2型糖尿病合并微血管病变患者的氧化DNA损伤及聚(ADP-核糖)聚合酶/核因子-κB信号通路增强
Oxidative DNA damage and augmentation of poly(ADP-ribose) polymerase/nuclear factor-kappa B signaling in patients with type 2 diabetes and microangiopathy.
作者信息
Adaikalakoteswari Antonysunil, Rema Mohan, Mohan Viswanathan, Balasubramanyam Muthuswamy
机构信息
Department of Cell and Molecular Biology, Madras Diabetes Research Foundation & Dr.Mohan's Diabetes Specialities Centre, 4 Conran Smith Road, Gopalapuram, Chennai 600086, India.
出版信息
Int J Biochem Cell Biol. 2007;39(9):1673-84. doi: 10.1016/j.biocel.2007.04.013. Epub 2007 Apr 25.
Although oxidative stress and the subsequent DNA damage is one of the obligatory signals for poly(ADP-ribose) polymerase (PARP) activation and nuclear factor-kappa B (NFkappaB) alterations, these molecular aspects have not been collectively examined in epidemiological and clinical settings. Therefore, this study attempts to assess the oxidative DNA damage and its downstream effector signals in peripheral blood lymphocytes from Type 2 diabetes subjects without and with microangiopathy along with age-matched non-diabetic subjects. The basal DNA damage, lipid peroxidation and protein carbonyl content were significantly (p<0.05) higher in patients with and without microangiopathy compared to control subjects. Formamido Pyrimidine Glycosylase (FPG)-sensitive DNA strand breaks which represents reliable indicator of oxidative DNA damage were also significantly (p<0.001) higher in diabetic patients with (19.41+/-2.5) and without microangiopathy (16.53+/-2.0) compared to control subjects (1.38+/-0.85). Oxidative DNA damage was significantly correlated to poor glycemic control. PARP mRNA expression and PARP activity were significantly (p<0.05) increased in cells from diabetic patients with (0.31+/-0.03 densitometry units; 0.22+/-0.02PARPunits/mgprotein, respectively) and without (0.35+/-0.02; 0.42+/-0.05) microangiopathy compared to control (0.19+/-0.02; 0.11+/-0.02) subjects. Diabetic subjects with and without microangiopathy exhibited a significantly (p<0.05) higher (80%) NFkappaB binding activity compared to control subjects. In diabetic patients, FPG-sensitive DNA strand breaks correlated positively with PARP gene expression, PARP activity and NFkappaB binding activity. This study provides a comprehensive molecular evidence for increased oxidative stress and genomic instability in Type 2 diabetic subjects even prior to vascular pathology and hence reveals a window of opportunity for early therapeutic intervention.
尽管氧化应激及随后的DNA损伤是聚(ADP - 核糖)聚合酶(PARP)激活和核因子-κB(NFκB)改变的必要信号之一,但这些分子层面的因素尚未在流行病学和临床环境中进行综合研究。因此,本研究试图评估2型糖尿病无微血管病变和有微血管病变患者以及年龄匹配的非糖尿病患者外周血淋巴细胞中的氧化性DNA损伤及其下游效应信号。与对照组相比,有和无微血管病变的患者基础DNA损伤、脂质过氧化和蛋白质羰基含量均显著更高(p<0.05)。代表氧化性DNA损伤可靠指标的甲酰胺嘧啶糖基化酶(FPG)敏感的DNA链断裂在有微血管病变(19.41±2.5)和无微血管病变(16.53±2.0)的糖尿病患者中也显著更高(p<0.001),而对照组为(1.38±0.85)。氧化性DNA损伤与血糖控制不佳显著相关。与对照组(分别为0.19±0.02密度测定单位;0.11±0.02 PARP单位/毫克蛋白质)相比,有微血管病变(分别为0.31±0.03密度测定单位;0.22±0.02 PARP单位/毫克蛋白质)和无微血管病变(0.35±0.02;0.42±0.05)的糖尿病患者细胞中PARP mRNA表达和PARP活性均显著增加(p<0.05)。与对照组相比,有和无微血管病变的糖尿病患者NFκB结合活性均显著更高(p<0.05)(高80%)。在糖尿病患者中,FPG敏感的DNA链断裂与PARP基因表达、PARP活性和NFκB结合活性呈正相关。本研究为2型糖尿病患者即使在血管病变之前氧化应激增加和基因组不稳定提供了全面的分子证据,因此揭示了早期治疗干预的机会窗口。
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