GABA和苦毒素等药物对螽斯听觉中间神经元AN2声反应特征的影响

利用单细胞电生理记录技术,观测了在前胸施加ＧＡＢＡ、苦毒素和筒箭毒等药物对螽斯Ｇａｍｐｏｃｌｅｉｓｇｒａｔｉｏｓａ听觉上升神经元ＡＮ２的声反应放电活动的影响。发现ＧＡＢＡ和筒箭毒都能抑制ＡＮ２的放电活动,而苦毒素则将其放电模式变为“ｔｏｎｉｃ”型。     

大鼠尾核微量注射γ—氨基丁酸对尾核痛反应神经元放电的影响

在５３只成年Ｗｉｓｔａｒ大鼠上,用玻璃微电极引导神经元放电,观察了尾核内注射γ－氨基丁酸后,尾核痛反应经元放电的变化和印防己毒素对ＧＡＢＡ作用的阻断效应。尾核内每２分钟分别注射ＧＡＢＡ２５,５０,１００μｇ／２μｌ,尾核痛兴奋神经元诱发放电频率减少,潜伏期延长;痛抑制神经元放诱发放电频率减少,潜伏期延长;痛抑制神经元放电抑制时程缩短,放电频率增加。ＰＥＮ和ＰＩＮ电活动反应与ＧＡＢＡ剂量间呈量效关系     

GABA参与兔杏仁体抑制内膝体神经元电活动

本文采用多管微电极胞外记录技术观察了短纯音引起兔内膝神经元的声反应及刺激杏仁体对声反应的影响,并在此基础上观察电泳ＧＡＢＡ及其拮抗剂Ｂｉｃｕｃｕｌｌｉｎｅ的效应。实验结果表明：ＧＡＢＡ可以抑制ＭＧＢ神经元的声反应及自发放电活动,而ＧＡＢＡＡ拮抗剂Ｂｉｃｕｃｕｌｌｉｎｅ的作用则相反;电泳ＧＡＢＡ对ＭＧＢ神经元产生同刺激杏仁体一样的抑制产应,并且这种影响可被Ｂｉｃｕｃｕｌｌｉｎｅ翻转;嗅鼻沟后缘听区农     

鲫鱼视网膜谷氨酸受体和GABA受体在爪蟾卵母细胞中的表达

我们以两栖类卵母细胞为功能表达系统,通过注射鲫鱼（Ｃａｒａｓｓｉｕｓｃａｒａｓｓｉｕｓ）视网膜ｍＲＮＡ,利用电压箝及药物灌流手段,系统地研究了鲫鱼视网膜内氨基酸受体的类型和特征,结果如下：（１）Ｇｌｕ受体：ＫＡ可以诱发明显的去极化电流,而且Ｄｉａｚｏｘｉｄｅ能增强ＫＡ诱导的反应,这提示鲫鱼视网膜内某些Ｃｌｕ受体是ＡＭＰＡ选择性亚型（ＡＭＰＡ－ｐｒｅｆｅｒｒｉｎｇｓｕｂｔｙｐｅ）。（２）ＣＡＢＡ受体：ＧＡＢＡ能诱发一个快速、光滑的内向电流,绝大部分对ＧＡＢＡ的反应可被ｂｉｃｕｃｕｌｌｉｎｅ所压抑,而ＧＡＢＡ＿Ｂ受体的激动剂ｂａｃｌｏｆｅｎ则无任何作用,这提示,鲫鱼视网膜内大部分是ＧＡＢＡ＿Ａ受体。     

GABAc受体及其功能特性

ＧＡＢＡｃ受体是近年来发现的新ＧＡＢＡ的受体，由ρ１或／和ρ２亚单位组成，基因突变研究显示，ρ１亚单位第二跨膜区３０９（人）或３１４（大鼠）位点上的氨基酸决定其对印防己毒素的敏感性，实验已证明：Ｚｎ＾２＋主要通过胞外机制阻断ＧＡＢＡｃ受体，谷氨酸，多巴胺则通过胞内ＰＫＡ和／或ＰＫＣ环路调制ＧＡＢＡｃ受体的活动，ＧＡＢＡｃ受体在视觉通路中特别丰富，已证明在视网膜的信息传递和调控中起重要作用。     

与人类原癌基因TTG同源的果蝇ttg基因克隆与分析

人类Ｔ淋巴细胞白血病基因家族（Ｔｃｅｌｌｔｒａｎｓｌｏｃａｔｉｏｎｇｅｎｅ,简称ＴＴＧ或Ｒｈｏｍｂｏｔｉｎ简称ＲＢＴＮ）是一个肿瘤基因家族,包括有３个基因,ＴＴＧ－１／ＲＢＴＮ－１,ＴＴＧ－２／ＲＢＴＮ－２,ＴＴＧ－３／ＲＢＴＮ－３,其中ＴＴＧ－１和ＴＴＧ－２是分别在二个具有不同染色休易位的Ｔ淋巴细胞白血病人中克隆到的,这个基因家族共同含有一个ＬＩＭ结构,这个ＬＩＭ结构编码一个二次重复出现的富含半     

THINOPYRUM BESSARABICUM和THINOPYRUM ELONGATUM的基 …

对２个八倍体Ｃ．Ｓ－Ｔｈｉｎｏｐｙｒｕｍ ｂｅｓｓａｒａｂｉｃｕｍ（ＡＡＢＢＤＤＪＪ,２ｎ＝８ｘ＝５６）和Ｇｏｓｈａｗｋ（ＧＨＫ）－Ｔｈｉｎｏｐｙｒｕｍ ｅｌｏｎｇａｔｕｍ（ＡＡＢＢＤＤＥＥ,２ｎ＝８ｘ＝５６）的根尖细胞染色体进行Ｃ－分带,从中分检出Ｔｈ．ｂｅｓｓａｒａｂｉｃｕｍ和Ｔｈ．ｅｌｏｎｇａｔｕｍ的各自染色体进行核型分析,结果表明：Ｔｈ．ｂｅｓｓａｒａｂｉｃｕｍ和Ｔｈ．ｅｌｏｎｇａｔｕｍ的     

王不留行环肽研究

从中药王不留行（Ｖａｃａｒｉａｓｅｇｅｔａｌｉｓ）种子中分离并鉴定了４个环肽化合物,分别命名为王不留行环肽Ａ,Ｂ,Ｃ,Ｄ（ｖａｃｃａｒｉｎｓＡ,Ｂ,Ｃ,Ｄ）,其中王不留行环肽Ａ为新环肽化合物。其结构通过光谱和化学方法分别确定为：ｖａｃｃａｒｉｎＡ——ｃｙｃｌｏ－（Ｔｒｐ－Ａｌａ１－Ｇｌｙ－Ｖａｌ－Ａｌａ２）,ｖａｃｃａｒｉｎＢ———ｃｙｃｌｏ－（Ｐｒｏ－Ｇｌｙ－Ｌｅｕ－Ｓｅｒ－Ｐｈｅ１－Ａｌａ－Ｐｈｅ２）,ｖａｃｃａｒｉｎＣ———ｃｙｃｌｏ－（Ｐｒｏ１－Ｇｌｙ－Ｔｙｒ－Ｖａｌ－Ｐｒｏ２－Ｌｅｕ－Ｔｒｐ）,ｖａｃａｒｉｎＤ———ｃｙｃｌｏ－（Ｐｒｏ－Ｖａｌ１－Ｔｒｐ－Ａｌａ－Ｇｌｙ－Ｖａｌ２）．     

微电泳GABA和5－HT对大鼠丘脑束旁核单位痛放电的影响

本实验用多管微电极细胞外记录和离子微电泳方法,在水含氯醛麻醉的ＳＤ大鼠上观察了γ－氨基丁酸（ＧＡＢＡ）和５－羟色胺（５－ＨＴ）以及它们的受体阻断剂（印防已毒素和赛庚啶）对丘脑束旁核（Ｐｆ）单位痛放电的影响。结果表明：（１）电泳ＧＡＢＡ可抑制Ｐｆ神经元的痛放电,这作用可被电泳印防已毒素所阻断,而单独电泳印防己毒素可加强Ｐｆ的痛放电。（２）电泳５－ＨＴ对Ｐｆ单位痛放电在有些单位表现加强作用,另一些单位表现抑制作用,仅前者可被电泳赛庚啶所阻断。上述结果提示：在Ｐｆ神经元的痛放电活动中,ＧＡＢＡ可能起抑制性作用,而５－ＨＴ可能通过不同的受体亚型既发挥其兴奋作用,也可有抑制作用。     

重庆地区“双千田”组合模式及效益分析

重庆地区“双千田”组合模式及效益分析郑钦玉,朱自均,胡声荣,袁可（西南农业大学,重庆６３０７１６）雷炎,李登国,程世宇,温永学,刘官堂（四川省巴县农业局）ＣｏｍｂｉｎａｔｉｏｎＭｏｄｅｌｓｏｆ＂ＴｏｎＧｒａｉｎＹｉｅｌｄｉｎｇＦｉｅｌｄ＂ｉｎＣｈｏｎｇｑｉｎｇＡｒｅａａｎｄＴｋｅｉｒＢｅｎｅｆｉｔＡｎａｌｙｓｉｓ￥．ＺｈｅｎｇＱｉｎｙｕ;ＺｈｕＺｈｉｊｕｎ;ＨｕＳｈｅｎｇｒｏｎｇ;ＹｕａｎＫｅ（ＳｏｕｔｈｗｅｓｔＡｇｒｉｃｕｌｔｕｒａｌＵｎｉｖｅｒｓｉｔｙ,Ｃｈｏｎｇｑｉｎｇ６３０７１６）,ＬｅｉＹａｎ,ＬｉＤｅｎｇｇｕｏ,ＣｈｅｎｇＳｈｉｙｕ,ＷｅｎＹｏｎｇｘｕｅ,ＬｉｕＧｕａｎｔａｎｇ（ＢａｘｉａｎＢｕｒｅａｕｏｆＡｇｒｉｃｕｌｔｕｒｅ,ＳｉｃｈｕａｎＰｒｏｖｉｎｃｅ）．ＣｈｉｎｅｓｅＪｏｕｍａｌｏｆＥｃｏｌｅｇｙ,１９９３,１２（２）：３４—３６．Ｉｎｔｈｅｌｉｇｈｔｏｆｔｈｅｅｆｆｅｃｔｓａｎｄｐｒｏｂｌｅｍｓｏｆｄｅｖｅｌｏｐｉｎｇｗｉｎｔｅｒ－ｃｒｏｐｐｉｎｇｐａｄｄｙｆｉｅｌｄｓｉｎＣｈｏｎｇｑｉｎｇａｒｅａａｎｄｉｎｏｒｄｅｒｔｏｓｅａｒｃｈａｆｔｅｒｔｈｅｏｐｔｉｍｕｍｍｏｄｅｌｏｆｒｅｆ     

蜚蠊单个棘—钟形感器冲动发放的特性

本文分析了蜚镰后胸足单个棘一钟形感器对机械位移刺激的反应模式以及冲动发放的特性.结果证明该感器是一种适应较慢的相位性触觉感受器,对触刺激有相当稳定的反应.     

安定减低家兔膈神经放电幅度的机制分析

本实验室曾经报道静脉注射安定对于清醒、麻痹、人工呼吸的家兔具有减低膈神经放电幅度、加快呼吸频率,缩短吸气时程(T_I)和呼气时程(T_E),降低动脉血压等作用。本工作在35只家兔中进一步分析了某些药物对安定的这些作用的影响。GABA 降低膈神经放电幅度和动脉血压,这与安定的作用相同,但 GABA 延长T_I、T_E和减慢呼吸频率,与安定的作用相反。事先用氨基酸脱羧酶抑制剂异烟肼处理,或用 GABA 受体拮抗剂印防己毒素处理,可阻遏安定减低膈神经放电幅度的作用。在事先用印防己毒素处理的家兔中,可见安定缩短 T_IT_E的作用不受影响。异烟肼或印防己毒素还能部分对抗安定的降压效应。阿片受体拮抗剂纳洛酮和5-HT 受体拮抗剂赛庚啶都不能阻遏安定降低膈神经放电幅度和动脉血压的作用。上述结果提示安定降低膈神经放电幅度的作用可能通过 GABA 这一中间环节,而内啡肽和5-HT可能不起重要作用。安定的降压作用需要有内源性 GABA 参与才得以持续较长时间,在减少GABA 或阻断 GABA 受体后,安定只有短暂的降压作用。     

正常猫膈神经单纤维电活动特征

在麻醉猫和麻痹的切断迷走神经的清醒猫,观察了膈神经单纤维电活动特征。1.电活动类型:按膈神经单纤维放电与其总干放电的相位关系分为三种类型。(1)完全同步型,即单纤维放电与总干放电同时开始并同时停止,占76.9％。(2)部分同步型占15.4％,其中早期同步,即单纤维放电与总干放电同时开始,但提前终止,占1.9％,中期同步,即单纤维放电较总干放电开始晚,又提前终止,占5.8％,晚期同步,即单纤维放电较总干放电开始晚,但两者同时终止,占7.7％。(8)非同步型,即吸气相和呼气相都有放电,但呼气相时冲动频率较低,占7.7％。前两型为单纯的吸气性放电,共占92.3％。2.单纤维放电平均参数值:麻醉猫每次吸气发放11个冲动,其频率为21次/秒,清醒猫每次吸气发放18个冲动,其频率为34次/秒。结果表明:猫膈神经单纤维放电类型和文献上报导的直接记录膈神经运动神经元放电一致,即以单纯的吸气性放电为最多。     

兔心迷走神经传出放电的活动特征

兔心迷走神经传出放电有三种类型:1.与后膈神经传出发放同步的节律性放电。这种节律性发放包含两个时相,第一时相大致与膈神经传出放电同时起止,第二时相在膈神经传出发放后期或发放终止时出现。2.持续性放电,出现在上述节律性放电的间歇期。3.偶然出现的高幅高频暴发放电。这种放电出现时,膈神经传出放电即受到明显的压抑。开放预先夹闭的颈总动脉使心迷走神经传出放电增强。窒息、静脉注射肾上腺素使心迷走神经传出放电增强,心率减慢;扩张肺、过度通气、吸入亚硝酸异戊酯使心迷走神经传出放电减少,心率增快。     

POST-MORTEM AND AMINOOXYACETIC ACID-INDUCED ACCUMULATION OF GABA: EFFECT OF GAMMA-BUTYROLACTONE AND PICROTOXIN

Abstract— The effects of γ-butyrolactone (GBL) and picrotoxin on both the post-mortem and amino-oxyacetic acid (AOAA) induced accumulations of γ-aminobutyric acid (GABA) were examined in rats. GBL produced a marked dose-dependent decrease in AOAA-induced GABA accumulation in caudate. globus pallidus, cerebellar and cerebral cortices. The cingulate cortex showed the greatest response to GBL treatment; subanesthetic doses completely blocked the effect of AOAA. Picrotoxin increased the AOAA-induced accumulation of GABA in parietal, entorhinal and cerebellar cortices, and had no significant effect in pyriform or cingulate cortices. Neither drug significantly altered the post-mortem accumulation of GABA. Results suggest that picrotoxin, a GABA antagonist and convulsant drug, causes an increase in GABA synthesis in vivo. The apparent decrease in GABA synthesis following GBL treatment was greater than that observed with anesthetic doses of chloral hydrate and was not blocked by picrotoxin. Alterations in the activity of GABA neurons, cerebral glucose metabolism and GAD activity may contribute to the apparent decrease in in vivo GABA synthesis caused by GBL.     

GABA-mediated inhibition of primary olfactory receptor neurons

Applying GABA (1 microM-1 mM) to the soma of cultured lobster olfactory receptor neurons evokes an inward current (V(m) = -60 mV) accompanied by an increase in membrane conductance, with a half-effect of 487 microM GABA. The current-voltage relationship of this current is linear between -100 and 100 mV and reverses polarity at the equilibrium potential for Cl(-). The current is blocked by picrotoxin and bicuculline methiodide, and is evoked by trans-aminocrotonic acid, isoguvacine, muscimol, imidazole-4-acetic acid, and 3-amino-1-propanesulfonic acid, but not by the GABA(C)-receptor agonist cis-4-aminocrotonic acid and the GABA(B)-receptor agonist 3-aminopropylphosphonic. Applying GABA to the soma of the cells in situ reversibly suppresses the spontaneous discharge and substantially decreases the odor-evoked discharge. The effects of GABA on the cell soma in situ are antagonized by both picrotoxin and bicuculline methiodide. Taken together with evidence that GABA directly activates a chloride channel in outside-out patches excised from the soma of these neurons, we conclude that lobster olfactory receptor neurons express an ionotropic GABA receptor that can potentially regulate the output of these cells. Copyright Copyright 1999 S. Karger AG, Basel     

Antidromic discharges of dorsal root afferents in the neonatal rat.

Presynaptic inhibition of primary afferents can be evoked from at least three sources in the adult animal: 1) by stimulation of several supraspinal structures; 2) by spinal reflex action from sensory inputs; or 3) by the activity of spinal locomotor networks. The depolarisation in the intraspinal afferent terminals which is due, at least partly, to the activation of GABA(A) receptors may be large enough to reach firing threshold and evoke action potentials that are antidromically conducted into peripheral nerves. Little is known about the development of presynaptic inhibition and its supraspinal control during ontogeny. This article, reviewing recent experiments performed on the in vitro brainstem/spinal cord preparation of the neonatal rat, demonstrates that a similar organisation is present, to some extent, in the new-born rat. A spontaneous activity consisting of antidromic discharges can be recorded from lumbar dorsal roots. The discharges are generated by the underlying afferent terminal depolarizations reaching firing threshold. The number of antidromic action potentials increases significantly in saline solution with chloride concentration reduced to 50% of control. Bath application of the GABA(A) receptor antagonist, bicuculline (5-10 microM) blocks the antidromic discharges almost completely. Dorsal root discharges are therefore triggered by chloride-dependent GABA(A) receptor-mediated mechanisms; 1) activation of descending pathways by stimulation delivered to the ventral funiculus (VF) of the spinal cord at the C1 level; 2) activation of sensory inputs by stimulation of a neighbouring dorsal root; or 3) pharmacological activation of the central pattern generators for locomotion evokes antidromic discharges in dorsal roots. VF stimulation also inhibited the response to dorsal root stimulation. The time course of this inhibition overlapped with that of the dorsal root discharge suggesting that part of the inhibition of the monosynaptic reflex may be exerted at a presynaptic level. The existence of GABA(A) receptor-independent mechanisms and the roles of the antidromic discharges in the neonatal rat are discussed.     

Discharge mechanism of pigeon optic tectum neurons in an in vitro preparation

The pattern of discharge of neurones of the pigeon's optic tectum to directly injected depolarizing current was investigated in in vitro slice preparation. Three patterns of discharge were found: some neurones (types I and II) give a tonic response: type I-neurones exhibited a repetitive firing whereas type II-neurones showed grouped discharges (doublets or triplets). Type III-neurones displayed a phasic response formed by a few action potentials of decreasing amplitude, triggered at the onset of the current pulse. Each pattern of response was associated with a specific shape of action potential.