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一种新型唐氏综合征小鼠模型,携带一个人类人工染色体(HAC),其中包含来自人类 21 号染色体的少量基因。

A novel mouse model for Down syndrome that harbor a single copy of human artificial chromosome (HAC) carrying a limited number of genes from human chromosome 21.

机构信息

Laboratory of Gene Medicine, Keio University School of Medicine, 35 Shinanomachi, Shinjuku-ku, Tokyo, 160-8582, Japan.

出版信息

Transgenic Res. 2014 Apr;23(2):317-29. doi: 10.1007/s11248-013-9772-x. Epub 2013 Nov 30.

Abstract

Down syndrome (DS), also known as Trisomy 21, is the most common chromosome aneuploidy in live-born children and displays a complicated symptom. To date, several kinds of mouse models have been generated to understand the molecular pathology of DS, yet the gene dosage effects and gene(s)-phenotype(s) correlation are not well understood. In this study, we established a novel method to generate a partial trisomy mice using the mouse ES cells that harbor a single copy of human artificial chromosome (HAC), into which a small human DNA segment containing human chromosome 21 genes cloned in a bacterial artificial chromosome (BAC) was recombined. The produced mice were found to maintain the HAC carrying human genes as a mini-chromosome, hence termed as a Trans-Mini-Chromosomal (TMC) mouse, and HAC was transmitted for more than twenty generations independent from endogenous mouse chromosomes. The three human transgenes including cystathionine β-synthase, U2 auxiliary factor and crystalline alpha A were expressed in several mouse tissues with various expression levels relative to mouse endogenous genes. The novel system is applicable to any of human and/or mouse BAC clones. Thus, the TMC mouse carrying a HAC with a limited number of genes would provide a novel tool for studying gene dosage effects involved in the DS molecular pathogenesis and the gene(s)-phenotype(s) correlation.

摘要

唐氏综合征(DS),又称 21 三体,是活产儿中最常见的染色体非整倍体,表现出复杂的症状。迄今为止,已经生成了多种小鼠模型来了解 DS 的分子病理学,但基因剂量效应和基因-表型相关性尚不清楚。在这项研究中,我们建立了一种使用携带人类人工染色体(HAC)的单个拷贝的小鼠胚胎干细胞(ES 细胞)来生成部分三体小鼠的新方法,在该 HAC 中重组了一个包含人类染色体 21 基因的克隆在细菌人工染色体(BAC)中的小人类 DNA 片段。发现产生的小鼠保持携带人类基因的 HAC 作为微型染色体,因此称为跨微型染色体(TMC)小鼠,并且 HAC 独立于内源性小鼠染色体传递了二十多代。三个人类转基因包括胱硫醚 β-合酶、U2 辅助因子和结晶 αA 在几种小鼠组织中表达,相对于小鼠内源性基因具有不同的表达水平。该新型系统适用于任何人类和/或小鼠 BAC 克隆。因此,携带有限数量基因的 HAC 的 TMC 小鼠将为研究涉及 DS 分子发病机制和基因-表型相关性的基因剂量效应提供一种新工具。

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