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用于评估卵母细胞和植入前胚胎健康状况的遗传学与影像学检查

Genetics and imaging to assess oocyte and preimplantation embryo health.

作者信息

Warner C M, Newmark J A, Comiskey M, De Fazio S R, O'Malley D M, Rajadhyaksha M, Townsend D J, McKnight S, Roysam B, Dwyer P J, DiMarzio C A

机构信息

Department of Biology, Northeastern University, Boston, MA 02115, USA.

出版信息

Reprod Fertil Dev. 2004;16(7):729-41. doi: 10.1071/rd04088.

Abstract

Two major criteria are currently used in human assisted reproductive technologies (ART) to evaluate oocyte and preimplantation embryo health: (1) rate of preimplantation embryonic development; and (2) overall morphology. A major gene that regulates the rate of preimplantation development is the preimplantation embryo development (Ped) gene, discovered in our laboratory. In mice, presence of the Ped gene product, Qa-2 protein, results in a fast rate of preimplantation embryonic development, compared with a slow rate of preimplantation embryonic development for embryos that are lacking Qa-2 protein. Moreover, mice that express Qa-2 protein have an overall reproductive advantage that extends beyond the preimplantation period, including higher survival to birth, higher birthweight, and higher survival to weaning. Data are presented that suggest that Qa-2 increases the rate of development of early embryos by acting as a cell-signalling molecule and that phosphatidylinositol-32 kinase is involved in the cell-signalling pathway. The most likely human homologue of Qa-2 has recently been identified as human leukocyte antigen (HLA)-G. Data are presented which show that HLA-G, like Qa-2, is located in lipid rafts, implying that HLA-G also acts as a signalling molecule. In order to better evaluate the second criterion used in ART (i.e. overall morphology), a unique and innovative imaging microscope has been constructed, the Keck 3-D fusion microscope (Keck 3DFM). The Keck 3DFM combines five different microscopic modes into a single platform, allowing multi-modal imaging of the specimen. One of the modes, the quadrature tomographic microscope (QTM), creates digital images of non-stained transparent cells by measuring changes in the index of refraction. Quadrature tomographic microscope images of oocytes and preimplantation mouse embryos are presented for the first time. The digital information from the QTM images should allow the number of cells in a preimplantation embryo to be counted non-invasively. The Keck 3DFM is also being used to assess mitochondrial distribution in mouse oocytes and embryos by using the k-means clustering algorithm. Both the number of cells in preimplantation embryos and mitochondrial distribution are related to oocyte and embryo health. New imaging data obtained from the Keck 3DFM, combined with genetic and biochemical approaches, have the promise of being able to distinguish healthy from unhealthy oocytes and embryos in a non-invasive manner. The goal is to apply the information from our mouse model system to the clinic in order to identify one and only one healthy embryo for transfer back to the mother undergoing an ART procedure. This approach has the potential to increase the success rate of ART and to decrease the high, and undesirable, multiple birth rate presently associated with ART.

摘要

目前在人类辅助生殖技术(ART)中,有两个主要标准用于评估卵母细胞和植入前胚胎的健康状况:(1)植入前胚胎发育率;(2)整体形态。我们实验室发现了一个调节植入前发育率的主要基因,即植入前胚胎发育(Ped)基因。在小鼠中,与缺乏Qa-2蛋白的胚胎相比,Ped基因产物Qa-2蛋白的存在会导致植入前胚胎发育速度加快。此外,表达Qa-2蛋白的小鼠具有超出植入前期的整体生殖优势,包括更高的出生存活率、更高的出生体重和更高的断奶存活率。有数据表明,Qa-2作为一种细胞信号分子,可提高早期胚胎的发育速度,且磷脂酰肌醇-32激酶参与了细胞信号通路。最近已确定Qa-2最可能的人类同源物为人白细胞抗原(HLA)-G。有数据显示,与Qa-2一样,HLA-G也位于脂筏中,这意味着HLA-G也作为一种信号分子发挥作用。为了更好地评估ART中使用的第二个标准(即整体形态),已构建了一台独特且创新的成像显微镜,即凯克三维融合显微镜(Keck 3DFM)。Keck 3DFM将五种不同的显微镜模式整合到一个平台上,允许对样本进行多模态成像。其中一种模式,即正交断层显微镜(QTM),通过测量折射率的变化来创建未染色透明细胞的数字图像。首次展示了卵母细胞和植入前小鼠胚胎的正交断层显微镜图像。来自QTM图像的数字信息应能使无创计数植入前胚胎中的细胞数量。Keck 3DFM还被用于通过使用k均值聚类算法评估小鼠卵母细胞和胚胎中的线粒体分布。植入前胚胎中的细胞数量和线粒体分布均与卵母细胞和胚胎健康有关。从Keck 3DFM获得的新成像数据,结合遗传和生化方法,有望能够以无创方式区分健康和不健康的卵母细胞及胚胎。目标是将我们小鼠模型系统中的信息应用于临床,以便识别出唯一的一个健康胚胎,将其移植回接受ART程序的母亲体内。这种方法有可能提高ART的成功率,并降低目前与ART相关的高且不理想的多胎出生率。

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