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肺牵张感受器传入神经激活大鼠孤束核中的兴奋性氨基酸受体。

Pulmonary stretch receptor afferents activate excitatory amino acid receptors in the nucleus tractus solitarii in rats.

作者信息

Bonham A C, Coles S K, McCrimmon D R

机构信息

Department of Physiology, Northwestern University Medical School, Chicago, IL 60611-3008.

出版信息

J Physiol. 1993 May;464:725-45. doi: 10.1113/jphysiol.1993.sp019660.

Abstract
  1. The goal of the present study was to identify potential neurotransmitter candidates in the Breuer-Hering (BH) reflex pathway, specifically at synapses between the primary afferents and probable second-order neurones (pump cells) within the nucleus tractus solitarii (NTS). We hypothesized that if activation of specific receptors in the NTS is required for production of the BH reflex, then (1) injection of the receptor agonist(s) would mimic the reflex response (apnoea), (2) injection of appropriate antagonists would impair the apnoea produced by either lung inflation or agonist injection, and (3) second-order neurones in the pathway would be excited by either lung inflation or agonists while antagonists would prevent the response to either. 2. Studies were carried out either in spontaneously breathing or in paralysed, thoracotomized and ventilated rats in which either diaphragm EMG or phrenic nerve activity, expired CO2 concentration and arterial pressure were continuously monitored. The BH reflex was physiologically activated by inflating the lungs. 3. Pressure injections (0.03-15 pmol) of selective excitatory amino acid (EAA) receptor agonists, quisqualic acid (Quis) and N-methyl-D-aspartic acid (NMDA) into an area of the NTS shown previously to contain neurones required for production of the BH reflex produced dose-dependent apnoeas that mimicked the response to lung inflation. Injection of substance P (0.03-4 pmol) did not alter baseline respiratory pattern. 4. Injections of the EAA antagonists, kynurenic acid (Kyn; 0.6-240 pmol), 6-cyano-7-nitro-quinoxaline-2,3-dione (CNQX) or 6,7-dinitroquinoxaline-2,3-dione (DNQX) into the BH region of the NTS reversibly impaired the apnoea produced by lung inflation. All three antagonists reduced or abolished the apnoeas resulting from injection of Quis or NMDA, and slowed baseline respiratory frequency. In contrast, injections of the highly selective NMDA receptor antagonist, D-2-amino-5-phosphonovaleric acids (AP5), in doses sufficient to block the apnoeic response to NMDA, neither altered the reflex apnoea evoked by lung inflation nor the baseline respiratory pattern. 5. Pump cells located within the BH region were excited by pressure injections of the broad spectrum EAA agonist, DL-homocysteic acid (DLH). Kyn reversibly blocked the excitation of pump cells in response to either lung inflation or DLH injection. 6. These findings suggest that EAAs mediate primary afferent excitation of second-order neurones in the Breuer-Hering reflex pathway, primarily through the activation of non-NMDA EAA receptor subtypes.
摘要
  1. 本研究的目的是确定布雷尔 - 黑林(BH)反射通路中的潜在神经递质候选物,特别是在孤束核(NTS)内初级传入神经与可能的二级神经元(泵细胞)之间的突触处。我们假设,如果NTS中特定受体的激活是产生BH反射所必需的,那么:(1)注射受体激动剂将模拟反射反应(呼吸暂停);(2)注射适当的拮抗剂将损害由肺膨胀或激动剂注射产生的呼吸暂停;(3)该通路中的二级神经元将被肺膨胀或激动剂兴奋,而拮抗剂将阻止对两者的反应。2. 研究在自主呼吸的大鼠或麻痹、开胸并通气的大鼠中进行,持续监测膈肌肌电图或膈神经活动、呼出二氧化碳浓度和动脉血压。通过肺膨胀在生理上激活BH反射。3. 向先前显示含有产生BH反射所需神经元的NTS区域选择性注射兴奋性氨基酸(EAA)受体激动剂喹啉酸(Quis)和N - 甲基 - D - 天冬氨酸(NMDA)(0.03 - 15 pmol),产生剂量依赖性呼吸暂停,模拟对肺膨胀的反应。注射P物质(0.03 - 4 pmol)未改变基线呼吸模式。4. 在NTS的BH区域注射EAA拮抗剂犬尿氨酸(Kyn;0.6 - 240 pmol)、6 - 氰基 - 7 - 硝基喹喔啉 - 2,3 - 二酮(CNQX)或6,7 - 二硝基喹喔啉 - 2,3 - 二酮(DNQX)可逆地损害由肺膨胀产生的呼吸暂停。所有三种拮抗剂均减少或消除了由Quis或NMDA注射引起的呼吸暂停,并减慢了基线呼吸频率。相比之下,注射高选择性NMDA受体拮抗剂D - 2 - 氨基 - 5 - 磷酸戊酸(AP5),剂量足以阻断对NMDA的呼吸暂停反应,既未改变由肺膨胀诱发的反射性呼吸暂停,也未改变基线呼吸模式。5. 位于BH区域的泵细胞通过压力注射广谱EAA激动剂DL - 高半胱氨酸(DLH)而兴奋。Kyn可逆地阻断泵细胞对肺膨胀或DLH注射的兴奋反应。6. 这些发现表明,EAA主要通过激活非NMDA EAA受体亚型介导布雷尔 - 黑林反射通路中二级神经元的初级传入兴奋。
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b22/1175411/7f82c64f0208/jphysiol00418-0722-a.jpg

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