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评估精子基因组完整性以改善不良辅助生殖技术临床结局。

Assessing male gamete genome integrity to ameliorate poor assisted reproductive technology clinical outcome.

机构信息

The Ronald O. Perelman and Claudia Cohen Center for Reproductive Medicine, Weill Cornell Medicine, New York, New York.

The Ronald O. Perelman and Claudia Cohen Center for Reproductive Medicine, Weill Cornell Medicine, New York, New York.

出版信息

F S Sci. 2023 Feb;4(1):2-10. doi: 10.1016/j.xfss.2022.08.001. Epub 2022 Aug 13.

Abstract

OBJECTIVE

To assess the role of evaluating sperm chromatin fragmentation (SCF) as a tool to guide treatment in couples who achieved unexpectedly poor clinical outcomes after intracytoplasmic sperm injection (ICSI).

DESIGN

We identified couples with an unexpectedly suboptimal clinical outcome after ICSI who were then screened for SCF. Consequently, the same couples were counseled to undergo a subsequent ICSI cycle using either ejaculates processed by microfluidic sperm selection (MFSS) or spermatozoa retrieved from the testis, and clinical outcomes were compared between history and treatment cycles. To confirm the sole effect of a compromised male gamete, we compared the ICSI outcome in cycles where male gametes with abnormal SCF were used to inseminate autologous and donor oocytes. Finally, to eliminate an eventual confounding female factor component, we compared the clinical outcome of ICSI cycles using sibling donor oocytes injected with spermatozoa with normal or abnormal SCF.

SETTING

Academic reproductive medicine center point of care.

PATIENT(S): The patient population consisted of 76 couples with reproductively healthy and relatively young female partners and male partners with compromised semen parameters, but suitable for ICSI. In a subanalysis, we identified 67 couples with abnormal SCF who underwent ICSI cycle(s) with donor oocytes. Furthermore, we identified 29 couples, 12 with normal SCF and 17 with abnormal, uncorrected SCF, and 7 couples with abnormal, corrected SCF vs. a control, who used sibling donor oocytes for their ICSI cycle(s).

INTERVENTION(S): For couples who resulted in surprisingly low clinical outcomes after ICSI, despite semen parameters adequate for ICSI and a normal female infertility evaluation, a SCF assessment was performed on the semen specimen using the terminal deoxynucleotidyl transferase-mediated fluorescein-deoxyuridine triphosphate nick-end labeling (TUNEL) assay. The couples then underwent a subsequent ICSI cycle with spermatozoa processed by MFSS or surgically retrieved. Moreover, cycles with donor oocytes were used to confirm the sole contribution of the male gamete.

MAIN OUTCOME MEASURE(S): Clinical outcomes, such as fertilization, embryo implantation, clinical pregnancy, delivery, and pregnancy loss rates were compared between history and treatment cycle(s) using ejaculated spermatozoa selected by MFSS or from a testicular biopsy, taking into consideration the level of SCF. In a subanalysis, we reported the clinical outcomes of 67 patients who used donor oocytes and compared them with cycles where their own oocytes were used. Furthermore, we compared the ICSI clinical outcomes between cycles using sibling donor oocytes injected with low or high SCF with or without sperm intervention aimed at correcting, or alleviating the degree of SCF.

RESULT(S): In a total of 168 cycles, 76 couples had in a prior cycle a 67.1% fertilization rate, and clinical pregnancy and pregnancy loss rates of 16.6% and 52.3%, respectively. After testing for SCF, the DNA fragmentation rate was 21.6%. This led to a subsequent ICSI cycle with MFSS or testicular sperm extraction, resulting in clinical pregnancy and delivery rates of 39.2%, and 37.3%, respectively. The embryo implantation rate increased to 23.5%, whereas the pregnancy loss rate decreased to 5% in the treatment cycle. This was particularly significant in the moderate SCF group, reaching embryo implantation, clinical pregnancy, and delivery rates of 24.3%, 40.4%, and 36.2%, respectively, and reducing the pregnancy loss rate to 10.5% in post-sperm treatment cycles. In 67 patients with high SCF who used donor oocytes, a significantly higher fertilization rate of 78.1% and embryo implantation rate of 29.1% were reported, compared with those in couples also with an elevated SCF who used their own. Interestingly, the clinical pregnancy and delivery rates only increased slightly from 28.0%-36.1% and from 23.7%-29.2%, respectively. To further control for a female factor, we observed couples who shared sibling donor oocytes, 17 with normal SCF and 12 with abnormal (uncorrected) SCF. Interestingly, the abnormal SCF group had impaired fertilization (69.3%), embryo implantation (15.0%), and delivery (15.4%) rates. For an additional 15 couples who split their donor oocytes, 8 had normal SCF, and although 7 couples originally had abnormal SCF, 4 used microfluidic processing, 2 used testicular spermatozoa, and 1 used donor spermatozoa to alleviate the degree of SCF, resulting in comparable clinical outcomes with the normal SCF group.

CONCLUSION(S): A superimposed male factor component may explain the disappointing ICSI outcome in some couples despite reproductively healthy female partners. Therefore, it may be useful to screen couples for SCF to guide treatment options and maximize chances of a successful pregnancy. The improved, but suboptimal pregnancy and delivery outcomes observed in couples using donor oocytes confirmed the exclusive detrimental role that the male gamete exerted on embryo development despite the presence of putative oocyte repair mechanisms.

摘要

目的

评估精子染色质碎片化(SCF)作为指导治疗工具的作用,这些夫妇在接受胞浆内单精子注射(ICSI)后获得了出乎意料的不良临床结局。

设计

我们确定了在 ICSI 后临床结局出乎意料不佳的夫妇,然后对他们进行 SCF 筛查。随后,对同一对夫妇进行咨询,建议他们进行后续的 ICSI 周期,使用微流控精子选择(MFSS)处理的精液或睾丸中提取的精子,比较病史和治疗周期的临床结局。为了确认仅男性配子受损的作用,我们比较了使用异常 SCF 的精子进行自体和供体卵受精的 ICSI 结局。最后,为了消除最终的女性因素混杂成分,我们比较了使用正常或异常 SCF 的精子受精的同胞供体卵的 ICSI 周期的临床结局。

地点

学术生殖医学中心。

患者

患者人群由 76 对生育健康且相对年轻的女性伴侣和男性伴侣组成,男性伴侣的精液参数受损,但适合 ICSI。在亚分析中,我们确定了 67 对 SCF 异常的夫妇,他们接受了供体卵的 ICSI 周期。此外,我们确定了 29 对夫妇,其中 12 对 SCF 正常,17 对 SCF 异常且未经校正,7 对夫妇的 SCF 异常,经校正后正常,与对照相比,他们使用了同胞供体卵进行 ICSI 周期。

干预

对于 ICSI 后临床结局出乎意料不佳的夫妇,尽管精液参数适合 ICSI,女性不孕评估正常,但对精液标本进行了精子染色质碎片化(SCF)评估,使用末端脱氧核苷酸转移酶介导的荧光素-脱氧尿苷三磷酸末端标记(TUNEL)检测法。然后,夫妇们进行了后续的 ICSI 周期,使用 MFSS 处理的精子或手术提取的精子。此外,使用供体卵的周期用于确认仅男性配子的贡献。

主要观察指标

比较病史和治疗周期(使用 MFSS 选择的射出精液或睾丸活检提取的精子)的受精率、胚胎着床率、临床妊娠率、分娩率和妊娠丢失率等临床结局,考虑 SCF 水平。在亚分析中,我们报告了使用供体卵的 67 名患者的临床结局,并将其与使用自身卵的周期进行了比较。此外,我们比较了使用低或高 SCF 的同胞供体卵的 ICSI 临床结局,以及是否进行精子干预以纠正或减轻 SCF 程度。

结果

在总共 168 个周期中,76 对夫妇在前一个周期的受精率为 67.1%,临床妊娠率和妊娠丢失率分别为 16.6%和 52.3%。测试 SCF 后,DNA 碎片化率为 21.6%。这导致了随后的 ICSI 周期,使用 MFSS 或睾丸精子提取,临床妊娠率和分娩率分别为 39.2%和 37.3%。胚胎着床率增加到 23.5%,而妊娠丢失率降低到治疗周期的 5%。在 67 名 SCF 较高的患者中,使用供体卵的受精率显著提高至 78.1%,胚胎着床率和临床妊娠率分别提高至 40.4%和 36.2%,妊娠丢失率降低至 10.5%。有趣的是,在 SCF 升高的夫妇中,胚胎着床率和临床妊娠率仅略有增加,分别为 28.0%-36.1%和 23.7%-29.2%。为了进一步控制女性因素,我们观察了使用同胞供体卵的夫妇,其中 17 对 SCF 正常,12 对 SCF 异常(未校正)。有趣的是,异常 SCF 组的受精率(69.3%)、胚胎着床率(15.0%)和分娩率(15.4%)受损。对于另外 15 对夫妇,他们将供体卵分开使用,其中 8 对 SCF 正常,尽管最初有 7 对 SCF 异常,但其中 4 对使用微流控处理,2 对使用睾丸精子,1 对使用供体精子来减轻 SCF 程度,与正常 SCF 组的临床结局相当。

结论

尽管女性伴侣生育健康,但一些夫妇的 ICSI 结局出乎意料不佳,可能存在叠加的男性因素。因此,筛查夫妇的 SCF 以指导治疗方案并最大限度地提高成功妊娠的机会可能是有用的。尽管存在潜在的卵修复机制,但使用供体卵的夫妇的妊娠和分娩结局得到改善,但仍不理想,这证实了男性配子对胚胎发育的唯一不利作用。

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