巴氯芬和苯环戊芬可调节大鼠大脑皮层和脊髓切片中γ-氨基丁酸（GABA）的释放，但对视网膜切片中的GABA释放无调节作用。

Baclofen and phaclofen modulate GABA release from slices of rat cerebral cortex and spinal cord but not from retina.

作者信息

Neal M J, Shah M A

机构信息

Department of Pharmacology, United Medical School of Guy's Hospital, London.

出版信息

Br J Pharmacol. 1989 Sep;98(1):105-12. doi: 10.1111/j.1476-5381.1989.tb16869.x.

DOI:10.1111/j.1476-5381.1989.tb16869.x

PMID:2804540

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1854689/

Abstract

The effects of (-)-baclofen, muscimol and phaclofen on endogenous gamma-aminobutyric acid (GABA) release from rat cortical slices, spinal cord slices and entire retinas were studied. 2. The spontaneous resting release of GABA from the three tissues was 3 to 6 pmol mg-1 wet wt 10 min-1. Depolarization of cortical slices with KCl (50 mM) (high-K) produced an 8 fold increase in GABA release but high-K did not evoke an increased release of GABA from spinal slices or retinas. 3. When rats were injected with gamma-vinyl-GABA (250 mg kg-1 i.p.) (GVG) 18 h before death, the tissue GABA stores were increased 3 to 6 fold and high-K then evoked striking Ca-dependent releases of GABA from all three tissues. Thus, in subsequent experiments, unless otherwise stated, the nervous tissues were taken from GVG-treated rats. 4. (-)-Baclofen (10 microM) significantly reduced the K-evoked release of GABA from cortical and spinal slices but retinal release was not affected, even at a concentration of (+/-)-baclofen of 1 mM. For cortical slices, the IC50 for baclofen was approximately 5.2 microM. The inhibitory effect of baclofen on GABA release from cortical slices also occurred in slices prepared from saline-injected rats, indicating that GVG treatment did not qualitatively affect the results. 5. The inhibitory effect of (-)-baclofen on the K-evoked release of GABA from cortical and spinal slices was antagonised by phaclofen (500 microM), confirming that baclofen was producing its effects by acting at the GABAB-receptor. 6. Phaclofen (500 microM) increased the spontaneous resting release of GABA from cortical slices taken from GVG-treated rats but not from saline-injected rats. Phaclofen did not increase GABA release from spinal slices or retinas taken from GVG-treated rats. 7. Baclofen (10 microM) significantly reduced the K-evoked release from cortical slices of glutamate, aspartate, glycine and taurine. 8. Muscimol (10 microM) and delta-aminolaevulinic acid (10 microM) had no effect on either the resting or Kevoked release of GABA from cortical slices prepared from saline-injected or GVG-treated rats. 9. The results obtained with cortical and spinal slices are consistent with the presence of inhibitory GABAB-autoreceptors. The phaclofen-induced increase in GABA release from cortical slices taken from GVG-treated rats, but not from saline-injected rats, implies that under conditions of high GABA release, considerable feedback inhibition is occurring via activation of the GABAB inhibitory autoreceptors. No evidence was found for GABAB-autoreceptors on retinal GABAergic amacrine cells or for GABAA-autoreceptors in cortical slices or spinal cord slices.

摘要

研究了(-)-巴氯芬、蝇蕈醇和苯氯芬对大鼠皮层切片、脊髓切片及整个视网膜内源性γ-氨基丁酸（GABA）释放的影响。2. 这三种组织中GABA的自发静息释放量为3至6 pmol mg-1湿重10分钟-1。用50 mM氯化钾（KCl）（高钾）使皮层切片去极化可使GABA释放增加8倍，但高钾并未引起脊髓切片或视网膜中GABA释放增加。3. 在大鼠死亡前18小时腹腔注射γ-乙烯基-GABA（250 mg kg-1）（GVG）后，组织GABA储备增加3至6倍，此时高钾可引起所有三种组织中显著的钙依赖性GABA释放。因此，在后续实验中，除非另有说明，神经组织均取自经GVG处理的大鼠。4. (-)-巴氯芬（10 μM）可显著降低高钾诱发的皮层和脊髓切片中GABA的释放，但即使在(±)-巴氯芬浓度为1 mM时，视网膜释放也不受影响。对于皮层切片，巴氯芬的IC50约为5.2 μM。巴氯芬对皮层切片中GABA释放的抑制作用在注射生理盐水的大鼠制备的切片中也存在，这表明GVG处理并未在质量上影响结果。5. 苯氯芬（500 μM）可拮抗(-)-巴氯芬对高钾诱发的皮层和脊髓切片中GABA释放的抑制作用，证实巴氯芬是通过作用于GABAB受体发挥其作用的。6. 苯氯芬（500 μM）可增加从经GVG处理的大鼠获取的皮层切片中GABA的自发静息释放，但不能增加从注射生理盐水的大鼠获取的皮层切片中GABA的自发静息释放。苯氯芬不能增加从经GVG处理的大鼠获取的脊髓切片或视网膜中GABA的释放。7. 巴氯芬（10 μM）可显著降低高钾诱发的皮层切片中谷氨酸、天冬氨酸、甘氨酸和牛磺酸的释放。8. 蝇蕈醇（10 μM）和δ-氨基乙酰丙酸（10 μM）对注射生理盐水或经GVG处理的大鼠制备的皮层切片中GABA的静息或高钾诱发释放均无影响。9. 皮层和脊髓切片的实验结果与抑制性GABAB自身受体的存在一致。苯氯芬诱导经GVG处理的大鼠获取的皮层切片中GABA释放增加，但注射生理盐水的大鼠获取的皮层切片中未增加，这意味着在高GABA释放条件下，通过GABAB抑制性自身受体的激活会发生相当程度的反馈抑制。未发现视网膜GABA能无长突细胞上存在GABAB自身受体，也未发现皮层切片或脊髓切片中存在GABAA自身受体。

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巴氯芬和苯环戊芬可调节大鼠大脑皮层和脊髓切片中γ-氨基丁酸（GABA）的释放，但对视网膜切片中的GABA释放无调节作用。

Baclofen and phaclofen modulate GABA release from slices of rat cerebral cortex and spinal cord but not from retina.

作者信息

Neal M J, Shah M A

机构信息

Department of Pharmacology, United Medical School of Guy's Hospital, London.

出版信息

Br J Pharmacol. 1989 Sep;98(1):105-12. doi: 10.1111/j.1476-5381.1989.tb16869.x.

DOI:10.1111/j.1476-5381.1989.tb16869.x

PMID:2804540

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1854689/

Abstract

The effects of (-)-baclofen, muscimol and phaclofen on endogenous gamma-aminobutyric acid (GABA) release from rat cortical slices, spinal cord slices and entire retinas were studied. 2. The spontaneous resting release of GABA from the three tissues was 3 to 6 pmol mg-1 wet wt 10 min-1. Depolarization of cortical slices with KCl (50 mM) (high-K) produced an 8 fold increase in GABA release but high-K did not evoke an increased release of GABA from spinal slices or retinas. 3. When rats were injected with gamma-vinyl-GABA (250 mg kg-1 i.p.) (GVG) 18 h before death, the tissue GABA stores were increased 3 to 6 fold and high-K then evoked striking Ca-dependent releases of GABA from all three tissues. Thus, in subsequent experiments, unless otherwise stated, the nervous tissues were taken from GVG-treated rats. 4. (-)-Baclofen (10 microM) significantly reduced the K-evoked release of GABA from cortical and spinal slices but retinal release was not affected, even at a concentration of (+/-)-baclofen of 1 mM. For cortical slices, the IC50 for baclofen was approximately 5.2 microM. The inhibitory effect of baclofen on GABA release from cortical slices also occurred in slices prepared from saline-injected rats, indicating that GVG treatment did not qualitatively affect the results. 5. The inhibitory effect of (-)-baclofen on the K-evoked release of GABA from cortical and spinal slices was antagonised by phaclofen (500 microM), confirming that baclofen was producing its effects by acting at the GABAB-receptor. 6. Phaclofen (500 microM) increased the spontaneous resting release of GABA from cortical slices taken from GVG-treated rats but not from saline-injected rats. Phaclofen did not increase GABA release from spinal slices or retinas taken from GVG-treated rats. 7. Baclofen (10 microM) significantly reduced the K-evoked release from cortical slices of glutamate, aspartate, glycine and taurine. 8. Muscimol (10 microM) and delta-aminolaevulinic acid (10 microM) had no effect on either the resting or Kevoked release of GABA from cortical slices prepared from saline-injected or GVG-treated rats. 9. The results obtained with cortical and spinal slices are consistent with the presence of inhibitory GABAB-autoreceptors. The phaclofen-induced increase in GABA release from cortical slices taken from GVG-treated rats, but not from saline-injected rats, implies that under conditions of high GABA release, considerable feedback inhibition is occurring via activation of the GABAB inhibitory autoreceptors. No evidence was found for GABAB-autoreceptors on retinal GABAergic amacrine cells or for GABAA-autoreceptors in cortical slices or spinal cord slices.

摘要

研究了(-)-巴氯芬、蝇蕈醇和苯氯芬对大鼠皮层切片、脊髓切片及整个视网膜内源性γ-氨基丁酸（GABA）释放的影响。2. 这三种组织中GABA的自发静息释放量为3至6 pmol mg-1湿重10分钟-1。用50 mM氯化钾（KCl）（高钾）使皮层切片去极化可使GABA释放增加8倍，但高钾并未引起脊髓切片或视网膜中GABA释放增加。3. 在大鼠死亡前18小时腹腔注射γ-乙烯基-GABA（250 mg kg-1）（GVG）后，组织GABA储备增加3至6倍，此时高钾可引起所有三种组织中显著的钙依赖性GABA释放。因此，在后续实验中，除非另有说明，神经组织均取自经GVG处理的大鼠。4. (-)-巴氯芬（10 μM）可显著降低高钾诱发的皮层和脊髓切片中GABA的释放，但即使在(±)-巴氯芬浓度为1 mM时，视网膜释放也不受影响。对于皮层切片，巴氯芬的IC50约为5.2 μM。巴氯芬对皮层切片中GABA释放的抑制作用在注射生理盐水的大鼠制备的切片中也存在，这表明GVG处理并未在质量上影响结果。5. 苯氯芬（500 μM）可拮抗(-)-巴氯芬对高钾诱发的皮层和脊髓切片中GABA释放的抑制作用，证实巴氯芬是通过作用于GABAB受体发挥其作用的。6. 苯氯芬（500 μM）可增加从经GVG处理的大鼠获取的皮层切片中GABA的自发静息释放，但不能增加从注射生理盐水的大鼠获取的皮层切片中GABA的自发静息释放。苯氯芬不能增加从经GVG处理的大鼠获取的脊髓切片或视网膜中GABA的释放。7. 巴氯芬（10 μM）可显著降低高钾诱发的皮层切片中谷氨酸、天冬氨酸、甘氨酸和牛磺酸的释放。8. 蝇蕈醇（10 μM）和δ-氨基乙酰丙酸（10 μM）对注射生理盐水或经GVG处理的大鼠制备的皮层切片中GABA的静息或高钾诱发释放均无影响。9. 皮层和脊髓切片的实验结果与抑制性GABAB自身受体的存在一致。苯氯芬诱导经GVG处理的大鼠获取的皮层切片中GABA释放增加，但注射生理盐水的大鼠获取的皮层切片中未增加，这意味着在高GABA释放条件下，通过GABAB抑制性自身受体的激活会发生相当程度的反馈抑制。未发现视网膜GABA能无长突细胞上存在GABAB自身受体，也未发现皮层切片或脊髓切片中存在GABAA自身受体。

巴氯芬和苯环戊芬可调节大鼠大脑皮层和脊髓切片中γ-氨基丁酸（GABA）的释放，但对视网膜切片中的GABA释放无调节作用。

Baclofen and phaclofen modulate GABA release from slices of rat cerebral cortex and spinal cord but not from retina.

作者信息

机构信息

出版信息

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引用本文的文献

本文引用的文献

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巴氯芬和苯环戊芬可调节大鼠大脑皮层和脊髓切片中γ-氨基丁酸（GABA）的释放，但对视网膜切片中的GABA释放无调节作用。

Baclofen and phaclofen modulate GABA release from slices of rat cerebral cortex and spinal cord but not from retina.

作者信息

机构信息

出版信息