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Genetic and developmental analysis of X-inactivation in interspecific hybrid mice suggests a role for the Y chromosome in placental dysplasia.

机译:对种间杂种小鼠X失活的遗传和发育分析表明Y染色体在胎盘发育异常中的作用。

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摘要

It has been shown previously that abnormal placental growth, i.e., hyper- and hypoplasia, occurs in crosses and backcrosses between different mouse (Mus) species. A locus that contributes to this abnormal development has been mapped to the X chromosome. Unexpectedly, an influence of fetal sex on placental development has been observed, in that placentas attached to male fetuses tended to exhibit a more pronounced phenotype than placentas attached to females. Here, we have analyzed this sex dependence in more detail. Our results show that differences between male and female placental weights are characteristic of interspecific matings and are not observed in intraspecific Mus musculus matings. The effect is retained in congenic lines that contain differing lengths of M. spretus-derived X chromosome. Expression of the X-linked gene Pgk1 from the maternal allele only and lack of overall activity of two paternally inherited X-linked transgenes indicate that reactivation or lack of inactivation of the paternal X chromosome in trophoblasts of interspecific hybrids is not a frequent occurrence. Thus, the difference between male and female placentas seems not to be caused by faulty preferential X-inactivation. Therefore, these data suggest that the sex difference of placental weights in interspecific hybrids is caused by interactions with the Y chromosome.
机译:先前已经表明,不同小鼠(Mus)物种之间的杂交和回交中发生异常的胎盘生长,即增生和发育不全。导致这种异常发育的基因座已被定位到X染色体。出乎意料的是,已经观察到胎儿性别对胎盘发育的影响,因为附着在雄性胎儿上的胎盘往往比附着在雌性上的胎盘表现出更明显的表型。在这里,我们已经更详细地分析了这种性别依赖性。我们的结果表明,男性和女性胎盘重量之间的差异是种间交配的特征,而在种内小家鼠交配中未观察到。该作用保留在含有不同长度的M. spretus衍生的X染色体的同系中。仅来自母体等位基因的X连锁基因Pgk1的表达以及缺乏两个父本遗传的X连锁转基因的总体活性表明,在种间杂种的滋养细胞中父X染色体的重新激活或缺乏失活并不常见。因此,雄性和雌性胎盘之间的差异似乎不是由错误的优先X失活引起的。因此,这些数据表明种间杂种中胎盘重量的性别差异是由与Y染色体的相互作用引起的。

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