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对母体血浆、卵泡液和植入前胚胎中的HLA - G进行分析,发现其表达模式不对称。

Analysis of HLA-G in maternal plasma, follicular fluid, and preimplantation embryos reveal an asymmetric pattern of expression.

作者信息

Shaikly Valerie R, Morrison Ian E G, Taranissi Mohamed, Noble Clare V, Withey Anna D, Cherry Richard J, Blois Sandra M, Fernández Nelson

机构信息

Department of Biological Sciences, University of Essex, Essex, United Kingdom.

出版信息

J Immunol. 2008 Mar 15;180(6):4330-7. doi: 10.4049/jimmunol.180.6.4330.

Abstract

Soluble HLA-G (sHLA-G) secretion by human preimplantation embryos in culture has been associated with successful embryo development, and therefore has potential to serve as a noninvasive marker of embryo viability. We have examined the spatial and temporal expression of HLA-G in embryos of varying developmental competence and the role of maternal factors in human embryonic HLA-G expression. Embryos that reached blastocyst stage on day 5 showed a higher frequency of sHLA-G secretion than those at morula or arrested stages (p < 0.05). There was no significant difference in sHLA-G secretion between normal embryos and those diagnosed as chromosomally abnormal by preimplantation genetic diagnosis. HLA-G detected in maternal plasma and follicular fluid did not appear to correlate with HLA-G expressed in the embryo or embryo supernatants. Confocal microscopy analysis indicated that HLA-G protein expression in embryos was not homogeneous; mostly, it was confined to blastocysts localized on trophectoderm and trophectoderm projections. Single-particle fluorescent imaging analysis of HLA-G on the cell surface of JEG-3 cells showed that HLA-G particles were mostly monomeric, but dimeric and higher order oligomers were also observed. These results suggest that HLA-G play an important role in preimplantation embryo development. However, the observed expression of HLA-G in arrested and chromosomally abnormal embryos indicates that HLA-G testing should be used with caution and in conjunction with conventional methods of embryo screening and selection.

摘要

体外培养的人类植入前胚胎分泌的可溶性 HLA - G(sHLA - G)与胚胎的成功发育有关,因此有潜力作为胚胎活力的非侵入性标志物。我们研究了不同发育能力胚胎中 HLA - G 的时空表达以及母体因素在人类胚胎 HLA - G 表达中的作用。在第 5 天达到囊胚阶段的胚胎比桑椹胚或停滞阶段的胚胎 sHLA - G 分泌频率更高(p < 0.05)。正常胚胎与通过植入前基因诊断被诊断为染色体异常的胚胎之间,sHLA - G 分泌没有显著差异。在母体血浆和卵泡液中检测到的 HLA - G 似乎与胚胎或胚胎上清液中表达 的 HLA - G 无关。共聚焦显微镜分析表明,胚胎中 HLA - G 蛋白表达不均匀;大多数情况下,它局限于位于滋养外胚层和滋养外胚层突起上的囊胚。对 JEG - 3 细胞表面 HLA - G 的单颗粒荧光成像分析表明,HLA - G 颗粒大多为单体,但也观察到二聚体和更高阶的寡聚体。这些结果表明 HLA - G 在植入前胚胎发育中起重要作用。然而,在停滞和染色体异常胚胎中观察到的 HLA - G 表达表明,HLA - G 检测应谨慎使用,并与传统的胚胎筛选和选择方法结合使用。

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