School of Biomedical Engineering, Shanghai Jiao Tong University, Med-X Research Institute, Shanghai, China.
Department of Andrology, Urologic Medical Center, Shanghai General Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, China.
J Med Genet. 2018 Mar;55(3):150-157. doi: 10.1136/jmedgenet-2016-104404. Epub 2018 Jan 12.
The mechanism of intramanchette transport is crucial to the transformation of sperm tail and the nuclear condensation during spermiogenesis. Although few dysfunctional proteins could result in abnormal junction between the head and tail of spermatozoon, little is known about the genetic cues in this process.
Based on patients with severe decapitated and decaudated spermatozoa (DDS) syndrome, the study aimed to validate whether new mutation exists on their Hook microtubule-tethering protein 1 () genes and follow their results of assisted reproduction treatment (ART).
7 severe teratozoospermia patients with DDS (proportion >95%) and three relative members in one pedigree were collected to sequence the whole genomic DNA. The fertilisation rates (FRs) of these patients were followed. Morphological observation and interspecies intracytoplasmic sperm injection (ICSI) assays were applied.
A novel missense mutation of A to G (p.Q286R) in patients with DDS (n=3/7) was found in the gene, which was inherited from the mother in one patient. This variant was absent in 160 fertile population-matched control individuals. Morphological observation showed that almost all the DDS broke into decaudated heads and headless tails at the implantation fossa or the basal plate. The clinical studies indicated that the mutation might cause reduced FRs on both ART (FR=18.07%) and interspecies ICSI (FR=16.98%).
An unreported mutation in gene was identified, which might be responsible to some patients with DDS. Further studies need to uncover the molecular mechanism of spermiogenesis for genomic therapy.
中繖体运输的机制对于精子尾部的转化和精子发生过程中的核浓缩至关重要。尽管很少有功能失调的蛋白质会导致精子头和尾之间的异常连接,但对于这个过程中的遗传线索知之甚少。
基于严重断头和尾缺失精子症(DDS)患者,本研究旨在验证他们的 Hook 微管连接蛋白 1()基因是否存在新的突变,并追踪他们的辅助生殖治疗(ART)结果。
收集了 7 名严重畸形精子症(DDS)患者(比例>95%)和一个家系中的 3 名相关成员,以对其全基因组 DNA 进行测序。随访这些患者的受精率(FR)。进行形态学观察和种间胞质内精子注射(ICSI)试验。
在 3 名 DDS 患者(n=3/7)的 基因中发现了一种新的错义突变 A 到 G(p.Q286R),该突变是一名患者从母亲那里遗传而来。这种变异在 160 名与生育力匹配的对照个体中不存在。形态学观察表明,几乎所有的 DDS 都在着床窝或基板处断裂成尾缺失的头部和无头的尾部。临床研究表明,该突变可能导致 ART(FR=18.07%)和种间 ICSI(FR=16.98%)的 FR 降低。
鉴定出一个未报道的 基因中的突变,该突变可能与一些 DDS 患者有关。需要进一步研究以揭示精子发生的分子机制,从而进行基因组治疗。
