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胚胎植入前遗传学筛查(PGS)假说是否仍站得住脚?一篇综述。

Is the hypothesis of preimplantation genetic screening (PGS) still supportable? A review.

作者信息

Gleicher Norbert, Orvieto Raoul

机构信息

The Center for Human Reproduction, New York, NY, 10021, USA.

Foundation for Reproductive Medicine, New York, NY, 10022, USA.

出版信息

J Ovarian Res. 2017 Mar 27;10(1):21. doi: 10.1186/s13048-017-0318-3.

Abstract

The hypothesis of preimplantation genetic diagnosis (PGS) was first proposed 20 years ago, suggesting that elimination of aneuploid embryos prior to transfer will improve implantation rates of remaining embryos during in vitro fertilization (IVF), increase pregnancy and live birth rates and reduce miscarriages. The aforementioned improved outcome was based on 5 essential assumptions: (i) Most IVF cycles fail because of aneuploid embryos. (ii) Their elimination prior to embryo transfer will improve IVF outcomes. (iii) A single trophectoderm biopsy (TEB) at blastocyst stage is representative of the whole TE. (iv) TE ploidy reliably represents the inner cell mass (ICM). (v) Ploidy does not change (i.e., self-correct) downstream from blastocyst stage. We aim to offer a review of the aforementioned assumptions and challenge the general hypothesis of PGS. We reviewed 455 publications, which as of January 20, 2017 were listed in PubMed under the search phrase < preimplantation genetic screening (PGS) for aneuploidy>. The literature review was performed by both authors who agreed on the final 55 references. Various reports over the last 18 months have raised significant questions not only about the basic clinical utility of PGS but the biological underpinnings of the hypothesis, the technical ability of a single trophectoderm (TE) biopsy to accurately assess an embryo's ploidy, and suggested that PGS actually negatively affects IVF outcomes while not affecting miscarriage rates. Moreover, due to high rates of false positive diagnoses as a consequence of high mosaicism rates in TE, PGS leads to the discarding of large numbers of normal embryos with potential for normal euploid pregnancies if transferred rather than disposed of. We found all 5 basic assumptions underlying the hypothesis of PGS to be unsupported: (i) The association of embryo aneuploidy with IVF failure has to be reevaluated in view how much more common TE mosaicism is than has until recently been appreciated. (ii) Reliable elimination of presumed aneuploid embryos prior to embryo transfer appears unrealistic. (iii) Mathematical models demonstrate that a single TEB cannot provide reliable information about the whole TE. (iv) TE does not reliably reflect the ICM. (v) Embryos, likely, still have strong innate ability to self-correct downstream from blastocyst stage, with ICM doing so better than TE. The hypothesis of PGS, therefore, no longer appears supportable. With all 5 basic assumptions underlying the hypothesis of PGS demonstrated to have been mistaken, the hypothesis of PGS, itself, appears to be discredited. Clinical use of PGS for the purpose of IVF outcome improvements should, therefore, going forward be restricted to research studies.

摘要

植入前基因诊断(PGS)的假说于20年前首次提出,该假说认为在体外受精(IVF)过程中,在移植前剔除非整倍体胚胎将提高剩余胚胎的着床率,增加妊娠率和活产率,并减少流产。上述改善结果基于5个基本假设:(i)大多数IVF周期失败是因为胚胎为非整倍体。(ii)在胚胎移植前剔除这些胚胎将改善IVF结局。(iii)在囊胚期进行的单次滋养外胚层活检(TEB)代表整个滋养外胚层。(iv)滋养外胚层的倍性可靠地代表内细胞团(ICM)。(v)从囊胚期下游开始,倍性不会改变(即自我纠正)。我们旨在对上述假设进行综述,并对PGS的一般假说提出质疑。我们检索了455篇出版物,截至2017年1月20日,这些出版物在PubMed上以搜索词<非整倍体的植入前基因筛查(PGS)>列出。文献综述由两位作者共同进行,最终确定了55篇参考文献。过去18个月的各种报告不仅对PGS的基本临床效用,而且对该假说的生物学基础、单次滋养外胚层(TE)活检准确评估胚胎倍性的技术能力都提出了重大质疑,并表明PGS实际上对IVF结局有负面影响,而对流产率没有影响。此外,由于滋养外胚层中高嵌合率导致的假阳性诊断率很高,PGS导致大量具有正常整倍体妊娠潜力的正常胚胎被丢弃,如果移植而非丢弃这些胚胎,它们本可以实现正常妊娠。我们发现PGS假说的所有5个基本假设都没有依据:(i)鉴于滋养外胚层嵌合现象比以前认识到的更为普遍,必须重新评估胚胎非整倍体与IVF失败之间的关联。(ii)在胚胎移植前可靠地剔除假定的非整倍体胚胎似乎不现实。(iii)数学模型表明,单次TEB不能提供关于整个滋养外胚层的可靠信息。(iv)滋养外胚层不能可靠地反映内细胞团。(v)胚胎在囊胚期下游可能仍具有很强的自我纠正先天能力,内细胞团的自我纠正能力比滋养外胚层更好。因此,PGS假说似乎不再站得住脚。由于PGS假说的所有5个基本假设都被证明是错误的,PGS假说本身似乎已声名扫地。因此,为改善IVF结局而临床使用PGS今后应仅限于研究。

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