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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Preferential blockade of cholecystokinin-8S-induced increases in aspartate and glutamate levels by the CCK(B) receptor antagonist, L-365,260, in rat brain.
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Preferential blockade of cholecystokinin-8S-induced increases in aspartate and glutamate levels by the CCK(B) receptor antagonist, L-365,260, in rat brain.

机译:CCK(B)受体拮抗剂L-365,260对大鼠脑中胆囊收缩素8S诱导的天冬氨酸和谷氨酸水平的优先阻断。

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摘要

In the present studies, the ability of a locally delivered cholecystokinin (CCK) receptor agonist and systemically delivered antagonists to modulate extracellular levels of aspartate and glutamate in the frontal cortex of anaesthetised rats and frontal cortex and caudate-putamen of freely moving rats was investigated using an in vivo microdialysis technique. In the anaesthetised rats, local application of sulphated CCK octapeptide (CCK-8S, 10 microM) into the frontal cortex enhanced extracellular aspartate levels to a maximum of 265+/-16% of the basal levels, whereas glutamate levels were increased to a maximum of 168+/-7% of the basal levels. Given 40 min prior to the cortical perfusion of 10 microM of CCK-8S, the CCK(B) receptor antagonist, L-365,260 (20 mg/kg, s.c.), limited the rise in cortical aspartate by over half to 170+/-10% of the basal levels. However, this same dose of L-365,260 still allowed CCK-8S to increase glutamate by 44+/-15% above the basal levels. Whereas the enhanced glutamate levels were totally unaffected by systemic administration of the CCK(A) receptor antagonist, L-364,718 (20 mg/kg, -40 min, s.c.), this treatment was able to limit the elevation in aspartate to 220+/-4% of the basal levels. In the freely moving rats, local perfusion of CCK-8S (10 microM) increased aspartate and glutamate levels to maxima of 275+/-12% and 225+/-14% of the basal levels, respectively, in the frontal cortex. In the caudate-putamen, aspartate and glutamate levels were also elevated by CCK-8S (10 microM) to 248+/-15% and 185+/-12% of the basal levels, respectively. The respective increase in aspartate and glutamate induced by CCK-8S (10 microM) were limited to 140+/-10% and 124+/-6% (frontal cortex), of the basal levels, and 162+/-15% and 143+/-8% (caudate-putamen), by 40 min pretreatment with L-365,260 (20 mg/kg, s.c.). In conclusion, CCK-8S was able to enhance both aspartate and glutamate overflow in the frontal cortex of anaesthetised rats, and frontal cortex and caudate-putamen of freely moving rats. These increases were preferentially offset by the selective CCK(B) receptor antagonist, L-365,260, since no influence could be discerned using the selective CCK(A) receptor antagonist, L-364,718.
机译:在本研究中,研究了局部递送的胆囊收缩素(CCK)受体激动剂和全身递送的拮抗剂调节麻醉大鼠额叶皮质和自由移动大鼠的额叶皮质和尾状囊膜中细胞外天冬氨酸和谷氨酸水平的能力。体内微透析技术。在麻醉的大鼠中,将硫酸化的CCK八肽(CCK-8S,10 microM)局部应用到额叶皮层中,可将细胞外天冬氨酸水平提高到基础水平的最大265 +/- 16%,而谷氨酸水平增加到最大是基础水平的168 +/- 7%。在皮层灌注10 microM CCK-8S之前40分钟,CCK(B)受体拮抗剂L-365,260(20 mg / kg,sc)将皮层天冬氨酸的升高限制了一半以上,达到170 +/-基础水平的10%。但是,同样剂量的L-365,260仍使CCK-8S的谷氨酸水平比基础水平高出44 +/- 15%。虽然全身性施用CCK(A)受体拮抗剂L-364,718(20 mg / kg,-40 min,sc)完全不影响谷氨酸水平的升高,但这种治疗能够将天冬氨酸的升高限制在220 + / -4%的基础水平。在自由运动的大鼠中,CCK-8S(10 microM)的局部灌注使额叶皮层中的天冬氨酸和谷氨酸水平分别增加至最大基础水平的275 +/- 12%和225 +/- 14%。在尾状丘脑中,天冬氨酸和谷氨酸水平也被CCK-8S(10 microM)升高至基础水平的248 +/- 15%和185 +/- 12%。 CCK-8S(10 microM)引起的天冬氨酸和谷氨酸的相应增加被限制在基础水平的140 +/- 10%和124 +/- 6%(额叶皮层),而162 +/- 15%和用L-365,260(20 mg / kg,sc)预处理40分钟后为143 +/- 8%(尾状-丘脑)。总之,CCK-8S能够增强麻醉大鼠额叶皮层以及自由移动大鼠额叶皮层和尾状壳-天门冬氨酸和谷氨酸的溢出。这些增加优先被选择性CCK(B)受体拮抗剂L-365,260抵消,因为使用选择性CCK(A)受体拮抗剂L-364,718无法识别影响。

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