Glutamatergic and purinergic transmitters and astrocyte modulation in the synaptic transmission in the NTS of rats exposed to short-term sustained hypoxia.

IF 2.2 3区医学 Q3 PHYSIOLOGY

American journal of physiology. Regulatory, integrative and comparative physiology Pub Date : 2024-10-01 Epub Date: 2024-08-05 DOI:10.1152/ajpregu.00293.2023

Darlan S Bazilio, Davi J A Moraes, Benedito H Machado

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引用次数: 0

Abstract

There is evidence that astrocytes modulate synaptic transmission in the nucleus tractus solitarius (NTS) interacting with glutamatergic and purinergic mechanisms. Here, using in situ working heart-brainstem preparations, we evaluated the involvement of astrocyte and glutamatergic/purinergic neurotransmission in the processing of autonomic and respiratory pathways in the NTS of control and rats exposed to sustained hypoxia (SH). Baseline autonomic and respiratory activities and the responses to chemoreflex activation (KCN) were evaluated before and after microinjections of fluorocitrate (FCt, an astrocyte metabolic inhibitor), kynurenic acid, and pyridoxalphosphate-6-azophenyl-2',4'-disulfonate (PPADS) (nonselective antagonists of glutamatergic and purinergic receptors) into the rostral aspect of the caudal commissural NTS. FCt had no effects on the baseline parameters evaluated but reduced the bradycardic response to chemoreflex activation in SH rats. FCt combined with kynurenic acid and PPADS in control rats reduced the baseline duration of expiration, which was attenuated after SH. FCt produced a large increase in PN frequency discharge in control rats, which was reduced after SH, indicating a reduction in the astrocyte modulation after SH. The data show that 1) the bradycardic component of the peripheral chemoreflex is reduced in SH rats after astrocytes inhibition, 2) the inhibition of astrocytes in the presence of double antagonists in the NTS affects the modulation of baseline duration of expiration in control but not in SH rats, and 3) the autonomic and respiratory responses to chemoreflex activation are mediated by glutamatergic and purinergic receptors in the rostral aspect of the caudal commissural NTS.NEW & NOTEWORTHY Our findings indicate that the neurotransmission of autonomic and respiratory components of the peripheral chemoreflex in the nucleus tractus solitarius (NTS) is mediated by glutamatergic and purinergic mechanisms and reveal a selective involvement of NTS astrocytes in controlling the chemoreflex parasympathetic response in rats exposed to sustained hypoxia (SH) and the baseline duration of expiration mainly in control rats, indicating a selective role for astrocytes modulation in the NTS of control and SH rats.

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暴露于短期持续缺氧的大鼠 NTS 中突触传递的谷氨酸能和嘌呤能递质以及星形胶质细胞的调节作用

有证据表明，星形胶质细胞能与谷氨酸能和嘌呤能机制相互作用，调节 NTS 中的突触传递。在这里，我们使用原位工作心脑干制备物评估了星形胶质细胞和谷氨酸能/嘌呤能神经传递参与对照组和暴露于持续缺氧（SH）的大鼠 NTS 自主神经和呼吸通路处理的情况。在向大鼠尾突NTS喙侧微量注射柠檬酸氟（FCt，一种星形胶质细胞代谢抑制剂）、犬尿酸和PPADS（谷氨酸能和嘌呤能受体的非选择性拮抗剂）前后，评估了大鼠的自律神经和呼吸活动基线以及对化学反射激活（KCN）的反应。FCt 对评估的基线参数没有影响，但降低了 SH 大鼠对化学反射激活的心动过缓反应。在对照组大鼠中，FCt 与犬尿酸和 PPADS 联用可缩短呼气的基线持续时间，而在 SH 组大鼠中则缩短了呼气的基线持续时间。FCt 可显著增加对照组大鼠的 PN 频率放电，而 SH 后这一频率放电减少，这表明 SH 后星形胶质细胞的调节作用减弱。这些数据表明：a）抑制星形胶质细胞后，SH 大鼠外周化学反射的心动过缓成分减少；b）在 NTS 双拮抗剂存在的情况下抑制星形胶质细胞会影响对照组大鼠呼气基线持续时间的调节，但不会影响 SH 大鼠；c）化学反射激活后的自主神经和呼吸反应是由尾突 NTS 喙侧的谷氨酸能和嘌呤能受体介导的。

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来源期刊

American journal of physiology. Regulatory, integrative and comparative physiology 医学-生理学

CiteScore

5.30

自引率

3.60%

发文量

145

审稿时长

2 months

期刊介绍： The American Journal of Physiology-Regulatory, Integrative and Comparative Physiology publishes original investigations that illuminate normal or abnormal regulation and integration of physiological mechanisms at all levels of biological organization, ranging from molecules to humans, including clinical investigations. Major areas of emphasis include regulation in genetically modified animals; model organisms; development and tissue plasticity; neurohumoral control of circulation and hypertension; local control of circulation; cardiac and renal integration; thirst and volume, electrolyte homeostasis; glucose homeostasis and energy balance; appetite and obesity; inflammation and cytokines; integrative physiology of pregnancy-parturition-lactation; and thermoregulation and adaptations to exercise and environmental stress.