Gsdf 的缺失导致了鱼类卵母细胞发育过程中 Igf2bp3 介导的失调。

Loss of Gsdf leads to a dysregulation of Igf2bp3-mediated oocyte development in medaka.

机构信息

Key Laboratory of Exploration and Utilization of Aquatic Genetic Resources, Ministry of Education, Shanghai 201306, China; Shanghai Collaborative Innovation for Aquatic Animal Genetics and Breeding, College of Fisheries and Life Sciences, Shanghai Ocean University, Shanghai 201306, China.

Department of Obstetrics and Gynecology, Sun Yat-sen Memorial Hospital, Sun Yat-sen University Yanjiang Road 107, Guangdong 510120, China.

出版信息

Gen Comp Endocrinol. 2019 Jun 1;277:122-129. doi: 10.1016/j.ygcen.2019.04.001. Epub 2019 Apr 2.

DOI:10.1016/j.ygcen.2019.04.001

PMID:30951723

Abstract

Gonadal soma-derived factor (Gsdf) is a unique TGF-β factor essential for both ovarian and testicular development in Hd-rR medaka (Oryzias latipes). However, the downstream genes regulated by Gsdf signaling remain unknown. Using a high-throughput proteomic approach, we identified a significant increase in the expression of the RNA-binding protein Igf2bp3 in gsdf-deficient ovaries. We verified this difference in transcription and protein expression against normal gonads using real-time PCR quantification and Western blotting. The genomic structure of igf2bp3 and the syntenic flanking segments are highly conserved across fish and mammals. igf2bp3 expression was correlated with oocyte development, which is consistent with the expression of the igf2bp3 ortholog Vg1-RBP/Vera in Xenopus. In contrast to the normal ovary, cysts of H3K27me3- and Igf2bp3-positive germ cells were dramatically increased in the one-month-old gsdf-deficient ovary, indicating that the gsdf depletion led to a dysregulation of Igf2bp3-mediated oocyte development. Our results provide novel insights into the Gsdf-Igf2bp3 signaling mechanisms that underlie the fundamental process of gametogenesis; these mechanisms may be well conserved across phyla.

摘要

生殖嵴源性因子（Gsdf）是一种独特的 TGF-β 因子，对于水稻斑纹型隐性致死突变系（Oryzias latipes）的卵巢和睾丸发育都是必需的。然而，Gsdf 信号调控的下游基因仍然未知。我们使用高通量蛋白质组学方法，发现 gsdf 缺陷型卵巢中 RNA 结合蛋白 Igf2bp3 的表达显著增加。我们使用实时 PCR 定量和 Western blot 验证了与正常性腺相比转录和蛋白表达的这种差异。igf2bp3 的基因组结构和相邻的侧翼片段在鱼类和哺乳动物中高度保守。igf2bp3 的表达与卵母细胞发育相关，这与 Xenopus 中的 igf2bp3 同源物 Vg1-RBP/Vera 的表达一致。与正常卵巢相比，gsdf 缺陷型卵巢中 1 月龄时 H3K27me3 和 Igf2bp3 阳性生殖细胞的小囊泡显著增加，表明 Gsdf 耗竭导致 Igf2bp3 介导的卵母细胞发育失调。我们的结果为 Gsdf-Igf2bp3 信号机制提供了新的见解，这些机制是配子发生这一基本过程的基础；这些机制在门之间可能很好地保守。

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Gsdf 的缺失导致了鱼类卵母细胞发育过程中 Igf2bp3 介导的失调。

Loss of Gsdf leads to a dysregulation of Igf2bp3-mediated oocyte development in medaka.

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