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斑马鱼(Danio rerio)XPD 基因的分子克隆与表达分析。

Molecular cloning and expression analysis of xpd from zebrafish (Danio rerio).

机构信息

Department of Biomedical Sciences and Medicine, University of Algarve, Faro, Portugal.

出版信息

Mol Biol Rep. 2012 May;39(5):5339-48. doi: 10.1007/s11033-011-1333-x. Epub 2011 Dec 21.

DOI:10.1007/s11033-011-1333-x
PMID:22187342
Abstract

The XPD gene, located in human chromosome 19, encodes one of the two helicase components of transcriptional factor IIH (TFIIH), a ten-subunit, multifunctional complex that is essential for multiple processes, including basal transcription initiation and DNA damage repair [1, 2]. Alterations in XPD resulting in defective TFIIH function are associated with UV-sensitive disorders including Xeroderma pigmentosum, Cockayne syndrome, and Trichothiodystrophy (TTD) [3, 4]. TTD mice exhibit many symptoms of premature aging, including osteoporosis, kyphosis and osteosclerosis [5]. This fact has triggered our interest in analyzing XPD involvement in bone biology using zebrafish as model organism. Although orthologs of xpd are present in all species analyzed, no specific data on its gene structure, regulation or function exists at this time in any fish system. In this study we isolated the zebrafish cDNA encoding xpd, and examined its spatial-temporal expression during early development as well as its tissue distribution in adult zebrafish. Only one gene was identified in zebrafish and its sequence analysis showed a molecular structure with 23 coding exons similar to other species. The amino acid sequences were also found to be largely conserved among all species analyzed, suggesting function maintenance throughout evolution. Gene expression analysis in different zebrafish tissues by qPCR showed xpd expression in all tissues examined with the highest expression in branchial arches. Analysis of xpd expression in zebrafish embryos showed maternal inheritance and presence of xpd transcripts in all developmental stages analyzed suggesting its implication in early zebrafish larval development.

摘要

XPD 基因位于人类染色体 19 上,编码转录因子 IIH(TFIIH)的两个解旋酶组件之一。TFIIH 是一个由十个亚基组成的多功能复合物,是多种过程所必需的,包括基础转录起始和 DNA 损伤修复[1,2]。导致 TFIIH 功能缺陷的 XPD 改变与包括 Xeroderma pigmentosum、Cockayne syndrome 和 Trichothiodystrophy(TTD)在内的紫外线敏感疾病有关[3,4]。TTD 小鼠表现出许多早衰症状,包括骨质疏松症、脊柱后凸和骨硬化症[5]。这一事实激发了我们使用斑马鱼作为模型生物分析 XPD 在骨生物学中的作用的兴趣。尽管在所有分析的物种中都存在 xpd 的同源物,但目前在任何鱼类系统中都没有关于其基因结构、调控或功能的具体数据。在这项研究中,我们分离了编码 xpd 的斑马鱼 cDNA,并在早期发育过程中检查了其时空表达,以及在成年斑马鱼中的组织分布。在斑马鱼中只鉴定出一个基因,其序列分析显示出具有 23 个编码外显子的分子结构,与其他物种相似。氨基酸序列在所有分析的物种中也发现高度保守,表明在进化过程中保持功能。qPCR 分析不同斑马鱼组织中的基因表达显示,xpd 在所有检查的组织中表达,在鳃弓中表达最高。在斑马鱼胚胎中分析 xpd 表达显示母系遗传,并且在分析的所有发育阶段都存在 xpd 转录本,表明其在早期斑马鱼幼虫发育中的作用。

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本文引用的文献

1
A history of TFIIH: two decades of molecular biology on a pivotal transcription/repair factor.TFIIH 历史:二十年的关键转录/修复因子的分子生物学研究。
DNA Repair (Amst). 2011 Jul 15;10(7):714-21. doi: 10.1016/j.dnarep.2011.04.021. Epub 2011 May 17.
2
On the traces of XPD: cell cycle matters - untangling the genotype-phenotype relationship of XPD mutations.XPD 踪迹:细胞周期很重要——解开 XPD 突变的基因型-表型关系。
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Structure of the DNA repair helicase XPD.DNA修复解旋酶XPD的结构
利用基于转录的DNA修复试验鉴定低分子量卵黄生成素1(Vg1)样蛋白作为斑马鱼(Danio rerio)发育过程中的核苷酸切除修复(NER)因子。
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Cell Res. 2007 Feb;17(2):163-73. doi: 10.1038/sj.cr.7310144.
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The DNA repair helicases XPD and FancJ have essential iron-sulfur domains.DNA修复解旋酶XPD和FancJ具有重要的铁硫结构域。
Mol Cell. 2006 Sep 15;23(6):801-8. doi: 10.1016/j.molcel.2006.07.019.
6
An Xpd mouse model for the combined xeroderma pigmentosum/Cockayne syndrome exhibiting both cancer predisposition and segmental progeria.一种兼具着色性干皮病/科凯恩综合征特征、表现出癌症易感性和节段性早衰的Xpd小鼠模型。
Cancer Cell. 2006 Aug;10(2):121-32. doi: 10.1016/j.ccr.2006.05.027.
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