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鉴定导致人类疾病的三核苷酸重复序列的猪同源序列。

Identification of the porcine homologous of human disease causing trinucleotide repeat sequences.

作者信息

Madsen Lone Bruhn, Thomsen Bo, Sølvsten Christina Ane Elisabeth, Bendixen Christian, Fredholm Merete, Jørgensen Arne Lund, Nielsen Anders Lade

机构信息

Section for Molecular Genetics and Systems Biology, Department of Genetics and Biotechnology, Danish Institute of Agricultural Sciences, Tjele, Denmark.

出版信息

Neurogenetics. 2007 Aug;8(3):207-18. doi: 10.1007/s10048-007-0088-y. Epub 2007 May 22.

DOI:10.1007/s10048-007-0088-y
PMID:17516099
Abstract

Expansion in the repeat number of intragenic trinucleotide repeats (TNRs) is associated with a variety of inherited human neurodegenerative diseases. To study the composition of TNRs in a mammalian species representing an evolutionary intermediate between humans and rodents, we describe in this paper the identification of porcine noncoding and polyglutamine-encoding TNR regions and the comparison to the homologous TNRs from human, chimpanzee, dog, opossum, rat, and mouse. Several of the porcine TNR regions are highly polymorphic both within and between different breeds. The TNR regions are more conserved in terms of repeat length between humans and pigs than between humans and rodents suggesting that TNR lengths could be implicated in mammalian evolution. The TNRs in the FMR2, SCA6, SCA12, and Huntingtin genes are comparable in length to alleles naturally occurring in humans, and also in FMR1, a long uninterrupted CGG TNR was identified. Most strikingly, we identified a Huntingtin allele with 21 uninterrupted CAG repeats encoding a stretch of 24 polyglutamines. Examination of this particular Huntingtin TNR in 349 porcine offspring showed stable transmission. The presence in the porcine genome of TNRs within genes that, in humans, can undergo pathogenic expansions support the usage of the pig as an alternative animal model for studies of TNR evolution, stability, and functional properties.

摘要

基因内三核苷酸重复序列(TNRs)重复数目的扩增与多种人类遗传性神经退行性疾病相关。为了研究在代表人类和啮齿动物进化中间体的哺乳动物物种中TNRs的组成,我们在本文中描述了猪非编码和聚谷氨酰胺编码TNR区域的鉴定,并与来自人类、黑猩猩、狗、负鼠、大鼠和小鼠的同源TNRs进行了比较。几个猪TNR区域在不同品种内和品种间都具有高度多态性。与人类和啮齿动物之间相比,人类和猪之间的TNR区域在重复长度方面更保守,这表明TNR长度可能与哺乳动物进化有关。FMR2、SCA6、SCA12和亨廷顿基因中的TNRs长度与人类中自然存在的等位基因相当,并且在FMR1中,还鉴定出了一个长的不间断CGG TNR。最引人注目的是,我们鉴定出了一个具有21个不间断CAG重复序列的亨廷顿等位基因,其编码一段24个聚谷氨酰胺。对349头猪后代中这个特定的亨廷顿TNR进行检测,结果显示其传递稳定。在猪基因组中,人类中可发生致病性扩增的基因内存在TNRs,这支持将猪用作研究TNR进化、稳定性和功能特性的替代动物模型。

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本文引用的文献

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Duplication of Atxn1l suppresses SCA1 neuropathology by decreasing incorporation of polyglutamine-expanded ataxin-1 into native complexes.Atxn1l的复制通过减少多聚谷氨酰胺扩展的ataxin-1掺入天然复合物来抑制SCA1神经病理学。
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