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猫丘脑前复合体中中间神经元产生的三种抑制性突触后电位。

Three types of inhibitory postsynaptic potentials generated by interneurons in the anterior thalamic complex of cat.

作者信息

Paré D, Dossi R C, Steriade M

机构信息

Laboratoire de Neurophysiologie, Faculté de Médecine, Université Laval, Quebec, Canada.

出版信息

J Neurophysiol. 1991 Oct;66(4):1190-204. doi: 10.1152/jn.1991.66.4.1190.

Abstract
  1. These experiments were carried out to study how thalamic interneurons generate inhibitory postsynaptic potentials (IPSPs) in relay cells. Intracellular recordings were performed in the anterior thalamic (AT) nuclei, a nuclear group in which interneurons constitute the only intrathalamic source of gamma-aminobutyric acid (GABA). 2. In the AT complex, as in most dorsal thalamic nuclei, interneurons can influence relay cells through their presynaptic dendrites (PSDs) and their axons. This dual mode of action is paralleled by a different termination pattern of prethalamic fibers and cortical axons on interneurons. Prethalamic fibers, which in the AT nuclei arise in the mammillary bodies (MBs), end mostly on PSDs, whereas cortical terminals usually synapse on the parent dendrites of PSDs. We therefore took advantage of the differential mode of termination of cortical and MB afferents on interneurons to infer the respective roles of the axons and PSDs of interneurons in the genesis of the IPSPs recorded from relay cells. 3. In all responsive AT cells, cortical stimuli delivered at low frequency (less than or equal to 0.5 Hz) evoked a biphasic IPSP, with an early and a late phase, having a total duration of 221.96 +/- 8.18 ms (mean +/- SE). The early part of the IPSP (termed A) had a reversal potential (ER) close to the equilibrium potential for Cl- ions: -79.25 +/- 2.14 mV. Furthermore, it reversed in polarity after impalement of the cells with KCl-filled pipettes. The late IPSP (termed B) always began before the end of the early IPSP, 45.93 +/- 2.50 ms after the onset of the A-IPSP. The B-IPSP had an ER of -109 +/- 2.4 mV and was not affected by Cl- injection. 4. By contrast, MB stimuli delivered at low frequency (less than or equal to 0.5 Hz) evoked a triphasic IPSP having a total duration of 220.5 +/- 9.42 ms in most (61.2%) AT cells. The IPSP with the shortest latency (termed a) was evoked only by MB stimuli. Before the return of the membrane potential to the resting level, a second hyperpolarizing potential began (7.41 +/- 0.46 ms after the onset of the a-IPSP). This second inhibitory phase was biphasic and had electrophysiological characteristics similar to the biphasic A- and B-IPSP evoked by cortical stimulation. Both the MB-evoked a- and A-IPSPs had an ER close to the equilibrium potential for Cl- ions (-72.22 +/- 0.68 and -72 +/- 0.82 mV, respectively) and reversed in polarity after impalement of the cells with KCl-filled pipettes.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 进行这些实验是为了研究丘脑中间神经元如何在中继细胞中产生抑制性突触后电位(IPSPs)。在前丘脑(AT)核进行了细胞内记录,在前丘脑核中,中间神经元是γ-氨基丁酸(GABA)的唯一丘脑内来源。2. 在AT复合体中,与大多数背侧丘脑核一样,中间神经元可以通过其突触前树突(PSD)和轴突影响中继细胞。这种双重作用模式与丘脑前纤维和皮质轴突在中间神经元上不同的终止模式相对应。在AT核中起源于乳头体(MBs)的丘脑前纤维大多终止于PSD,而皮质终末通常与PSD的母树突形成突触。因此,我们利用皮质和MB传入纤维在中间神经元上不同的终止模式,来推断中间神经元的轴突和PSD在中继细胞记录到的IPSP产生过程中的各自作用。3. 在所有有反应的AT细胞中,低频(小于或等于0.5 Hz)施加的皮质刺激诱发了一个双相IPSP,有早期和晚期两个阶段,总持续时间为221.96±8.18毫秒(平均值±标准误)。IPSP的早期部分(称为A)具有接近Cl⁻离子平衡电位的反转电位(ER):-79.25±2.14毫伏。此外,在用充满KCl的微电极刺入细胞后,其极性发生反转。晚期IPSP(称为B)总是在早期IPSP结束前开始,在A-IPSP开始后45.93±2.50毫秒。B-IPSP的ER为-109±2.4毫伏,不受Cl⁻注入的影响。4. 相比之下,低频(小于或等于0.5 Hz)施加的MB刺激在大多数(61.2%)AT细胞中诱发了一个三相IPSP,总持续时间为220.5±9.42毫秒。潜伏期最短的IPSP(称为a)仅由MB刺激诱发。在膜电位恢复到静息水平之前,第二个超极化电位开始(在a-IPSP开始后7.41±0.46毫秒)。这个第二个抑制阶段是双相的,其电生理特征与皮质刺激诱发的双相A-和B-IPSP相似。MB诱发的a-和A-IPSP的ER都接近Cl⁻离子平衡电位(分别为-72.22±0.68和-72±0.82毫伏),在用充满KCl的微电极刺入细胞后其极性发生反转。(摘要截断于400字)

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