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哺乳动物呼吸节律的产生:突触和膜特性

Respiratory rhythm generation in mammals: synaptic and membrane properties.

作者信息

Ramirez J M, Telgkamp P, Elsen F P, Quellmalz U J, Richter D W

机构信息

Department of Organismal Biology and Anatomy, University of Chicago, IL 60637, USA.

出版信息

Respir Physiol. 1997 Nov;110(2-3):71-85. doi: 10.1016/s0034-5687(97)00074-1.

Abstract

Respiratory rhythm generation depends on a complex interaction between synaptic and membrane properties of functionally defined neurons. To gain a better understanding of how inhibitory and excitatory synaptic inputs lead to the generation of the respiratory rhythm we analyzed the depolarization pattern of respiratory neurons that were recorded in the transverse slice preparation of mice (P8-22) and the in vivo adult cat. Using voltage-calmp recordings from respiratory neurons and specific antagonists for inhibitory synaptic transmission we demonstrate under in vitro conditions, that inspiratory (n = 7) and post-inspiratory neurons (n = 13) received concurrent glycinergic and glutamatergic synaptic input during inspiration. A similar conclusion was gained with chloride injections into in vivo respiratory neurons. The inhibitory input was essential not only for generating the characteristic depolarization pattern of respiratory neurons, but also for switching the respiratory rhythm between inspiration and post-inspiration. The generation of the depolarization pattern depends also on intrinsic membrane properties. Negative current injections reveal that excitatory synaptic input was amplified by intrinsic bursting properties in some inspiratory neurons (n = 4) recorded in vitro. Although such properties have not been described under in vivo conditions our findings suggest that with respect to inspiratory, post-inspiratory and late-inspiratory neurons, the principle network organization is similar under both in vitro and in vivo conditions.

摘要

呼吸节律的产生依赖于功能明确的神经元的突触特性和膜特性之间的复杂相互作用。为了更好地理解抑制性和兴奋性突触输入如何导致呼吸节律的产生,我们分析了在小鼠(P8 - 22)横切片标本和成年猫体内记录的呼吸神经元的去极化模式。利用呼吸神经元的电压钳记录和抑制性突触传递的特异性拮抗剂,我们在体外条件下证明,吸气神经元(n = 7)和吸气后神经元(n = 13)在吸气期间同时接受甘氨酸能和谷氨酸能突触输入。向体内呼吸神经元注射氯离子也得出了类似的结论。抑制性输入不仅对于产生呼吸神经元特征性的去极化模式至关重要,而且对于在吸气和吸气后之间切换呼吸节律也至关重要。去极化模式的产生还取决于内在膜特性。负电流注入显示,在体外记录的一些吸气神经元(n = 4)中,兴奋性突触输入被内在爆发特性放大。尽管在体内条件下尚未描述此类特性,但我们的研究结果表明,就吸气、吸气后和吸气末神经元而言,体外和体内条件下的主要网络组织相似。

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