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首页> 外文期刊>Molecular human reproduction. >No evidence for paternal mtDNA transmission to offspring or extra-embryonic tissues after ICSI.
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No evidence for paternal mtDNA transmission to offspring or extra-embryonic tissues after ICSI.

机译:没有证据表明ICSI后,父系mtDNA可传播至后代或胚外组织。

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摘要

There is a risk that ICSI may increase the transmission of mtDNA diseases to children born after this technique. Knowledge of the fate and transmission of paternal mitochondrial DNA is important since mutations in mitochondrial DNA have been described in oligozoospermic males. We have used an adaptation of solid phase mini-sequencing to exclude the presence of levels of paternal mtDNA >0.001% in ICSI families. This method is more sensitive than those used in previous studies and is sufficient to detect the likely paternal contribution (approximately 0.1-0.5% from simple calculations of expected dilution during fertilization). Using this method, we were able to detect concentrations as low as 0.001% paternal mtDNA in a maternal mtDNA background. No paternal mtDNA was detected in the embryonic (blood or buccal swabs) tissue of children born after ICSI nor in extra-embryonic tissue (placenta or umbilical cord). In conclusion, we did not detect paternal mtDNA in blood, buccal swabs, placenta or umbilical cord of children born after ICSI. We have found no evidence that ICSI increases the risk of paternal transmission of mtDNA and hence of mtDNA disorders.
机译:ICSI可能会增加使用该技术出生的儿童的mtDNA疾病传播。父系线粒体DNA的命运和传播的知识很重要,因为已经在少精症男性中描述了线粒体DNA的突变。我们采用了固相微测序技术,以排除ICSI家族中父体mtDNA的水平> 0.001%。该方法比以前的研究中的方法更灵敏,并且足以检测可能的父本影响(从受精过程中预期稀释度的简单计算中大约占0.1-0.5%)。使用这种方法,我们能够在母体mtDNA背景中检测到低至0.001%父本mtDNA的浓度。在ICSI后出生的孩子的胚胎(血液或颊拭子)组织中,或在胚外组织(胎盘或脐带)中均未检测到父系mtDNA。总之,我们没有在ICSI后出生的孩子的血液,颊拭子,胎盘或脐带中检测到父亲的mtDNA。我们没有发现证据表明ICSI增加了父系传播mtDNA的风险,从而增加了mtDNA疾病的风险。

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