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丙咪嗪、齐美利定和阿普氯胺亚慢性治疗对大鼠脑和脊髓中P物质及神经激肽A/神经激肽B样免疫反应性区域组织水平的影响。

Effects of subchronic treatment with imipramine, zimelidine and alaproclate on regional tissue levels of substance P- and neurokinin A/neurokinin B-like immunoreactivity in the brain and spinal cord of the rat.

作者信息

Brodin E, Ogren S O, Theodorsson-Norheim E

出版信息

Neuropharmacology. 1987 Jun;26(6):581-90. doi: 10.1016/0028-3908(87)90151-1.

Abstract

The effects of subchronic (14 day) treatment with the inhibitors at the uptake of monoamines, zimelidine, alaproclate and imipramine, on regional levels of substance P (SP) and other tachykinins in tissue in the central nervous system of the rat were studied by radioimmunoassay. In the ventral spinal cord, in which substance P is known to exist together with 5-hydroxytryptamine (5-HT), in the terminals of descending neurones, treatment with the selective inhibitors of the uptake of 5-HT zimelidine (2 X 10 mumol/kg p.o.) or alaproclate (2 X 10 mumol/kg or 2 X 20 mumol/kg p.o.), increased the level of substance P-like immunoreactivity (SP-LI). The effect of alaproclate appeared to be dose-dependent. After treatment with imipramine (2 X 10 mumol/kg p.o.) only a tendency to increased levels of substance P-like immunoreactivity spinal cord was seen. Treatment with alaproclate, at the highest dose level, also elevated the concentration of neurokinin A/neurokinin B-like immunoreactivity (NKA/NKB-LI) in the ventral spinal cord. In the frontal cortex, in which separate monoaminergic and tachykinin-containing neurones interact, treatment with imipramine reduced the levels of SP-LI and NKA/NKB-LI, while treatment with alaproclate had the opposite effect. In the periaqueductal grey matter, treatment with zimelidine and alaproclate increased the levels of SP-LI and NKA/NKB-LI, while treatment with imipramine increased only the level of NKA/NKB-LI. In conclusion, subchronic treatment of rats with inhibitors of the uptake of monoamines induced changes in levels of tachykinin in frontal cortex, periaqueductal grey and spinal cord. The selective inhibitors of the uptake zimelidine and alaproclate, had similar effects on levels of tachykinin, while the inhibitor of the uptake of 5-HT and noradrenaline, imipramine induced changes in the frontal cortex, which were qualitatively different from the effects of zimelidine and alaproclate. Furthermore, the levels of different tachykinins were not always changed in parallel by the same treatment.

摘要

采用放射免疫分析法研究了单胺摄取抑制剂齐美利定、阿普氯胺和丙咪嗪对大鼠中枢神经系统组织中P物质(SP)和其他速激肽区域水平的亚慢性(14天)治疗效果。在腹侧脊髓中,已知P物质与5-羟色胺(5-HT)共存于下行神经元的终末,用5-HT摄取的选择性抑制剂齐美利定(2×10 μmol/kg口服)或阿普氯胺(2×10 μmol/kg或2×20 μmol/kg口服)治疗,可增加P物质样免疫反应性(SP-LI)水平。阿普氯胺的作用似乎呈剂量依赖性。用丙咪嗪(2×10 μmol/kg口服)治疗后,仅观察到脊髓中P物质样免疫反应性水平有升高的趋势。以最高剂量水平的阿普氯胺治疗,也可提高腹侧脊髓中神经激肽A/神经激肽B样免疫反应性(NKA/NKB-LI)的浓度。在额叶皮质中,单胺能神经元和含速激肽的神经元相互作用,用丙咪嗪治疗可降低SP-LI和NKA/NKB-LI水平,而用阿普氯胺治疗则产生相反的效果。在导水管周围灰质中,用齐美利定和阿普氯胺治疗可增加SP-LI和NKA/NKB-LI水平,而用丙咪嗪治疗仅增加NKA/NKB-LI水平。总之,用单胺摄取抑制剂对大鼠进行亚慢性治疗可引起额叶皮质、导水管周围灰质和脊髓中速激肽水平的变化。摄取的选择性抑制剂齐美利定和阿普氯胺对速激肽水平有相似的影响,而5-HT和去甲肾上腺素摄取抑制剂丙咪嗪在额叶皮质中引起的变化在性质上与齐美利定和阿普氯胺的作用不同。此外,同一治疗并不总是使不同速激肽的水平平行变化。

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