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Chromosomal disorders and male infertility

机译:染色体疾病和男性不育

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摘要

Infertility in humans is surprisingly common occurring in approximately 15% of the population wishing to start a family. Despite this, the molecular and genetic factors underlying the cause of infertility remain largely undiscovered. Nevertheless, more and more genetic factors associated with infertility are being identified. This review will focus on our current understanding of the chromosomal basis of male infertility specifically: chromosomal aneuploidy, structural and numerical karyotype abnormalities and Y chromosomal microdeletions. Chromosomal aneuploidy is the leading cause of pregnancy loss and developmental disabilities in humans. Aneuploidy is predominantly maternal in origin, but concerns have been raised regarding the safety of intracytoplasmic sperm injection as infertile men have significantly higher levels of sperm aneuploidy compared to their fertile counterparts. Males with numerical or structural karyotype abnormalities are also at an increased risk of producing aneuploid sperm. Our current understanding of how sperm aneuploidy translates to embryo aneuploidy will be reviewed, as well as the application of preimplantation genetic diagnosis (PGD) in such cases. Clinical recommendations where possible will be made, as well as discussion of the use of emerging array technology in PGD and its potential applications in male infertility.
机译:令人惊讶的是,人类不育症在希望组建家庭的人口中约有15%发生。尽管如此,导致不孕的分子和遗传因素仍未发现。然而,越来越多的与不育有关的遗传因素正在被鉴定。这项审查将侧重于我们目前对男性不育染色体基础的理解,特别是:染色体非整倍性,结构和数值核型异常以及Y染色体微缺失。染色体非整倍性是人类妊娠流失和发育障碍的主要原因。非整倍体主要起源于母体,但是由于胞质内精子注射的安全性较可育男性高得多,因此引起了人们的关注。具有数字或结构核型异常的男性也有增加产生非整倍性精子的风险。我们将对我们目前对精子非整倍性如何转化为胚胎非整倍性的理解以及在这种情况下的植入前遗传学诊断(PGD)的应用进行综述。将提出可能的临床建议,并讨论在PGD中使用新兴阵列技术及其在男性不育症中的潜在应用。

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