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首页> 外文期刊>Biogerontology >Daily chronomics of proteomic profile in aging and rotenone-induced Parkinson's disease model in male Wistar rat and its modulation by melatonin
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Daily chronomics of proteomic profile in aging and rotenone-induced Parkinson's disease model in male Wistar rat and its modulation by melatonin

机译:蛋白质组学概况的日常编音学在衰老和旋转龙诱导的帕金森病疾病模型中的雄性Wistar大鼠及其褪黑素调节

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摘要

Aging is associated with changes in several basic parameters of circadian timing system (CTS) in mammals leading to circadian dysfunction. We had reported earlier that upon aging and in rotenone induced Parkinson's disease (RIPD) rat model there were significant alterations in the core clock genes expression levels and daily pulses. To identify biomarkers of aging and PD chronomics of proteomic day-night profiles in suprachiasmatic nucleus (SCN), pineal and substantia nigra (SN) in 3 month (m), 12, 24 m and RIPD rat model were studied at two time points i.e. Zeitgeber Time (ZT)-6 (mid-day) and ZT-18 (mid-night). Proteome analysis was done by using two dimensional (2-D) electrophoresis and the spots showing robust day-night variations were identified by using MALDI TOF/TOF analysis. In 3 m rats the number of proteins showing day-night variations were relatively more than 12, 24 m and RIPD rat model in SCN and SN. But in pineal there was increase in number of protein spots showing day-night variations in 24 m. Mass spectroscopy of the protein spots showing robust day night variation in aging and RIPD rats were identified. As melatonin, a multitasking molecule, an endogenous synchronizer of rhythm, an antioxidant and an antiaging drug, declines with aging, the effects of melatonin administration on differential alterations in chronomics of 2-D protein profiles in aging and RIPD male Wistar rats were studied. We report here that the melatonin could be playing an important role in modulating the chronomics of 2-D protein profiles. Additionally, various proteins were identified for the first time in this study showing significant day night variation in SCN, pineal and SN may prove useful towards targeting novel treatments for circadian dysfunction, good health and longevity.
机译:老化与哺乳动物中的昼夜节奏时序系统(CTS)的几个基本参数的变化有关,导致昼夜功能障碍。我们之前报道,在老化和Rotenone诱导帕金森病(RIPD)大鼠模型后,核心时钟基因表达水平和每日脉冲存在显着改变。为了鉴定3个月(M),12,24M和RIPD大鼠模型中的3个月(M),12,24M和RIPD大鼠模型中的蛋白质组日夜间蛋白质组昼夜曲线的蛋白质组季夜间曲线的衰老和PD编音学器的生物标志物。 Zeitgeber时间(ZT)-6(中午)和ZT-18(中午)。通过使用二维(2-D)电泳来完成蛋白质组分析,并且通过使用MALDI TOF / TOF分析来鉴定显示稳健的日夜变异的斑点。在3米的大鼠中,SCN和Sn中的蛋白质显示日夜间变异的蛋白质数量相对大于12,24M和RIPD大鼠模型。但在松果中,蛋白质点数增加了24米的夜间变化的数量。鉴定了显示老化和RIPD大鼠稳健日夜间变异的蛋白质点的质谱。作为褪黑素,多任务分子,节律的内源性同步器,抗氧化剂和抗衰老药物,随着衰老的下降,研究了褪黑素给药对衰老和RIPD雄性Wistar大鼠的2-D蛋白谱系统编程中的差异变化的影响。我们在此报道,褪黑激素可能在调节2-D蛋白质谱的编音学方面发挥重要作用。另外,在本研究中首次鉴定各种蛋白质,显示出SCN,松果和Sn的大量夜间变异,可能对靶心昼夜功能障碍,健康和寿命造成新的治疗方法。

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