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新的孕前免疫生物标志物用于临床实践:子宫内膜侧的白细胞介素-18、白细胞介素-15 和 TWEAK,卵泡侧的粒细胞集落刺激因子。

New pre-conception immune biomarkers for clinical practice: interleukin-18, interleukin-15 and TWEAK on the endometrial side, G-CSF on the follicular side.

机构信息

Unité 782 INSERM, Hôpital Antoine Béclère et Université Paris Sud Orsay, 32 rue des Carnets, 92141 Clamart Cedex, France.

出版信息

J Reprod Immunol. 2011 Mar;88(2):118-23. doi: 10.1016/j.jri.2011.01.007. Epub 2011 Feb 18.

DOI:10.1016/j.jri.2011.01.007
PMID:21334074
Abstract

Identification of biomarkers of optimal uterine receptivity to the implanting embryo as well as biomarkers of oocyte competence would undoubtedly improve the efficiency of assisted reproductive technology (ART). Expression of IL-15 and IL-18 has been shown to be different in patients with failed implantation after IVF/ICSI compared with fertile controls and both correlate with local uNK (CD56+) recruitment and angiogenesis. Tumor necrosis factor weak inducer of apoptosis (TWEAK) has been described in mice as a potent early immune regulator able to protect the conceptus. The results of our studies in human suggest that TWEAK modulates the IL-18 related cytotoxicity of uNK cells. Quantification of IL-18, TWEAK and IL-15 mRNA expression by real-time PCR in endometrial tissue collected in mid-luteal phase of non-conception cycles allowed documentation of physiological events that occur at the time of uterine receptivity. Such information may be useful for the physician especially in patients where embryos fail to implant. Cytokine quantification may assist in understanding the mechanisms leading to repeated IVF/ICSI failure: either depletion of cytokines necessary for the apposition-adhesion, or an excess of cytokines leading to local cytotoxicity, may impair the implantation of the embryo. Other new data suggest that a pre-conception dialogue mediated by the oocyte and the follicular fluid and the oocyte may contribute to later implantation success. Follicular concentration of G-CSF appears as a useful biomarker of oocyte competence before fertilization. Moreover both in human and animal models, evidence of a role of the endometrium as a biosensor of the embryo is emerging.

摘要

鉴定对植入胚胎具有最佳子宫接受能力的生物标志物以及卵母细胞功能的生物标志物无疑将提高辅助生殖技术(ART)的效率。与生育能力正常的对照组相比,在体外受精/卵胞浆内单精子注射(IVF/ICSI)后着床失败的患者中,IL-15 和 IL-18 的表达显示出不同,并且两者均与局部 uNK(CD56+)募集和血管生成相关。在小鼠中,肿瘤坏死因子弱凋亡诱导剂(TWEAK)被描述为一种有效的早期免疫调节剂,能够保护胚胎。我们在人类中的研究结果表明,TWEAK 调节 uNK 细胞的 IL-18 相关细胞毒性。通过实时 PCR 定量分析非妊娠周期中黄体中期收集的子宫内膜组织中 IL-18、TWEAK 和 IL-15 mRNA 的表达,记录了在子宫接受能力发生时发生的生理事件。这些信息可能对医生有用,特别是在胚胎着床失败的患者中。细胞因子的定量分析可能有助于了解导致重复 IVF/ICSI 失败的机制:要么是必需的细胞因子的耗竭对于附着-黏附是必要的,要么是局部细胞毒性的细胞因子过量,可能会损害胚胎的着床。其他新数据表明,卵母细胞和卵泡液介导的受孕前对话以及卵母细胞可能有助于随后的着床成功。在受精前,卵泡中 G-CSF 的浓度似乎是卵母细胞功能的有用生物标志物。此外,在人类和动物模型中,子宫内膜作为胚胎生物传感器的作用证据正在出现。

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