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Molecular characterization of selenoproteins based on decreased glutathione peroxidase activity in preeclampsia

机译:子痫前期基于谷胱甘肽过氧化物酶活性降低的硒蛋白分子表征

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Glutathione peroxidase (GPx) and other selenoproteins (SeP) are involved in the detoxification of reactive oxygen species (ROS). ROS is implicated in preeclampsia (PE). Generation of ROS and antioxidant effect of total GPx in women with PE was estimated. Since we found a significant decrease in total GPx level of women with PE, we were motivated to characterize at a molecular level SeP present in GPx (GPx 1-4, 6). Other SeP including selenoprotein P (SEPP), selenoprotein S (SELS) and thioredoxin reductase (TXNRD) were also analyzed since literature suggests that they also play a critical role in down regulation of oxidative stress (OS) in PE. Non SeP GPx were also analyzed for comparison purposes. Serum GPx was measured in venous blood samples of women with PE (Group A; n=25) and normotensive pregnant women (Group B; n=32) spectrophotometrically. Intracellular ROS generated by peripheral blood mononuclear cells was measured using flow cytometry. Molecular characterization of the SeP was done by sequence analysis at nucleotide, codon and amino acid levels. Intracellular ROS level was significantly increased in Group A as compared to Group B. ROS and GPx were significantly negatively correlated in both Group A and Group B. SePs involved in PE, primarily belonged to two nucleotide biasing groups, AT and GC. Dinucleotide usage and codon preferences in these two groups were found to be in accordance with their respective compositional bias. Such nucleotide compositional bias seemed to be major factor driving their selective codon choices. These SePs differ within themselves with respect to their relative amino acid abundance.
机译:谷胱甘肽过氧化物酶(GPx)和其他硒蛋白(SeP)参与活性氧(ROS)的解毒。 ROS与先兆子痫(PE)有关。估计PE妇女中ROS的产生和总GPx的抗氧化作用。由于我们发现患有PE的女性的总GPx水平显着下降,因此我们有动机以GPx中存在的分子水平SeP进行表征(GPx 1-4、6)。还对其他SeP进行了分析,包括硒蛋白P(SEPP),硒蛋白S(SELS)和硫氧还蛋白还原酶(TXNRD),因为文献表明它们在PE氧化应激(OS)的下调中也起着关键作用。还比较了非SeP GPx,以进行比较。用分光光度法测定PE妇女(A组; n = 25)和血压正常孕妇(B组; n = 32)的静脉血样本中的血清GPx。使用流式细胞术测量由外周血单核细胞产生的细胞内ROS。通过在核苷酸,密码子和氨基酸水平上的序列分析来完成SeP的分子表征。与B组相比,A组的细胞内ROS水平显着增加。A组和B组中ROS和GPx均显着负相关。PE中涉及的SePs主要属于两个核苷酸偏向组:AT和GC。发现这两组中的二核苷酸用法和密码子偏好性是根据它们各自的组成偏差而定的。这种核苷酸组成的偏差似乎是驱动其选择性密码子选择的主要因素。这些SeP在其内部的相对氨基酸丰度方面有所不同。

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