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P物质从猫脊髓的释放。

Release of substance P from the cat spinal cord.

作者信息

Go V L, Yaksh T L

机构信息

Division of Gastroenterology, Mayo Clinic, Rochester, MN 55905.

出版信息

J Physiol. 1987 Oct;391:141-67. doi: 10.1113/jphysiol.1987.sp016731.

Abstract
  1. The present experiments examine the physiology and pharmacology of the release of substance P-like immunoreactivity (SP-l.i.), from the spinal cord in the halothane-anaesthetized, artificially ventilated cat. 2. Resting release of SP-l.i. was 36 +/- 4 fmol/30 min (mean +/- S.E.; n = 106). Bilateral stimulation of the sciatic nerves at intensities which evoked activity in fibres conducting at A beta conduction velocities (greater than 40 m/s), resulted in no change in blood pressure, pupil diameter or release of SP-l.i. Stimulation intensities which activate fibres conducting at velocities less than 2 m/s resulted in increased blood pressure, miosis and elevated release of SP-l.i. (278 +/- 16% of control). 3. The relationship between nerve-stimulation frequency and release was monotonic up to approximately 20 Hz. Higher stimulation frequencies did not increase the amounts of SP-l.i. released. At 200 Hz there was a reduction. 4. Capsaicin (0.1 mM) increased the release of SP-l.i. from the spinal cord and resulted in an acute desensitization to subsequent nerve stimulation. This acute effect was not accompanied by a reduction in spinal levels of SP-l.i. measured 2 h after stimulation. 5. Cold block of the cervical spinal cord resulted in an increase in the amounts of SP-l.i. released by nerve stimulation. 6. Pre-treatment with intrathecal 5,6-dihydroxytryptamine (300 micrograms) 7 days prior to the experiment caused a reduction in the dorsal and ventral horn stores of SP-l.i., but had no effect on the release of SP-l.i. evoked by nerve stimulation. Similar pre-treatment with intrathecal capsaicin (300 micrograms) resulted in depletion of SP-l.i. in the dorsal but not in the ventral horn of the spinal cord and diminished the release of SP-l.i. evoked by nerve stimulation. 7. Intense thermal stimulation of the flank resulted in small (20-35%), but reliable increases in the release of SP-l.i. above control. 8. Putative agonists for the opioid mu-receptor (morphine, 10-100 microM; sufentanil, 1 microM), and for the delta-receptor (D-Ala2-D-Leu5-enkephalin, 1-10 microM; D-Pen2-D-Pen5-enkephalin, 10 microM), but not the kappa-receptor (U50488H, 100-1000 microM), produced a dose-dependent, naloxone-reversible reduction of the evoked, but not of the resting release of SP-l.i. (-)-Naloxone, but not (+)-naloxone, resulted in a significant increase in evoked but not resting SP-l.i. release.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 本实验研究了在氟烷麻醉、人工通气的猫中,脊髓释放P物质样免疫反应性物质(SP-l.i.)的生理学和药理学特性。2. SP-l.i.的基础释放量为36±4飞摩尔/30分钟(平均值±标准误;n = 106)。以能引起Aβ传导速度(大于40米/秒)的纤维兴奋的强度双侧刺激坐骨神经,血压、瞳孔直径或SP-l.i.的释放均无变化。刺激强度激活传导速度小于2米/秒的纤维会导致血压升高、瞳孔缩小以及SP-l.i.释放增加(为对照值的278±16%)。3. 直至约20赫兹,神经刺激频率与释放之间的关系呈单调变化。更高的刺激频率不会增加SP-l.i.的释放量。在200赫兹时释放量减少。4. 辣椒素(0.1毫摩尔)增加了脊髓中SP-l.i.的释放,并导致对后续神经刺激的急性脱敏。这种急性效应在刺激后2小时测量时,并未伴有脊髓中SP-l.i.水平的降低。5. 颈脊髓的冷阻断导致神经刺激引起的SP-l.i.释放量增加。6. 在实验前7天鞘内注射5,6-二羟基色胺(300微克)预处理,导致脊髓背角和腹角中SP-l.i.的储存量减少,但对神经刺激引起的SP-l.i.释放没有影响。类似地,鞘内注射辣椒素(300微克)预处理导致脊髓背角而非腹角中的SP-l.i.耗竭,并减少了神经刺激引起的SP-l.i.释放。7. 对侧腹进行强烈热刺激导致SP-l.i.释放量比对照值有小幅度(20 - 35%)但可靠的增加。8. 阿片μ受体的假定激动剂(吗啡,10 - 100微摩尔;舒芬太尼,1微摩尔)以及δ受体的假定激动剂(D-Ala2-D-Leu5-脑啡肽,1 - 10微摩尔;D-Pen2-D-Pen5-脑啡肽,10微摩尔),但κ受体的假定激动剂(U50488H,100 - 1000微摩尔)除外,产生了剂量依赖性、纳洛酮可逆的诱发SP-l.i.释放的减少,但对基础释放无影响。(-)-纳洛酮而非(+)-纳洛酮导致诱发的而非基础的SP-l.i.释放显著增加。(摘要截短至400字)

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