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评估雄性大鼠不同脑区 FADD 及其相关分子标记物的日调制。

Evaluating the daily modulation of FADD and related molecular markers in different brain regions in male rats.

机构信息

IUNICS, University of the Balearic Islands, Palma, Spain.

Health Research Institute of the Balearic Islands (IdISBa), Palma, Spain.

出版信息

J Neurosci Res. 2024 Feb;102(2):e25296. doi: 10.1002/jnr.25296.

Abstract

Fas-Associated protein with Death Domain (FADD), a key molecule controlling cell fate by balancing apoptotic versus non-apoptotic functions, is dysregulated in post-mortem brains of subjects with psychopathologies, in animal models capturing certain aspects of these disorders, and by several pharmacological agents. Since persistent disruptions in normal functioning of daily rhythms are linked with these conditions, oscillations over time of key biomarkers, such as FADD, could play a crucial role in balancing the clinical outcome. Therefore, we characterized the 24-h regulation of FADD (and linked molecular partners: p-ERK/t-ERK ratio, Cdk-5, p35/p25, cell proliferation) in key brain regions for FADD regulation (prefrontal cortex, striatum, hippocampus). Samples were collected during Zeitgeber time (ZT) 2, ZT5, ZT8, ZT11, ZT14, ZT17, ZT20, and ZT23 (ZT0, lights-on or inactive period; ZT12, lights-off or active period). FADD showed similar daily fluctuations in all regions analyzed, with higher values during lights off, and opposite to p-ERK/t-ERK ratios regulation. Both Cdk-5 and p35 remained stable and did not change across ZT. However, p25 increased during lights off, but exclusively in striatum. Finally, no 24-h modulation was observed for hippocampal cell proliferation, although higher values were present during lights off. These results demonstrated a clear daily modulation of FADD in several key brain regions, with a more prominent regulation during the active time of rats, and suggested a key role for FADD, and molecular partners, in the normal physiological functioning of the brain's daily rhythmicity, which if disrupted might participate in the development of certain pathologies.

摘要

Fas 相关死亡结构域蛋白(FADD)是一种通过平衡凋亡与非凋亡功能来控制细胞命运的关键分子,其在精神病理学患者的死后大脑、模拟这些疾病某些方面的动物模型以及几种药理学制剂中失调。由于正常昼夜节律功能的持续中断与这些疾病有关,因此关键生物标志物(如 FADD)的时间波动可能在平衡临床结果方面发挥关键作用。因此,我们描述了 FADD(及其相关分子伴侣:p-ERK/t-ERK 比值、Cdk-5、p35/p25、细胞增殖)在 FADD 调节的关键大脑区域(前额叶皮层、纹状体、海马体)中的 24 小时调节。在 Zeitgeber 时间(ZT)2、ZT5、ZT8、ZT11、ZT14、ZT17、ZT20 和 ZT23(ZT0,光照或非活动期;ZT12,光照关闭或活动期)收集样本。FADD 在所有分析区域均表现出相似的日波动,在光照关闭期间值较高,与 p-ERK/t-ERK 比值的调节相反。Cdk-5 和 p35 保持稳定,在整个 ZT 期间均无变化。然而,p25 在光照关闭期间增加,但仅在纹状体中增加。最后,未观察到海马体细胞增殖的 24 小时调节,但在光照关闭期间存在更高的值。这些结果表明 FADD 在几个关键大脑区域存在明显的日调节,在大鼠的活动时间表现出更为明显的调节,并表明 FADD 和分子伴侣在大脑日常节律的正常生理功能中具有关键作用,如果中断,可能会参与某些疾病的发展。

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