Testosterone enanthate at a dose of 200 mg/week decreases HDL-cholesterol levels in healthy men
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Marcovina, Santica M.
Meriggiola, M. Cristina
Bremner, William J.
Paulsen, C. Alvin
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Volume Title
Publisher
Blackwell Publishing
Abstract
The concept that androgen alone can provide an effective male
contraceptive has been tested in a multicentre, multiphase trial by the
World Health Organization. Results from this trial showed that an ester of
testosterone, testosterone enanthate (TE), administered at a dose of 200
mg/week, has a very high contraceptive efficacy, and suggested that, at
least in some populations, androgen alone might provide a viable option
for the control of male fertility. It has been claimed that testosterone
represents one of the gender-related risk factors for coronary artery
disease (CAD) in men. Epidemiological and interventional studies have
failed to establish a convincing relationship between testosterone and
high density lipoprotein cholesterol (HDL-C). Therefore, there is concern
about possible negative effects on lipoprotein asset of an androgen-alone
male contraceptive. In this study we analysed the effects of long-term (12
months) administration of TE (200 mg/week) in normal healthy men. Blood
samples (six men > 10 h fast = Group 1; 30 men > 4 h fast = Group 2) were
drawn from 36 men, monthly before the beginning of the injections
(control), every 3 months throughout the study period (treatment), and 1
month after stopping TE injections (recovery). Total cholesterol (chol),
triglycerides, HDL-C and LDL-C levels were measured in these samples.
Biochemical parameters were also monitored. TE administration induced a
significant decrease (15-20%) in HDL-C levels that was of comparable
magnitude in men from both groups (fasting and non-fasting) and occurred
regardless of basal HDL-C levels. No statistically significant effect on
other lipoproteins was detected. Considering all men together, HDL-C
levels were decreased in 78% of the men by month 3, 83% by month 6, 94% by
month 9 and 97% by month 12 of treatment. In all men the HDL-C decrease
was reversible within 1 month of stopping TE administration. It is
concluded that: (1) injection of 200 mg TE/week causes a 15-20% decrease
in HDL-C in normal men with no effect on other lipoproteins, (2) the
suppressive effect of TE is maintained throughout the 1-year-injection
period, and a direct relationship between the duration of TE
administration and the proportion of men showing decreased HDL-C levels,
was observed. (3) The HDL-C decrease was reversible within 1 month of
stopping TE administration. These data will be important in designing
further studies on male contraception, and in interpreting the
relationship between testosterone levels, HDL-C levels and potential
cardiovascular risk.
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Citation
Int J Androl. 1995 Oct;18(5):237-42
