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Vol. 296, Issue 1, 160-167, January 2001
1A-Adrenoceptor Subtype
Selectivity of KMD-3213 in Rat Tissues
Department of Biopharmacy, School of Pharmaceutical Sciences,
University of Shizuoka, Shizuoka, Japan
The present study was undertaken to characterize the in vivo
1-adrenoceptor binding of KMD-3213, a novel selective
antagonist of 1A-adrenoceptors, in rat tissues by using
a tritiated ligand with high specific activity, in comparison with that
of [3H]prazosin. A significant degree of in vivo specific
binding of [3H]KMD-3213 after i.v. injection of the
radioligand (1.4 nmol/kg) was seen in most rat tissues, except the
cerebral cortex, spleen, and liver, which showed a little or no
specific binding. There was a notable difference among tissues in the
time course of specific [3H]KMD-3213 binding after i.v.
injection of the ligand. The specific binding in the lung, kidney, and
spleen was greatest at 10 min and declined rapidly with the
disappearance of the ligand from the plasma. On the other hand,
[3H]KMD-3213 binding in the submaxillary gland, vas
deferens, and prostate attained peak levels at 60 min, and a
considerable degree of binding was present even at 240 min. After i.v.
injection of a similar dose (1.2 nmol/kg) of [3H]prazosin
in rats, the in vivo specific binding in the submaxillary gland was
greatest at 10 min and then it fell rapidly, whereas [3H]prazosin binding in the spleen attained a peak level
at 60 min, and this was maintained even at 120 min. The
AUC0-120 values of the specific binding for
[3H]KMD-3213, compared with those of
[3H]prazosin, were markedly lower in the rat aorta,
spleen, and liver, whereas the prostate, submaxillary gland, and lung
showed significantly higher AUC0-120 values of
[3H]KMD-3213 compared with [3H]prazosin.
Furthermore, the in vivo specific binding of [3H]KMD-3213
at dose ranges of 1.4 to 13.6 nmol/kg increased linearly in the
prostate and submaxillary gland, but did not increase in a
dose-dependent manner in the spleen. On the other hand, there was a
dose-dependent increase in the in vivo specific binding of
[3H]prazosin at doses of 1.2 to 10.6 nmol/kg in all
tissues. The in vivo specific binding of [3H]KMD-3213 in
rat tissues was reduced by concomitant i.v. injection of low doses of
prazosin in a dose-dependent manner, but not by even a relatively high
dose of yohimbine. In conclusion, the present study shows that KMD-3213
binds to the 1A-adrenoceptor subtype with a higher
affinity than to the 1B- and 1D- subtypes
under in vivo condition, thus leading to prostate selectivity.
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