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黑腹果蝇卵巢和脂肪体中的卵黄原蛋白合成。

Ovarian and fat-body vitellogenin synthesis in Drosophila melanogaster.

作者信息

Isaac P G, Bownes M

出版信息

Eur J Biochem. 1982 Apr;123(3):527-34. doi: 10.1111/j.1432-1033.1982.tb06563.x.

Abstract

The ovary and the fat body of Drosophila melanogaster both synthesise vitellogenins in vivo. The ovary contributes nearly as much vitellogenin to the yolk of an oocyte as does the fat body. Densitometry of fluorographs and gels has been used to compare the amount of the smallest vitellogenin polypeptide, yolk protein 3, synthesised by each tissue. Cell-free translations indicate that the ovary, in contrast to the fat body, contains a much reduced level of the mRNA for yolk protein 3 compared with the mRNAs for the other vitellogenin polypeptides. However, if tissues are cultured in vitro, the underproduction of this protein by the ovary is not significant. Because young embryos have levels of this polypeptide which are expected if the ovary has a low level of its corresponding mRNA, we argue that the ovary genuinely underproduces this protein in vivo and that the relative levels synthesised by the ovary in vitro are an artefact. Egg chambers of previtellogenic stages can synthesise vitellogenins, but the maximum level of vitellogenin synthesis occurs in egg chambers of the early vitellogenic stages. We conclude that the expression of the vitellogenin genes is subject to different controls at each site of synthesis. The possible cell types responsible for ovarian vitellogenin synthesis are discussed; the follicle epithelial cells are tentatively nominated for this role. We also suggest that a specific repression mechanism for vitellogenin gene expression exists in the ovary.

摘要

黑腹果蝇的卵巢和脂肪体在体内均能合成卵黄原蛋白。卵巢对卵母细胞卵黄中卵黄原蛋白的贡献几乎与脂肪体相当。已通过对荧光照片和凝胶的光密度测定来比较每个组织合成的最小卵黄原蛋白多肽——卵黄蛋白3的量。无细胞翻译表明,与脂肪体相比,卵巢中卵黄蛋白3的mRNA水平与其他卵黄原蛋白多肽的mRNA相比大幅降低。然而,如果组织在体外培养,卵巢中该蛋白产量不足并不显著。由于年轻胚胎中该多肽的水平与卵巢中其相应mRNA水平较低时预期的水平相符,我们认为卵巢在体内确实会少产这种蛋白,而卵巢在体外合成的相对水平是一种假象。卵黄发生前期的卵室能够合成卵黄原蛋白,但卵黄原蛋白合成的最高水平出现在卵黄发生早期的卵室中。我们得出结论,卵黄原蛋白基因的表达在每个合成位点受到不同的调控。讨论了可能负责卵巢卵黄原蛋白合成的细胞类型;初步确定卵泡上皮细胞具有这一作用。我们还认为卵巢中存在一种针对卵黄原蛋白基因表达的特异性抑制机制。

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