Alterations in the potassium-evoked release of substance P from the spinal cord of streptozotocin-induced diabetic rats in vitro.

J Kamei, Y Ogawa, Y Ohhashi, Y Kasuya
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引用次数: 15

Abstract

1. The release of SPLI evoked by high levels of K+ (50 mM) from the spinal cord of diabetic rats was greater than in the case of spinal cord from control rats. 2. Morphine (10(-5) M) significantly inhibited the K(+)-evoked release of SPLI release in both the groups. However, in spinal cord from diabetic rats, morphine reduced the K(+)-evoked release of SPLI only to the levels that were observed in material from control rats prior to treatment with morphine. 3. Glucose (20 mM) and dibutyryl cyclic-AMP (10(-4) M) significantly potentiated the K(+)-evoked release of SPLI in spinal cord from control rats. 4. These findings suggest that excessive release of SPLI from the spinal cord may be associated with the reported abnormalities in nociceptive transmission in diabetic rats, and that excessive release of SPLI may be modulated by levels of glucose and/or cyclic-AMP in the spinal cord.

链脲佐菌素诱导的糖尿病大鼠脊髓钾诱导P物质释放的变化。
1. 高水平K+ (50 mM)诱导的SPLI在糖尿病大鼠脊髓中的释放量高于对照大鼠。2. 吗啡(10(-5)M)显著抑制K(+)诱导的SPLI释放。然而,在糖尿病大鼠的脊髓中,吗啡仅将K(+)诱发的SPLI释放降低到与吗啡治疗前对照大鼠材料中观察到的水平。3.葡萄糖(20 mM)和二丁基环amp (10(-4) M)显著增强K(+)诱发的脊髓SPLI释放。4. 这些发现表明,脊髓中SPLI的过度释放可能与糖尿病大鼠的伤害性传递异常有关,并且SPLI的过度释放可能受到脊髓中葡萄糖和/或循环amp水平的调节。
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