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克隆小鼠胚胎及其衍生的胚胎干细胞的染色体稳定性存在差异。

Chromosome stability differs in cloned mouse embryos and derivative ES cells.

作者信息

Balbach Sebastian T, Jauch Anna, Böhm-Steuer Barbara, Cavaleri Fatima M, Han Yong-Mahn, Boiani Michele

机构信息

Max Planck Institute for Molecular Biomedicine, Röntgenstrasse 20, D-48149 Münster, Germany.

出版信息

Dev Biol. 2007 Aug 15;308(2):309-21. doi: 10.1016/j.ydbio.2007.05.034. Epub 2007 Jun 2.

Abstract

The mechanisms that have evolved to maintain genome stability during cell cycle progression are challenged when a somatic cell nucleus is placed in a meiotic environment such as the ooplasm. Chromosomal spindle aberrations ensue in the majority of reconstructed oocytes within 2 h of transplantation, but it is not known if they recover or persist with the onset of embryonic divisions. We analyzed the chromosomal spindles and the karyotype of cumulus cell-derived mouse clones through the initial and hence most critical mitoses. Cloned embryos start out with less aneuploidy than fertilized embryos but surpass them after ES cell derivation, as measured by frequencies of chromosome trisomies and structural rearrangements. Despite the limited proportion of cloned mouse embryos that reach late gestation, a phenotypic mutation lacking a karyotypic mark was found in a newborn mouse cloned in 2002 and has been inherited since by its offspring. These data concur with a prevalent epigenetic, rather than genetic, basis for cloned embryo failure, but they also warn against the temptation to think that all conditions of clones are epigenetic and recover during gametogenesis. The cloning procedure is defenseless (no matter how technically refined) towards pre-existing or induced subchromosomal mutations that are below the experimental detection limit of the cytogenetic assay.

摘要

当将体细胞的细胞核置于减数分裂环境(如卵质)中时,在细胞周期进程中进化出的维持基因组稳定性的机制会受到挑战。移植后2小时内,大多数重构卵母细胞会出现染色体纺锤体畸变,但尚不清楚它们在胚胎分裂开始时是恢复正常还是持续存在。我们通过最初也是最关键的有丝分裂分析了卵丘细胞来源的小鼠克隆胚胎的染色体纺锤体和核型。通过染色体三体和结构重排的频率测量,克隆胚胎开始时的非整倍体比受精胚胎少,但在胚胎干细胞衍生后超过了受精胚胎。尽管只有有限比例的克隆小鼠胚胎能发育到妊娠后期,但在2002年克隆的一只新生小鼠中发现了一种缺乏核型标记的表型突变,并且其后代一直遗传该突变。这些数据支持克隆胚胎失败的主要原因是表观遗传而非遗传这一观点,但它们也警示人们不要认为克隆胚胎的所有问题都是表观遗传的且在配子发生过程中会恢复正常。克隆程序对于低于细胞遗传学检测实验极限的预先存在的或诱导产生的亚染色体突变是无能为力的(无论技术上多么精细)。

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