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大鼠视交叉上核中对兰尼碱敏感的细胞内钙离子通道是行为昼夜节律控制所必需的。

Ryanodine-sensitive intracellular Ca2+ channels in rat suprachiasmatic nuclei are required for circadian clock control of behavior.

作者信息

Mercado Clara, Díaz-Muñoz Mauricio, Alamilla Javier, Valderrama Karla, Morales-Tlalpan Verónica, Aguilar-Roblero Raúl

机构信息

Departamento de Neurociencias, Instituto de Fisiología Celular, Distrito Federal, Mexico.

出版信息

J Biol Rhythms. 2009 Jun;24(3):203-10. doi: 10.1177/0748730409333354.

DOI:10.1177/0748730409333354
PMID:19465697
Abstract

Electrophysiological and calcium mobilization experiments have suggested that the intracellular calcium release channel ryanodine receptors (RyRs) are involved in the circadian rhythmicity of the suprachiasmatic nucleus (SCN). In the present report the authors provide behavioral evidence that RyRs play a specific and major role in the output of the molecular circadian clock in SCN neurons. They measured the circadian rhythm of drinking and locomotor behaviors in dim red light before, during, and after administration of an activator (ryanodine 0.1 microM) or an inhibitor (ryanodine 100 microM) of the RyRs. Drugs were delivered directly into the SCN by cannulas connected to osmotic minipumps. Control treatments included administration of artificial cerebrospinal fluid, KCl (20 mM), tetrodotoxin (1 microM), and anysomicin (5 microg/microl). Activation of RyRs induced a significant shortening of the endogenous period, whereas inhibition of these Ca2+ release channels disrupted the circadian rhythmicity. After the pharmacological treatments the period of rhythmicity returned to basal values and the phase of activity onset was predicted from a line projected from the activity onset of basal recordings. These results indicate that changes in overt rhythms induced by both doses of ryanodine did not involve an alteration in the clock mechanism. The authors conclude that circadian modulation of RyRs is a key element of the output pathway from the molecular circadian clock in SCN neurons in rats.

摘要

电生理和钙动员实验表明,细胞内钙释放通道兰尼碱受体(RyRs)参与了视交叉上核(SCN)的昼夜节律。在本报告中,作者提供了行为学证据,证明RyRs在SCN神经元分子生物钟的输出中发挥着特定且重要的作用。他们测量了在给予RyRs激活剂(0.1微摩尔兰尼碱)或抑制剂(100微摩尔兰尼碱)之前、期间和之后,昏暗红光下饮水和运动行为的昼夜节律。药物通过连接到渗透微型泵的套管直接注入SCN。对照处理包括给予人工脑脊液、氯化钾(20毫摩尔)、河豚毒素(1微摩尔)和茴香霉素(5微克/微升)。RyRs的激活导致内源性周期显著缩短,而这些钙释放通道的抑制则破坏了昼夜节律。药理学处理后,节律周期恢复到基础值,并且根据基础记录活动开始时投射的一条线预测活动开始的相位。这些结果表明,两种剂量的兰尼碱诱导的明显节律变化并不涉及时钟机制的改变。作者得出结论,RyRs的昼夜调节是大鼠SCN神经元分子生物钟输出途径的关键要素。

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Ryanodine-sensitive intracellular Ca2+ channels in rat suprachiasmatic nuclei are required for circadian clock control of behavior.大鼠视交叉上核中对兰尼碱敏感的细胞内钙离子通道是行为昼夜节律控制所必需的。
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