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人类生长分化因子9(GDF-9)及其新的同源物GDF-9B在卵泡早期发生过程中在卵母细胞中表达。

Human growth differentiation factor 9 (GDF-9) and its novel homolog GDF-9B are expressed in oocytes during early folliculogenesis.

作者信息

Aaltonen J, Laitinen M P, Vuojolainen K, Jaatinen R, Horelli-Kuitunen N, Seppä L, Louhio H, Tuuri T, Sjöberg J, Bützow R, Hovata O, Dale L, Ritvos O

机构信息

Department of Bacteriology and Immunology, Haartman Institute, University of Helsinki, Finland.

出版信息

J Clin Endocrinol Metab. 1999 Aug;84(8):2744-50. doi: 10.1210/jcem.84.8.5921.

Abstract

Growth differentiation factor 9 (GDF-9) is a transforming growth factor-beta family member that is required for normal folliculogenesis in female mice, but its role as a regulator of human fertility is still unclear. We determined here by in situ hybridization and immunohistochemical analyses the localization of the GDF-9 messenger ribonucleic acid (mRNA) and protein during human folliculogenesis. The GDF-9 transcripts were not detected in primordial follicles, but they are abundantly expressed in primary follicles in frozen sections of ovarian cortical tissue material obtained at laparoscopic surgery. We raised antipeptide antibodies against GDF-9 and showed by immunohistochemical studies on paraffin sections of whole human ovaries that the GDF-9 protein is most abundantly expressed in primary follicles. We recently demonstrated that a novel GDF-9-related factor, GDF-9B, is coexpressed with GDF-9 during murine folliculogenesis. We now isolated human GDF-9B complementary DNA and genomic clones and report the unusually restricted expression pattern of human GDF-9B. The human GDF-9B transcript can be detected only in the gonads by RT-PCR analysis, and in situ hybridization studies indicate that it is not expressed in small primary follicles but, rather, in the oocytes of late primary follicles. Functional studies using the Xenopus laeuis embryo model indicate that unlike the transforming growth factor-beta family members activin and bone morphogenetic protein-4, neither GDF-9 nor GDF-9B affects mesoderm induction, suggesting that they may use signaling pathways distinct from those well defined for activin and bone morphogenetic protein-4. We conclude that 1) both GDF-9 mRNA and protein are abundantly expressed in oocytes of primary follicles in human ovary, suggesting that the GDF-9 transcript is translated at this early stage of folliculogenesis; 2) human GDF-9B is specifically expressed in gonads at low levels; and 3) the expression of GDF-9 mRNA begins slightly earlier than that of GDF-9B in the human oocytes during follicular development. Our results are consistent with the suggestion that GDF-9 and GDF-9B may regulate human folliculogenesis in a manner specific to the ovary.

摘要

生长分化因子9(GDF - 9)是转化生长因子-β家族成员,雌性小鼠正常卵泡发生需要该因子,但它作为人类生育调节因子的作用仍不清楚。我们通过原位杂交和免疫组化分析确定了人卵泡发生过程中GDF - 9信使核糖核酸(mRNA)和蛋白质的定位。在原始卵泡中未检测到GDF - 9转录本,但在腹腔镜手术获取的卵巢皮质组织材料冰冻切片的初级卵泡中大量表达。我们制备了针对GDF - 9的抗肽抗体,并通过对整个人卵巢石蜡切片的免疫组化研究表明,GDF - 9蛋白在初级卵泡中表达最为丰富。我们最近证明,一种新型的GDF - 9相关因子GDF - 9B在小鼠卵泡发生过程中与GDF - 9共表达。我们现在分离了人GDF - 9B互补DNA和基因组克隆,并报告了人GDF - 9B异常受限的表达模式。通过RT - PCR分析,仅在性腺中可检测到人GDF - 9B转录本,原位杂交研究表明它不在小的初级卵泡中表达,而是在晚期初级卵泡的卵母细胞中表达。使用非洲爪蟾胚胎模型进行的功能研究表明,与转化生长因子-β家族成员激活素和骨形态发生蛋白-4不同,GDF - 9和GDF - 9B均不影响中胚层诱导,这表明它们可能使用与激活素和骨形态发生蛋白-4所明确的信号通路不同的信号通路。我们得出以下结论:1)GDF - 9 mRNA和蛋白在人卵巢初级卵泡的卵母细胞中大量表达,这表明GDF - 9转录本在卵泡发生的早期阶段被翻译;2)人GDF - 9B在性腺中低水平特异性表达;3)在卵泡发育过程中,人卵母细胞中GDF - 9 mRNA的表达比GDF - 9B略早开始。我们的结果与GDF - 9和GDF - 9B可能以卵巢特异性方式调节人卵泡发生的观点一致。

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