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From the * Institute of Reproductive Medicine of
the University and
Institute of Clinical
Chemistry of the University, Münster, Germany.
| Correspondence to: Prof Dr E. Nieschlag FRCP, Institute of Reproductive Medicine of the University, Domagkstr. 11, D 48149 Münster, Germany (e-mail: nieschl{at}uni-muenster.de ). |
2-antiplasmin-complex (PAP); and fibrinogen. NET-EN
alone led to a depletion of sexual hormones and a marked shift in hemostatic
parameters with increasing levels of FXIIc, fibrinogen, antithrombin, and
F1+2, whereas FVIIc and FVIIa levels decreased. PAP levels increased
significantly. Opposite effects were seen in the TU/placebo group, with a
significant down-regulation of fibrinolysis and the hemostatic turnover rate.
Testosterone effects were attenuated by additional administration of
gestagens. The effect of hormonal male contraception using long-acting
testosterone esters with or without gestagens was significantly measurable
within the hemostatic system. Down-regulation of the hemostatic system with
testosterone alone may indicate an antithrombotic effect, whereas clinical
consequences of an additional gestagen compound cannot be derived.
Key words: Cardiovascular risk, gestagens, hemostasis, hormonal male contraception, testosterone
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