8-hydroxyguanine

8 - 羟基鸟嘌呤
  • 文章类型: Journal Article
    DNA损伤的产生导致突变并因此导致癌症。活性氧是在人类癌症中发现的DNA损伤和一些突变特征的重要来源。8-氧代-7,8-二氢鸟嘌呤(GO,8-羟基鸟嘌呤)是最丰富的氧化碱基之一,并在修饰位点诱导G→T颠换突变。受损的G碱基还导致人类细胞中5'-GpA-3'二核苷酸G碱基的非靶向碱基置换突变(远距离作用突变),和胞嘧啶脱氨酶载脂蛋白BmRNA编辑酶,催化多肽样3(APOBEC3)参与突变过程。脱氨基的胞嘧啶,即,尿嘧啶,预计尿嘧啶DNA糖基化酶会去除碱基。5'-GpA-3'的G碱基处的大多数取代突变可能是由糖基化酶形成的无碱基位点引起的。在这项研究中,我们在人U2OS细胞中表达了来自枯草芽孢杆菌噬菌体PBS2的尿嘧啶DNA糖基化酶抑制剂,并研究了其对GO诱导的作用距离突变的影响.尿嘧啶DNA糖基化酶的抑制增加了突变频率,特别是,G→A跃迁的频率。这些结果表明尿嘧啶DNA糖基化酶,除APOBEC3外,还参与GO诱导的非靶向突变过程。
    The generation of DNA damage causes mutations and consequently cancer. Reactive oxygen species are important sources of DNA damage and some mutation signatures found in human cancers. 8-Oxo-7,8-dihydroguanine (GO, 8-hydroxyguanine) is one of the most abundant oxidized bases and induces a G→T transversion mutation at the modified site. The damaged G base also causes untargeted base substitution mutations at the G bases of 5\'-GpA-3\' dinucleotides (action-at-a-distance mutations) in human cells, and the cytosine deaminase apolipoprotein B mRNA-editing enzyme, catalytic polypeptide-like 3 (APOBEC3) is involved in the mutation process. The deaminated cytosine, i.e., uracil, bases are expected to be removed by uracil DNA glycosylase. Most of the substitution mutations at the G bases of 5\'-GpA-3\' might be caused by abasic sites formed by the glycosylase. In this study, we expressed the uracil DNA glycosylase inhibitor from Bacillus subtilis bacteriophage PBS2 in human U2OS cells and examined the effects on the GO-induced action-at-a-distance mutations. The inhibition of uracil DNA glycosylase increased the mutation frequency, and in particular, the frequency of G→A transitions. These results indicated that uracil DNA glycosylase, in addition to APOBEC3, is involved in the untargeted mutation process induced by GO.
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  • 文章类型: Journal Article
    DNA氧化是对基因组完整性的严重威胁,并参与突变和癌症的发生。G底座最常损坏,和8-氧代-7,8-二氢鸟嘌呤(GO,8-羟基鸟嘌呤)是主要的受损碱基之一。在人类细胞中,GO在修饰的位点引起G:C﹤T:transversion突变,并且还在5'-GpA-3'二核苷酸的G碱基处诱导非靶向置换突变(作用在距离突变)。5'-GpA-3'序列与5'-TpC-3'序列互补,载脂蛋白BmRNA编辑酶的首选底物,催化多肽样3(APOBEC3)胞嘧啶脱氨酶,因此,它们对诱变的贡献已被考虑。在这项研究中,APOBEC3B,人类U2OS细胞中最丰富的APOBEC3蛋白,在人类U2OS细胞中被击倒,然后将GO-穿梭质粒转染到细胞中。通过击倒,在距离上的作用突变减少到~25%,表明在该细胞系中,GO诱导的作用-距离突变高度依赖于APOBEC3B。
    DNA oxidation is a serious threat to genome integrity and is involved in mutations and cancer initiation. The G base is most frequently damaged, and 8-oxo-7,8-dihydroguanine (GO, 8-hydroxyguanine) is one of the predominant damaged bases. In human cells, GO causes a G:C→T:A transversion mutation at the modified site, and also induces untargeted substitution mutations at the G bases of 5\'-GpA-3\' dinucleotides (action-at-a-distance mutations). The 5\'-GpA-3\' sequences are complementary to the 5\'-TpC-3\' sequences, the preferred substrates for apolipoprotein B mRNA-editing enzyme, catalytic polypeptide-like 3 (APOBEC3) cytosine deaminases, and thus their contribution to mutagenesis has been considered. In this study, APOBEC3B, the most abundant APOBEC3 protein in human U2OS cells, was knocked down in human U2OS cells, and a GO-shuttle plasmid was then transfected into the cells. The action-at-a-distance mutations were reduced to ~25% by the knockdown, indicating that GO-induced action-at-a-distance mutations are highly dependent on APOBEC3B in this cell line.
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  • 文章类型: Journal Article
    许多报道发现Cd诱导植物中活性氧(ROS)的形成。然而,通常会研究一般的ROS池,没有区别的生产场所。在本研究中,我们使用了一种线粒体特异性抗氧化剂,MitoTEMPO,阐明线粒体衍生的ROS在大豆幼苗对短期(48h)Cd胁迫的响应中的作用。结果表明,Cd引起根长和鲜重的减少,超氧阴离子水平的增加,过氧化氢,脂质过氧化标记物(硫代巴比妥反应性物质,TBARS)和RNA氧化标记(8-羟基鸟苷,8-OHG)在幼苗根中。MitoTEMPO的应用以剂量依赖性方式影响Cd的吸收,并减少了Cd依赖性的超氧阴离子和脂质过氧化的诱导。
    Numerous reports find that Cd induces formation of reactive oxygen species (ROS) in plants. However, a general ROS pool is usually studied, without distinction of their production site. In the present study, we applied a mitochondria-specific antioxidant, MitoTEMPO, to elucidate the role of mitochondria-derived ROS in the response of soybean seedlings to short-term (48 h) Cd stress. The obtained results showed that Cd caused a reduction in root length and fresh weight and increase in the level of superoxide anion, hydrogen peroxide, markers of lipid peroxidation (thiobarbituric reactive substances, TBARS) and markers of RNA oxidation (8-hydroxyguanosine, 8-OHG) in seedling roots. Application of MitoTEMPO affected Cd uptake in a dose-dependent manner and diminished the Cd-dependent induction of superoxide anion and lipid peroxidation.
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  • 文章类型: Journal Article
    8-氧代-7,8-二氢鸟嘌呤(8-羟基鸟嘌呤,G°)是一种主要的氧化碱,被认为在各种疾病的发病机理中起关键作用,包括癌症.G°在损伤位点诱导G:C→T:在5'-GpA序列的G碱基的非靶向(在距离作用)突变。在这项研究中,我们检查了作用-距离突变的分布以及相对于G°的复制起点位置对非靶向诱变的影响。将G°碱基引入两个穿梭质粒中,各自在相对于supF基因的不同位置具有SV40复制起点。氧化的碱基位于上游或下游位点(基因外部),或编码基因pre-tRNA序列的区域的中心,在这个意义上的链。将这些穿梭质粒导入人U2OS细胞。当G°碱基位于supF基因的下游而不是该基因的上游时,在距离上的作用突变被更频繁地诱导。此外,当SV40起源存在于G°碱基的5'侧,观察到更多的作用在距离上的突变。这些结果表明,远距离作用突变主要在病变的5'侧诱导,并且当受损碱基位于滞后链模板上时发生的频率更高。
    8-Oxo-7,8-dihydroguanine (8-hydroxyguanine, G°) is a major oxidized base that is considered to play pivotal roles in the pathogenesis of various diseases, including cancer. G° induces G:C → T:A transversions at the damage site and untargeted (action-at-a-distance) mutations of G bases at 5\'-GpA sequences. In this study, we examined the distribution of the action-at-a-distance mutations and the effects of the replication origin position relative to G° on the untargeted mutagenesis. The G° base was introduced into two shuttle plasmids, each with the SV40 replication origin at a different position with respect to the supF gene. The oxidized base was located at an upstream or downstream site (outside of the gene), or the center of the region encoding the pre-tRNA sequence of the gene, in the sense strand. These shuttle plasmids were introduced into human U2OS cells. The action-at-a-distance mutations were more frequently induced when the G° base was located downstream of the supF gene than upstream of the gene. In addition, more action-at-a-distance mutations were observed when the SV40 origin was present on the 5\'-side of the G° base. These results indicated that the action-at-a-distance mutations are predominantly induced on the 5\'-side of the lesion and occurred more frequently when the damaged base was located on the lagging strand template.
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  • 文章类型: Journal Article
    虽然大量文献显示了非法药物使用的健康问题,需要研究药物滥用如何影响血液中的DNA损伤和污染物,尤其是受铅污染的鸦片。这项试点研究旨在评估铅(Pb)的水平,8-羟基二鸟嘌呤(8-氧代-瓜),鸦片成瘾者和非成瘾者血清中的丙二醛(MDA)。本研究是横断面设计的病例对照研究。本研究采用方便和随机抽样的方法,选取了50名鸦片成瘾者和非成瘾者的样本。参与者分为两组:成瘾者和非成瘾者。采用原子吸收光谱法测定Pb的含量,采用酶联免疫吸附试验(ELISA)方法测定8-氧代-瓜和MDA的含量。使用独立t检验分析数据。结果表明,成瘾者男女血清中铅含量均高于非成瘾者男女,对于研究参与者(p值=0.001)。对于8-oxo-Gua(女性p值=0.647,男性p值=0.785)和MDA(女性p值=0.867,男性p值=0.995),男性和非成瘾者的血液水平没有显着差异。总的来说,在这项初步研究中,发现成瘾者的血液铅水平大大高于正常的非成瘾者。因此,在症状尚无定论的情况下,对成瘾者的血铅水平进行检测可能会提供信息。
    While a large body of literature has shown the health problems of illicit drug use, research is needed on how substance abuse impacts DNA damage and contaminants in blood, especially given Pb-contaminated opium. This pilot study aimed to evaluate the levels of lead (Pb), 8-hydroxy di-guanine (8-oxo-Gua), and malondialdehyde (MDA) in the blood serum of opium addicts and non-addict people. The current study is a case-control study with a cross-sectional design. A sample of 50 opium-addicted and non-addict adults were chosen for this study using convenience and random sampling methods. Participants were divided into two groups: addicts and non-addicts. The atomic absorption spectroscopy method was used to measure the quantity of Pb, and the Enzyme-Linked Immunosorbent Assay (ELISA) method was used to measure the amount of 8-oxo-Gua and MDA. The data were analyzed using an independent t-test. The results show that the amount of Pb in the blood serum of addicted women and men was higher than levels in non-addict men and women, for the study participants (p-value = 0.001). Blood levels were not significantly different between addicts and non-addicts for men or women for 8-oxo-Gua (p-value = 0.647 for women and p-value = 0.785 for men) and MDA (p-value = 0.867 for women and p-value = 0.995 for men). In general, addicts\' blood Pb levels were found to be substantially higher than those of normal non-addict persons in this pilot study. As a result, testing for blood Pb levels in addicts may be informative in instances when symptoms are inconclusive.
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  • 文章类型: Journal Article
    氧化损伤的碱基诱导突变并参与癌症的发生。8-氧代-7,8-二氢鸟嘌呤(G°,8-羟基鸟嘌呤)是一种丰富的氧化碱基,可诱导人体细胞中的靶向G:C→T:A颠换,以及5'-GpA-3'二核苷酸G碱基的非靶向碱基取代(远距离作用)突变。当Werner综合征(WRN)蛋白的数量减少时,作用在距离上的突变变得比靶向的颠覆性更频繁。在这项研究中,OGG1,受损碱基的主要DNA糖基化酶,和WRN在人U2OS细胞中被分离和组合敲除,并将携带G°的穿梭质粒引入敲除细胞中。有趣的是,在WRN加OGG1双敲低细胞中观察到较少的作用在距离上的突变,与WRN单敲低细胞相比。这些结果表明OGG1的自相矛盾的作用,它是氧化鸟嘌呤碱基作用的距离突变的促进剂。
    Oxidatively damaged bases induce mutations and are involved in cancer initiation. 8-Oxo-7,8-dihydroguanine (G°, 8-hydroxyguanine) is an abundant oxidized base that induces targeted G:C→T:A transversions in human cells, as well as untargeted base substitution (action-at-a-distance) mutations of the G bases of 5\'-GpA-3\' dinucleotides. The action-at-a-distance mutations become more frequent than the targeted transversions when the amount of Werner syndrome (WRN) protein is decreased. In this study, OGG1, the major DNA glycosylase for the damaged base, and WRN were knocked down in isolation and in combination in human U2OS cells, and a shuttle plasmid carrying G° was introduced into the knockdown cells. Interestingly, fewer action-at-a-distance mutations were observed in the WRN plus OGG1 double knockdown cells, as compared to the WRN single knockdown cells. These results indicated the paradoxical role of OGG1, as an accelerator of the action-at-a-distance mutations by the oxidized guanine base.
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  • 文章类型: Journal Article
    UNASSIGNED: Cellular RNA is less compact than DNA, more easily accessible to ROS and therefore could be more susceptible to oxidative damage. This study was conceived in order to analyze the RNA oxidative damage in the urine of patients undergoing operation for colorectal cancer (CRC), to compare with healthy controls, and correlate with the stage.
    UNASSIGNED: The study population was constituted by a group of 147 patients and a group of 128 healthy controls. Urine and blood samples were collected before the colonoscopy in all participants and 24 hours post-operatively for those who underwent surgery. Urine 8-hydroxyguanine (8-OHG) was determined as marker of RNA oxidation, and serum uric acid (UA) as antioxidant marker.
    UNASSIGNED: Preoperatively, 8-OHG (ng/ml) values of CRC patients were found to be significantly higher than those of controls (p = 0.001). More specifically, stages II/III had significantly higher 8-OHG values (p < 0.001 and p = 0.007) than stages 0/I. Post-operatively, 8-OHG values were similar to controls (p = 0.053). Preoperatively, UA values (mg/dl) were significantly lower (p = 0.001), while postoperatively were similar to controls (p = 0.069).
    UNASSIGNED: Oxidative RNA damage occurs in CRC patients. Stages II/III are associated with higher values of 8-OHG than stages 0/I. 8-OHG could act as a marker for the identification of patients with advanced disease.
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  • 文章类型: Journal Article
    在这里,通过超声化学路线在40kHz和50W的超声辐照浴下制备了铜铁氧体纳米颗粒(CuFe2O4NPs)/壳聚糖的合成。通过简单的超声方法,使用与生物聚合物配位的铜铁氧体纳米颗粒的组合物开发了高灵敏度和稳定的改性电化学传感器。此外,功率和频率参数对于声化学合成和特别是结构非常重要,以及在超声辐照时间内纳米材料发展的尺寸。在这项工作中,用超声波浴在40kHz、1h的条件下合成了CuFe2O4纳米材料。用FESEM对CuFe2O4/壳聚糖进行了表征,EDX,XRD和电化学方法。此外,8-羟基鸟嘌呤是氧化应激的生物标志物之一。细胞内8-羟基鸟嘌呤的浓度是人体氧化应激的量度。因此,血清样品中8-羟基鸟嘌呤的高特异性测定是最重要的。CuFe2O4/壳聚糖修饰电极显示出8.6nM的低检测限和长线性范围(0.025-697.175µM)。
    Herein, the synthesis of copper ferrite nanoparticles (CuFe2O4 NPs)/chitosan have been prepared by sonochemical route under ultrasonic irradiation bath at 40 kHz and 50 W. A high sensitive and stable modified electrochemical sensor was developed using a composition of copper ferrite nanoparticles coordinated with biopolymer through a facile ultrasound approach. Besides, power and frequency parameters are highly important for sonochemical synthesis and specifically structure, and size of the nanomaterials development during the ultrasonic irradiation time. In this work, ultrasonic bath was used to synthesis of CuFe2O4 nanomaterial at 40 kHz with 1 h. CuFe2O4/chitosan was characterized by FESEM, EDX, XRD and electrochemical methods. Furthermore, 8-hydroxyguanine is one of biomarker by oxidative stress. The concentrations of 8-hydroxyguanine within a cell are a measurement of oxidative stress in human body. Consequently, the measurement of 8-hydroxyguanine in blood serum samples with high specificity is of greatest importance. The CuFe2O4/chitosan modified electrode is displayed a low detection limit of 8.6 nM and long linear range (0.025-697.175 µM).
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  • 文章类型: Journal Article
    UNASSIGNED: Oxidative stress leads to many kinds of diseases. Currently, urinary 8-hydroxydeoxyguanosine (8-OHdG) is widely measured as an oxidative stress biomarker. There is a specific advantage if saliva can be used as the sample to measure the oxidative stress biomarker, because saliva is much easier to collect than urine. In this study, we investigated the measurement of 8-hydroxyguanine (8-OHGua) as an oxidative stress marker in saliva, by a column switching HPLC system equipped with an electrochemical detector (HPLC-ECD).
    UNASSIGNED: The 8-OHGua in saliva could be detected as a single peak by HPLC-ECD. The average level of 8-OHGua in saliva was 3.80 ng/mL in ordinary, non-smoking subjects. The salivary 8-OHGua levels of smokers were significantly higher than those of non-smokers.
    UNASSIGNED: Salivary 8-OHGua may be a useful noninvasive and promising oxidative stress biomarker.
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  • 文章类型: Review
    鸟嘌呤氧化发生在DNA和细胞核苷酸池中,主要产物之一是8-羟基鸟嘌呤(8-氧代-7,8-二氢鸟嘌呤)。已在各种实验系统中检查了这种氧化碱的诱变潜力。在这次审查中,我们总结了碱基在哺乳动物细胞中的致突变性。我们还描述了专门的DNA聚合酶的作用,DNA修复蛋白,和核苷酸池消毒酶。
    Guanine oxidation occurs in both DNA and the cellular nucleotide pool, and one of the major products is 8-hydroxyguanine (8-oxo-7,8-dihydroguanine). The mutagenic potentials of this oxidized base have been examined in various experimental systems. In this review, we summarize the mutagenicity of the base in mammalian cells. We also describe the effects of specialized DNA polymerases, DNA repair proteins, and nucleotide pool sanitization enzymes.
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