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Abnormal Early Cleavage Events Predict Early Embryo Demise: Sperm Oxidative Stress and Early Abnormal Cleavage

机译:异常早期卵裂事件可预测早期胚胎消亡:精子氧化应激和早期异常卵裂

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摘要

Human embryos resulting from abnormal early cleavage can result in aneuploidy and failure to develop normally to the blastocyst stage. The nature of paternal influence on early embryo development has not been directly demonstrated although many studies have suggested effects from spermatozoal chromatin packaging, DNA damage, centriolar and mitotic spindle integrity, and plasma membrane integrity. The goal of this study was to determine whether early developmental events were affected by oxidative damage to the fertilizing sperm. Survival analysis was used to compare patterns of blastocyst formation based on P2 duration. Kaplan-Meier survival curves demonstrate that relatively few embryos with short (<1 hr) P2 times reached blastocysts, and the two curves diverged beginning on day 4, with nearly all of the embryos with longer P2 times reaching blastocysts by day 6 (p < .01). We determined that duration of the 2nd to 3rd mitoses were sensitive periods in the presence of spermatozoal oxidative stress. Embryos that displayed either too long or too short cytokineses demonstrated an increased failure to reach blastocyst stage and therefore survive for further development. Although paternal-derived gene expression occurs later in development, this study suggests a specific role in early mitosis that is highly influenced by paternal factors.
机译:异常早期切割产生的人类胚胎会导致非整倍性,并且无法正常发育到胚泡期。父亲对早期胚胎发育的影响的性质尚未得到直接证实,尽管许多研究表明,精子染色质包装,DNA损伤,中心粒和有丝分裂纺锤体完整性以及质膜完整性均会产生影响。这项研究的目的是确定早期发育事件是否受精子的氧化损伤的影响。生存分析被用来比较基于P2持续时间的囊胚形成模式。 Kaplan-Meier生存曲线表明,相对较少的P2时间短(<1 hr)的胚胎到达了胚泡,并且两条曲线从第4天开始发散,几乎所有P2时间较长的胚都在第6天到达了胚泡(p < .01)。我们确定在有精子体氧化应激的情况下,第二至第三次有丝分裂的持续时间是敏感期。表现出太长或太短的细胞因子的胚胎显示出进入胚泡阶段的失败增加,因此可以存活以进行进一步的发育。尽管父本来源的基因表达发生在发育后期,但这项研究表明,在父本有丝分裂中的特定作用受到父本因素的高度影响。

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