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首页> 外文期刊>Human Molecular Genetics >Non-disjunction of chromosome 13.
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Non-disjunction of chromosome 13.

机译:不分离第13号染色体。

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We performed a molecular study with 21 microsatellites on a sample of 82 trisomy 13 conceptuses, the largest number of cases studied to date. The parental origin was determined in every case and in 89% the extra chromosome 13 was of maternal origin with an almost equal number of maternal MI and MII errors. The latter finding is unique among human autosomal trisomies, where maternal MI (trisomies 15, 16, 21, 22) or MII (trisomy 18) errors dominate. Of the nine paternally derived cases five were of MII origin but none arose from MI errors. There was some evidence for elevated maternal age in cases with maternal meiotic origin for liveborn infants. Maternal and paternal ages were elevated in cases with paternal meiotic origin. This is in contrast to results from a similar study of non-disjunction of trisomy 21 where paternal but not maternal age was elevated. We find clear evidence for reduced recombination in both maternal MI and MII errors and the former is associated with a significant number of tetrads (33%) that are nullichiasmate, which do not appear to be a feature of normal chromosome 13 meiosis. This study supports the evidence for subtle chromosome-specific influences on the mechanisms that determine non-disjunction of human chromosomes, consistent with the diversity of findings for other trisomies.
机译:我们对82个三体性13个概念性动物的样本进行了21个微卫星的分子研究,这是迄今为止研究最多的病例。在每种情况下都确定了亲本起源,在89%的额外染色体13中,有13个是母亲起源的,而母亲MI和MII错误的数目几乎相等。后者的发现在人类常染色体三体性中是独特的,其中母亲MI(三体性15、16、21、22)或MII(18三体性)错误占主导。在9例父系病例中,有5例来自MII,但均未因MI错误而引起。有证据表明,对于活产婴儿而言,母亲减数分裂起源的病例中,母亲的年龄升高了。具有父系减数分裂起源的病例的母本和父本年龄均升高。这与21号三分法不分离的类似研究结果相反,在该研究中,父亲而非母亲的年龄有所提高。我们发现明显的证据表明母体MI和MII错误的重组减少,而前者与无效四倍体的大量四分体(33%)有关,这似乎不是正常13号染色体减数分裂的特征。这项研究支持证据表明,细微的染色体特异性影响决定人类染色体不分离的机制,这与其他三体性发现的多样性相一致。

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