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Ventrolateral medullary functional connectivity and the respiratory and central chemoreceptor-evoked modulation of retrotrapezoid-parafacial neurons

机译:腹侧延髓功能连通性和梯形后面神经元的呼吸和中央化学感受器诱发的调制

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摘要

The medullary ventral respiratory column (VRC) of neurons is essential for respiratory motor pattern generation; however, the functional connections among these cells are not well understood. A rostral extension of the VRC, including the retrotrapezoid nucleus/parafacial region (RTN-pF), contains neurons responsive to local perturbations of CO2/pH. We addressed the hypothesis that both local RTN-pF interactions and functional connections from more caudal VRC compartments—extending from the Bötzinger and pre-Bötzinger complexes to the ventral respiratory group (Böt-VRG)—influence the respiratory modulation of RTN-pF neurons and their responses to central chemoreceptor and baroreflex activation. Spike trains from 294 RTN-pF and 490 Böt-VRG neurons were monitored with multielectrode arrays along with phrenic nerve activity in 14 decerebrate, vagotomized cats. Overall, 214 RTN-pF and 398 Böt-VRG neurons were respiratory modulated; 124 and 95, respectively, were cardiac modulated. Subsets of these neurons were tested with sequential, selective, transient stimulation of central chemoreceptors and arterial baroreceptors; each cell's response was evaluated and categorized according to the change in firing rate (if any) following the stimulus. Cross-correlation analysis was applied to 2,884 RTN-pF↔RTN-pF and 8,490 Böt-VRG↔RTN-pF neuron pairs. In total, 174 RTN-pF neurons (59.5%) had significant features in short-time scale correlations with other RTN-pF neurons. Of these, 49 neurons triggered cross-correlograms with offset peaks or troughs (n = 99) indicative of paucisynaptic excitation or inhibition of the target. Forty-nine Böt-VRG neurons (10.0%) were triggers in 74 Böt-VRG→RTN-pF correlograms with offset features, suggesting that Böt-VRG trigger neurons influence RTN-pF target neurons. The results support the hypothesis that local RTN-pF neuron interactions and inputs from Böt-VRG neurons jointly contribute to respiratory modulation of RTN-pF neuronal discharge patterns and promotion or limitation of their responses to central chemoreceptor and baroreceptor stimulation.
机译:神经元的延髓腹侧呼吸柱(VRC)对于呼吸运动模式的产生至关重要。但是,这些单元之间的功能连接尚不清楚。 VRC的延展性延伸,包括梯形后核/界面区(RTN-pF),包含对CO2 / pH的局部扰动有响应的神经元。我们解决了以下假设:局部RTN-pF相互作用和更多尾VRC隔室的功能连接-从Bötzinger和前Bötzinger复合体延伸到腹侧呼吸组(Böt-VRG)-影响RTN-pF神经元和他们对中枢化学感受器和压力反射激活的反应。用多电极阵列监测了294例RTN-pF和490个Böt-VRG神经元的穗状花序,以及14神经切除的14例去脑切除的猫的神经活动。总体而言,呼吸调节了214个RTN-pF和398个Böt-VRG神经元。分别对124和95进行了心脏调节。通过对中央化学感受器和动脉压力感受器的顺序,选择性,短暂刺激来测试这些神经元的亚群。根据刺激后发射率(如果有)的变化,对每个细胞的反应进行评估和分类。将互相关分析应用于2,884个RTN-pF↔RTN-pF和8,490个Böt-VRG↔RTN-pF神经元对。总共174个RTN-pF神经元与其他RTN-pF神经元在短时尺度相关性中具有显着特征。在这些神经元中,有49个神经元触发了具有相关峰或谷(n = 99)的互相关图,表明峰突触激发或抑制了靶标。在具有偏移特征的74个Böt-VRG→RTN-pF相关图中,触发了49个Böt-VRG神经元,表明Böt-VRG触发神经元影响RTN-pF目标神经元。结果支持以下假设:局部RTN-pF神经元相互作用和来自Böt-VRG神经元的输入共同有助于RTN-pF神经元放电模式的呼吸调节,并促进或限制其对中枢化学感受器和压力感受器刺激的反应。

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