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睡眠剥夺会在幼年和老年大鼠的肝脏和胰腺中引发氧化应激。

Sleep deprivation induces oxidative stress in the liver and pancreas in young and aging rats.

作者信息

Hernández Santiago Karina, López-López Ana Laura, Sánchez-Muñoz Fausto, Cortés Altamirano José Luis, Alfaro-Rodríguez Alfonso, Bonilla-Jaime Herlinda

机构信息

Maestria en Biologia de la Reproducción, Universidad Autónoma Metropolitana-Iztapalapa, CP 09340, Ciudad de Mexico, Mexico.

CINVESTAV sede sur, Departamento de Farmacología, Calz. de los Tenorios 235, Coapa, Rinconada de las Hadas, Tlalpan, Ciudad de México, 14330, México.

出版信息

Heliyon. 2021 Mar 11;7(3):e06466. doi: 10.1016/j.heliyon.2021.e06466. eCollection 2021 Mar.

Abstract

The aging process is characterized by a gradual impairment generally caused by oxidative stress and, more specifically, sleep deprivation, which induces oxidative stress in the brain. The objective of this study was to assess the effect of three types of paradoxical sleep deprivation (PSD): 96 h of PSD (96PSD group); 192 h of PSD (192PSD group); 192 h of PSD followed by a recovery period of 20 days (192PSD + Recovery group) on an oral glucose tolerance test (OGTT), lipid peroxidation (LPO), and superoxide dismutase (SOD) and catalase (CAT) activities in the liver and pancreas of young (3-month-old) and adult (14-month-old) rats. The 96PSD and 192PSD groups of young rats showed lower glucose levels on the OGTT than the control group. In the adult rats, only the 96PSD group had lower glucose levels than the control group. However, the areas under the curve for the young and adult 192 and 192PSD + Recovery groups showed significant differences. Both LPO and SOD increased in the 192PSD and 192PSD + Recovery groups, but CAT decreased in the liver of young rats in the 192PSD group. Regarding the pancreas, LPO and SOD levels increased after 96 h of PSD. In adult animals, CAT decreased in the liver after 96 and 192 h of PSD, while LPO and SOD increased in the pancreas of the 192PSD and PSD + Recovery groups. Differences in the SOD and CAT activities in the liver and SOD activities in the pancreas were also observed between the young and adult rats and maintained across all the PSD groups. In conclusion, PSD induced differential responses that appeared to depend on the duration of the induced condition, the animals' age, and the tissue analyzed. It was found that adult rats were more susceptible to the effects of PSD than young rats.

摘要

衰老过程的特征是通常由氧化应激引起的逐渐损伤,更具体地说,是睡眠剥夺,它会在大脑中诱导氧化应激。本研究的目的是评估三种类型的异相睡眠剥夺(PSD):96小时PSD(96PSD组);192小时PSD(192PSD组);192小时PSD后接着20天恢复期(192PSD + 恢复期组)对年轻(3个月大)和成年(14个月大)大鼠口服葡萄糖耐量试验(OGTT)、脂质过氧化(LPO)以及肝脏和胰腺中超氧化物歧化酶(SOD)和过氧化氢酶(CAT)活性的影响。年轻大鼠的96PSD组和192PSD组在OGTT上的血糖水平低于对照组。在成年大鼠中,只有96PSD组的血糖水平低于对照组。然而,年轻和成年的192PSD组及192PSD + 恢复期组的曲线下面积显示出显著差异。192PSD组和192PSD + 恢复期组的LPO和SOD均升高,但192PSD组年轻大鼠肝脏中的CAT降低。关于胰腺,PSD 96小时后LPO和SOD水平升高。在成年动物中,PSD 96小时和192小时后肝脏中的CAT降低,而192PSD组和PSD + 恢复期组胰腺中的LPO和SOD升高。在年轻和成年大鼠之间还观察到肝脏中SOD和CAT活性以及胰腺中SOD活性的差异,并且在所有PSD组中均保持。总之,PSD诱导的差异反应似乎取决于诱导条件的持续时间、动物的年龄以及所分析的组织。研究发现成年大鼠比年轻大鼠更容易受到PSD的影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dbf1/7966994/d109eebcd1e7/gr1.jpg

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