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HLA-G expression during preimplantation human embryo development.

机译:植入前人类胚胎发育过程中的HLA-G表达。

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摘要

HLA-G is a nonclassical class I major histocompatibility complex molecule with a restricted pattern of expression that includes the placental extravillus cytotrophoblast cells in direct contact with maternal tissues. Circumstantial evidence suggests that HLA-G may play a role in protection of the semiallogeneic human fetus. We examined whether HLA-G is expressed during the critical period of preimplantation human development and whether expression of this molecule could be correlated with the cleavage rate of embryos. Using reverse transcription PCR on surplus human embryos and unfertilized oocytes from patients undergoing in vitro fertilization we detected HLA-G heavy chain mRNA in 40% of 148 of blastocysts tested. The presence of HLA-G mRNA was also detected in unfertilized oocytes and in early embryos, but not in control cumulus oophorus cells. beta 2-Microglobulin mRNA was also found in those embryos expressing HLA-G. In concordance with our mRNA data, a similar proportion of embryos stained positive for HLA-G utilizing a specific monoclonal antibody. Interestingly, expression of HLA-G mRNA was associated with an increased cleavage rate, as compared to embryos lacking HLA-G transcript. Thus, HLA-G could be a functional homologue of the mouse Qa-2 antigen, which has been implicated in differences in the rate of preimplantation embryo development. To our knowledge, the presence of HLA-G mRNA and protein in human preimplantation embryos and oocytes has not been reported previously. The correlation of HLA-G mRNA expression with cleavage rate suggests that this molecule may play an important role in human pre-embryo development.
机译:HLA-G是非经典的I类主要组织相容性复杂分子,其表达模式受到限制,其中包括与母体组织直接接触的胎盘绒毛外滋养细胞。间接证据表明,HLA-G可能在保护半同基因人类胎儿中起作用。我们检查了HLA-G是否在植入前人类发育的关键时期表达,并且该分子的表达是否与胚胎的裂解率相关。使用逆转录PCR对来自体外受精患者的剩余人类胚胎和未受精卵母细胞进行检测,我们在测试的148个囊胚中有40%检测到了HLA-G重链mRNA。在未受精卵母细胞和早期胚胎中也检测到HLA-G mRNA的存在,但在对照卵丘卵细胞中未检测到HLA-G mRNA的存在。在表达HLA-G的那些胚胎中也发现了β2-微球蛋白mRNA。根据我们的mRNA数据,利用特异性单克隆抗体将HLA-G染色呈阳性的胚胎比例相似。有趣的是,与缺乏HLA-G转录本的胚胎相比,HLA-G mRNA的表达与卵裂率增加有关。因此,HLA-G可能是小鼠Qa-2抗原的功能同源物,其与胚胎植入前胚胎发育速度的差异有关。据我们所知,人类植入前的胚胎和卵母细胞中HLA-G mRNA和蛋白质的存在尚未见报道。 HLA-G mRNA表达与切割率的相关性表明该分子可能在人类胚胎前发育中发挥重要作用。

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