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Comparative effects of neonatal exposure of male rats to potent and weak (environmental) estrogens on spermatogenesis at puberty and the relationship to adult testis size and fertility: evidence for stimulatory effects of low estrogen levels.
- Atanassova N, McKinnell C, Turner KJ, Walker M, Fisher JS, Morley M, Millar MR, Groome NP, Sharpe RM
Endocrinology. 2000 Oct;141(10):3898-907.
This study investigated whether neonatal
exposure of male rats to estrogenic compounds altered pubertal spermatogenesis
(days 18 and 25) and whether the changes observed resulted in long-term changes in testis
size, mating, or fertility (days 90-100). Rats were treated neonatally with a range of doses (0.01-10 microg) of diethylstilbestrol
(DES; administered on alternate days from days 2-12), a high dose of octylphenol (OP; 2 mg
administered daily from days 2-12) or bisphenol A (Bis-A; 0.5 mg
administered daily from days 2-12), or vehicle,
while maintained on a standard soy-containing diet.
The effect on the same parameters of rearing control
animals on a soy-free diet
was also assessed as was the effect of administering such animals genistein
(4 mg/kg/day daily from days 2-18). Testis
weight, seminiferous tubule
lumen
formation, the germ cell
apoptotic index (apoptotic/viable germ cell
nuclear
volume), and spermatocyte
nuclear
volume per unit
Sertoli cell
nuclear
volume were used to characterize pubertal spermatogenesis.
Compared with (soy-fed) controls, DES administration
caused dose-dependent retardation of pubertal spermatogenesis
on day 18, as evidenced by decreases in testis
weight, lumen
formation, and spermatocyte
nuclear
volume per unit
Sertoli cell
and elevation of the germ cell
apoptotic index. However, the two lowest doses of DES (0.1 and 0.01 microg) significantly increased spermatocyte
nuclear
volume per unit
Sertoli cell.
Similarly, treatment with either OP or Bis-A significantly advanced this and some of the other aspects of pubertal spermatogenesis.
Maintenance
of control
animals on a soy-free diet
also significantly advanced lumen
formation and spermatocyte
nuclear
volume per unit
Sertoli cell
compared with controls fed a soy-containing diet.
Administration
of genistein
reversed the stimulatory effects of a soy-free diet
and significantly retarded most measures of pubertal spermatogenesis.
In general, plasma
FSH
levels in the treatment groups changed in parallel to the spermatogenic changes (reduced when pubertal spermatogenesis
retarded, increased when pubertal spermatogenesis
advanced). By day 25, although the changes in FSH
levels largely persisted, all
of the stimulatory effects on spermatogenesis
seen on day 18 in the various treatment groups were no longer evident. In adulthood, testis
weight was decreased dose dependently in rats treated neonatally with DES, but only the lowest dose group (0.01 microg) showed evidence of mating (3 of 6) and normal fertility (3 litters). Animals treated neonatally with OP or Bis-A had normal or increased (Bis-A) testis
weights and exhibited reasonably normal mating/fertility. Animals fed a soy-free diet
had significantly larger testes than controls fed a soy-containing diet,
and this difference was confirmed in a much larger study of more than 24 litters, which also showed a significant decrease in plasma
FSH
levels and a significant increase in body weight in the males kept on a soy-free diet.
Neonatal
treatment with genistein
did not alter adult testis
weight, and although most males exhibited normal mating and fertility, a minority did not mate
or were infertile. It is concluded that 1) neonatal
exposure of rats to low levels of estrogens
can advance the first wave of spermatogenesis
at puberty,
although it is unclear whether this is due to direct effects of the estrogen
or to associated elevation of FSH
levels; 2) the effect of high doses of OP and Bis-A on these processes is essentially benign;
and 3) the presence or absence of soy
or genistein
in the diet
has significant short-term (pubertal spermatogenesis)
and long-term (body weight, testis
size, FSH
levels, and possibly mating) effects on males.
This abstract at PubMed.