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在细胞核中过表达人过氧化氢酶的小鼠体内,DNA损伤水平未发生改变。

Levels of DNA damage are unaltered in mice overexpressing human catalase in nuclei.

作者信息

Schriner S E, Ogburn C E, Smith A C, Newcomb T G, Ladiges W C, Dollé M E, Vijg J, Fukuchi K, Martin G M

机构信息

Department of Genetics, University of Washington, Seattle, WA 98195-7470, USA.

出版信息

Free Radic Biol Med. 2000 Oct 1;29(7):664-73. doi: 10.1016/s0891-5849(00)00352-x.

Abstract

Two types of transgenic mice were generated to evaluate the role of hydrogen peroxide in the formation of nuclear DNA damage. One set of lines overexpresses wild-type human catalase cDNA, which is localized to peroxisomes. The other set overexpresses a human catalase construct that is targeted to the nucleus. Expression of the wild-type human catalase transgene was found in liver, kidney, skeletal muscle, heart, spleen, and brain with muscle and heart exhibiting the highest levels. Animals containing the nuclear-targeted construct had a similar pattern of expression with the highest levels in muscle and heart, but with lower levels in liver and spleen. In these animals, immunofluorescence detected catalase present in the nuclei of kidney, muscle, heart, and brain. Both types of transgenic animals had significant increases of catalase activities compared to littermate controls in most tissues examined. Despite enhanced activities of catalase, and its presence in the nucleus, there were no changes in levels of 8OHdG, a marker of oxidative damage to DNA. Nor were there differences in mutant frequencies at a Lac Z reporter transgene. This result suggests that in vivo levels of H(2)O(2) may not generate 8OHdG or other types of DNA damage. Alternatively, antioxidant defenses may be optimized such that additional catalase is unable to further protect nuclear DNA against oxidative damage.

摘要

为了评估过氧化氢在核DNA损伤形成中的作用,构建了两种转基因小鼠。一组品系过表达定位于过氧化物酶体的野生型人过氧化氢酶cDNA。另一组过表达靶向细胞核的人过氧化氢酶构建体。在肝脏、肾脏、骨骼肌、心脏、脾脏和大脑中均发现了野生型人过氧化氢酶转基因的表达,其中肌肉和心脏中的表达水平最高。含有核靶向构建体的动物具有相似的表达模式,肌肉和心脏中的表达水平最高,但肝脏和脾脏中的表达水平较低。在这些动物中,免疫荧光检测到肾脏、肌肉、心脏和大脑细胞核中存在过氧化氢酶。与同窝对照相比,在大多数检测组织中,两种类型的转基因动物的过氧化氢酶活性均显著增加。尽管过氧化氢酶活性增强且存在于细胞核中,但作为DNA氧化损伤标志物的8-羟基脱氧鸟苷(8OHdG)水平并未改变。Lac Z报告基因转基因的突变频率也没有差异。这一结果表明,体内过氧化氢(H₂O₂)水平可能不会产生8OHdG或其他类型的DNA损伤。或者,抗氧化防御机制可能已得到优化,以至于额外的过氧化氢酶无法进一步保护核DNA免受氧化损伤。

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