spermatozoa. Our data support the hypothesis that mannose–BSA, but not progesterone, activates T-type Ca2+ channels in human spermatozoa for the following reasons: (i) the capacity of mannose–BSA to increase [Ca2+]i was inhibited by the specific T-type Ca2+ channel blocker mibefradil (IC50 = 10–6 mol/l) while progesterone was not inhibited by 10–5 M mibefradil; (ii) the effect of mannose–BSA to elevate [Ca2+]i was inhibited more potently by Ni2+ (IC50 = 0.1 mmol/l) than Cd2+ (IC50 = 0.5 mmol/l), whereas the effect of progesterone to elevate [Ca2+]i was inhibited equally by Ni2+ and Cd2+ (IC50 = 0.25 mmol/l); (iii) the effects of mannose–BSA and progesterone to increase [Ca2+]i were greater than additive. These data support the idea that mannose–BSA and progesterone were activating distinct Ca2+ channels, one of which was a T-type Ca2+ channel activated by mannose–BSA whereas the Ca2+ channel that was activated by progesterone has yet to be defined at the molecular level.

calcium/mannose–BSA/progesterone/spermatozoa/T-type

*Some of the material in this manuscript was presented during a talk given by Peter Blackmore at The First International Meeting on Rapid Responses of Steroid Hormones, held in Mannheim, Germany, September 18–20, 1998.

1 To whom correspondence should be addressed


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