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健康受试者和一名患有昼夜节律睡眠障碍的患者全血细胞中生物钟基因的每日表达情况。

Daily expression of clock genes in whole blood cells in healthy subjects and a patient with circadian rhythm sleep disorder.

作者信息

Takimoto Mieko, Hamada Akinobu, Tomoda Akemi, Ohdo Shigehiro, Ohmura Takafumi, Sakato Hisao, Kawatani Junko, Jodoi Takako, Nakagawa Hiroo, Terazono Hideyuki, Koyanagi Satoru, Higuchi Shun, Kimura Miyuki, Tukikawa Hiroshi, Irie Shin, Saito Hideyuki, Miike Teruhisa

机构信息

Department of Pharmacy, Kumamoto University Hospital, 1-1-1 Honjo, Kumamoto 860-8556, Japan.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2005 Nov;289(5):R1273-9. doi: 10.1152/ajpregu.00126.2005. Epub 2005 Jun 16.

Abstract

In recent years, circadian rhythm sleep disorders in humans have been increasing. Clinical features characteristic of this disorder are well known, but the specific causes remain unknown. However, various derangements of circadian expression of the clock gene are a probable cause of this disease. We have attempted to elucidate the relationship between the expression of the clock genes in whole blood cells and the clinical features characteristic of this disorder. In this study, we indicate the daily expression of clock genes period (Per) 1, 2, 3, Bmal1, and Clock in whole blood cells in 12 healthy male subjects. The peak phase of Per1, Per2, and Per3 appeared in the early morning, whereas that of Bmal1 and Clock appeared in the midnight hours. Furthermore, in one patient case with circadian rhythm sleep disorder, we observed variations of the peak phase in clock genes by treatments such as light therapy, exercise therapy, and medicinal therapy. This study suggested that the monitoring of human clock genes in whole blood cells, which may be functionally important for the molecular control of the circadian pacemaker as well as in suprachiasmatic nucleus, might be useful to evaluate internal synchronization.

摘要

近年来,人类昼夜节律睡眠障碍呈上升趋势。这种疾病的临床特征广为人知,但其具体病因仍不明晰。然而,生物钟基因昼夜节律表达的各种紊乱可能是该疾病的病因。我们试图阐明全血细胞中生物钟基因的表达与这种疾病的临床特征之间的关系。在本研究中,我们测定了12名健康男性受试者全血细胞中生物钟基因周期蛋白(Per)1、2、3、脑和肌肉组织ARNT样蛋白1(Bmal1)以及生物钟(Clock)的每日表达情况。Per1、Per2和Per3的峰值相位出现在清晨,而Bmal1和Clock的峰值相位出现在午夜时分。此外,在1例昼夜节律睡眠障碍患者中,我们观察到通过光疗、运动疗法和药物疗法等治疗手段,生物钟基因的峰值相位发生了变化。本研究表明,监测全血细胞中的人类生物钟基因,这可能对昼夜节律起搏器以及视交叉上核的分子控制具有重要功能,可能有助于评估体内同步情况。

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