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在来自DM1转基因小鼠的精原细胞中,持续产生依赖MSH2的生发CTG重复序列扩增。

MSH2-dependent germinal CTG repeat expansions are produced continuously in spermatogonia from DM1 transgenic mice.

作者信息

Savouret Cédric, Garcia-Cordier Corinne, Megret Jérôme, te Riele Hein, Junien Claudine, Gourdon Geneviève

机构信息

INSERM U383 Génétique, Chromosome et Cancer, Clinique M. Lamy 2ème étage, Hôpital Necker Enfants Malades, 149 rue de Sèvres, 75015 Paris, France.

出版信息

Mol Cell Biol. 2004 Jan;24(2):629-37. doi: 10.1128/MCB.24.2.629-637.2004.

Abstract

Myotonic dystrophy type 1 is a neuromuscular affection associated with the expansion of an unstable CTG repeat in the DM protein kinase gene. The disease is characterized by somatic tissue-specific mosaicism and very high intergenerational instability with a strong bias towards expansions. We used transgenic mice carrying more than 300 unstable CTG repeats within their large human genomic environment to investigate the dynamics of CTG repeat germinal mosaicism in males. Germinal mosaicism towards expansions was already present in spermatozoa at 7 weeks of age and continued to increase with age, suggesting that expansions are continuously produced throughout life. To determine the precise stage at which germinal expansions occur during spermatogenesis, we sorted and collected the different germ cell types produced during spermatogenesis from males of different ages and analyzed the CTG repeat mosaicism in each fraction. Strong mosaicisms towards expansions were already observed in spermatogonia before meiosis. In transgenic Msh2-deficient mice, germinal instability of the CTG repeats (only contractions) also occurs premeiotically. No significant difference in mosaicism was detected between spermatogonia and spermatozoa, arguing against continued expansions during postmeiotic stages. This indicates that germinal expansions are produced at the beginning of spermatogenesis, in spermatogonia, by a meiosis-independent mechanism involving MSH2.

摘要

1型强直性肌营养不良是一种神经肌肉疾病,与DM蛋白激酶基因中不稳定的CTG重复序列扩增有关。该疾病的特征是体细胞组织特异性嵌合现象以及非常高的代际不稳定性,且强烈倾向于扩增。我们使用了在其庞大的人类基因组环境中携带超过300个不稳定CTG重复序列的转基因小鼠,来研究雄性小鼠中CTG重复序列生殖系嵌合现象的动态变化。在7周龄时,精子中就已经存在向扩增方向的生殖系嵌合现象,并且随着年龄的增长持续增加,这表明扩增在整个生命过程中持续产生。为了确定在精子发生过程中生殖系扩增发生的确切阶段,我们对不同年龄雄性小鼠精子发生过程中产生的不同生殖细胞类型进行了分选和收集,并分析了每个部分中的CTG重复序列嵌合现象。在减数分裂前的精原细胞中就已经观察到强烈向扩增方向的嵌合现象。在转基因Msh2缺陷小鼠中,CTG重复序列的生殖系不稳定性(仅收缩)也在减数分裂前发生。在精原细胞和精子之间未检测到嵌合现象的显著差异,这表明在减数分裂后阶段不存在持续的扩增。这表明生殖系扩增是在精子发生开始时,在精原细胞中,通过一种涉及MSH2的不依赖减数分裂的机制产生的。

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