1) Urethane 마취가토(痲醉家兎)의 내뇌(腦內)(측뇌실(刻腦室) 또는 소뇌연수조내(小腦延髓槽內)에 norepinephrine (NE), clonidine을 주입(注入)할 때 일어나는 심박감소(心搏減少), 혈압하강(血壓下降)에 관한 이들 약물(藥物)의 작용점(作用點)을 조사(調査)할 것을 시도(試圖)하였다. 2) NE의 뇌내주입(腦內注入)은 심박감소(心搏減少)를 일으켰으나 혈압(血壓)에 미치는 영향(影響)은 뚜렷치 않았다. Clonidine은 심박감소(心搏減少), 혈압하강(血壓下降)을 일으켰다. 3) 측뇌실내주입(刻腦室內注入) 소뇌연수조내주입간(小腦延髓槽內注入間)에는 NE, clonidine, phenylephrine, isoproterenol의 심박(心搏), 혈압효과(血壓效果)에 차이(差異)가 없었다. 또 NE에 의한 심박감소효과(心搏減少效果)의 출현(出現)은 소뇌연수조내주입시(小腦延髓槽內注入時) 더 빨랐다. 4) 약(約) 2시간(時間) 간격(間隔)으로 NE를 반복(反復) 주입(注入)할 때 심박효과(心搏效果)에는 거의 변동(變動)이 없었으나 혈압효과(血壓效果)는 반복주입(反復注入)함에 따라 혈압상승효과(血壓上昇效果)가 현저(顯著)히 나타났다. Clonidine의 심박감소(心搏減少) 및 혈압하강효과(血壓下降效果)는 반복주입(反復注入)에 따라 점차 약화(弱化)되었다. 5) NE 주입후(注入後) NE 효과(效果)가 지속(持續)하고 있을 때 clonidine은 더 이상(以上)의 심박감소(心搏減少)를 일으키지 않고, 혈압하강(血壓下降)도 일으키지 않았다. Clonidine 주입후(注入後) clonidine 효과(效果)가 지속(持續)하고 있을 때 NE는 더 이상(以上)의 심박감소(心搏減少)를 일으키지 않았고 현저(顯著)한 혈압상승(血壓上昇)을 일으켰다. 6) Regitine 또는 desmethylimipramine의 뇌내주입후(腦內注入後) NE는 심박(心搏)에 거의 변동(變動)을 일으키지 않았으나 현저(顯著)한 혈압상승(血壓上昇)을 일으켰다. Clonidine은 심박(心搏), 혈압(血壓)에 거의 변동(變動)을 일으키지 않았다. 7) Reserpine 처리가토(處理家兎)에서는 NE는 심박증가(心搏增加)와 혈압상승(血壓上昇)을 일으켰으며, clonidine은 심박(心搏)에는 거의 변동(變動)을 일으키지 않았고 경미(輕微)한 혈압상승(血壓上昇)을 일으켰다. 8) NE 및 clonidine에 의한 심박감소(心搏減少), clonidine에 의한 혈압하강(血壓下降)은 주(主)로 presynaptic α-adrenoceptor를 중개(仲介)하여 일어나나, NE 및 clonidine에 의한 혈압상승(血壓上昇)은 presynaptic site 이외(以外)의 부위(部位)를 중개(仲介)하여 일어나는것 같다.
1) It was attempted to clarify the sites of action of central (either intraventricular or intracisternal) norepinephrine(NE) and clonidine to cause cardiac slowing and hypotension in urethane-anesthetized rabbits. 2) NE produced cardiac slowing but indistinct effect on blood pressure. Clonidine produced cardiac slowing and hypotension. 3) Intraventricular and intracisternal administration of NE, clonidine, phenylephrine and isoproterenol did not make difference in their effects, except that the onset of cardiac slowing by intracisternal NE was more rapid than intraventricular NE. 4) Upon repeated administration of NE at the intervals of about two hours, blood pressure responses changed to the pressor ones, the cardiac slowing unchanged. By this procedure the cardiac slowing as well as the hypotension by clonidine were gradually diminished. 5) Clonidine, when given during the NE effects were persisting, did not produce the lowering of blood pressure and further decrease of heart rate. NE, when given during the clonidine effects were persisting, produced marked elevation of blood pressure but did not produce further decrease of heart rate. 6) After intraventricular administration of regitine or desmethylimipramine, the cardiac slowing effect of NE and the clonidine effects were not observed, whereas NE produced marked elevation of blood pressure. 7) Reserpinized rabbits showed pressor and cardiac accelerating responses to NE; slight pressor, and little cardiac responses to clonidine. 8) It seems that the cardiac slowing by both clonidine and NE as well as the hypotetsion by clonidine are mediated by the presynaptic α-adrenoceptor in the brain but the pressor responses to NE and clonidine are mediated by other site(s) than the presynaptic ones. 1) It was attempted to clarify the sites of action of central (either intraventricular or intracisternal) norepinephrine(NE) and clonidine to cause cardiac slowing and hypotension in urethane-anesthetized rabbits. 2) NE produced cardiac slowing but indistinct effect on blood pressure. Clonidine produced cardiac slowing and hypotension. 3) Intraventricular and intracisternal administration of NE, clonidine, phenylephrine and isoproterenol did not make difference in their effects, except that the onset of cardiac slowing by intracisternal NE was more rapid than intraventricular NE. 4) Upon repeated administration of NE at the intervals of about two hours, blood pressure responses changed to the pressor ones, the cardiac slowing unchanged. By this procedure the cardiac slowing as well as the hypotension by clonidine were gradually diminished. 5) Clonidine, when given during the NE effects were persisting, did not produce the lowering of blood pressure and further decrease of heart rate. NE, when given during the clonidine effects were persisting, produced marked elevation of blood pressure but did not produce further decrease of heart rate. 6) After intraventricular administration of regitine or desmethylimipramine, the cardiac slowing effect of NE and the clonidine effects were not observed, whereas NE produced marked elevation of blood pressure. 7) Reserpinized rabbits showed pressor and cardiac accelerating responses to NE; slight pressor, and little cardiac responses to clonidine. 8) It seems that the cardiac slowing by both clonidine and NE as well as the hypotetsion by clonidine are mediated by the presynaptic α-adrenoceptor in the brain but the pressor responses to NE and clonidine are mediated by other site(s) than the presynaptic ones.
