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Posttranslational processing of mouse and human BMP-15: Potential implication in the determination of ovulation quota

机译:小鼠和人类BMP-15的翻译后加工:在确定排卵额方面的潜在意义

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摘要

There has been significant attention to the growing recognition that oocytes have a critical capacity to organize and govern surrounding somatic cells. Bone morphogenetic protein 15 (BMP-15) is an oocyte-secreted factor that has raised particular interest due to its established role in determining ovulation quota and female fertility in mammals. As a first step in determining whether there are species-specific differences in the BMP-15 system that may play causal roles in the differences in ovulation quota observed in different mammalian species, we here compare the molecular characteristics of BMP-15 of polyovulatory mice with that of monoovulatory humans. We found that, although human BMP-15 mature protein is readily produced, there are defects in the production of mouse BMP-15 mature protein in an in vitro system of transfected cells. The generation of chimeric constructs consisting of different combinations of mouse and human BMP-15 proregions, cleavage sites, and mature regions indicates that the defects in the production of mouse BMP-15 mature protein depend on the presence of the mouse BMP-15 proregion. The mouse proregion also caused a significant reduction in the production of human BMP-15 mature protein. The coexpression with a convertase cleavage enzyme, furin, results in complete processing of all these chimeras; however, no mouse mature protein is detected in either secreted or cell-confined forms except when associated with the human proregion. Based on the biological role of BMP-15, defects in the production of mouse BMP-15 mature protein could correlate with the high ovulation quota and litter size observed in mice.
机译:人们对卵母细胞具有组织和控制周围体细胞的关键能力的认识日益受到关注。骨形态发生蛋白15(BMP-15)是一种卵母细胞分泌因子,由于其在确定哺乳动物的排卵量和雌性育性中已确立的作用而引起了人们的特别关注。作为确定BMP-15系统中是否存在物种特异性差异的第一步,在不同哺乳动物物种中观察到的排卵配额差异中可能起因果作用,我们在此比较多排卵小鼠BMP-15的分子特征单排卵的人类。我们发现,尽管很容易产生人BMP-15成熟蛋白,但是在体外转染细胞系统中,小鼠BMP-15成熟蛋白的生产仍存在缺陷。由小鼠和人BMP-15前区,切割位点和成熟区的不同组合组成的嵌合构建体的产生表明,小鼠BMP-15成熟蛋白生产中的缺陷取决于小鼠BMP-15前区的存在。小鼠前区也引起人BMP-15成熟蛋白产量的显着降低。与转化酶裂解酶弗林蛋白酶的共表达可导致所有这些嵌合体的完整加工;但是,除了与人的前区相关联外,均未检测到分泌或细胞限制形式的小鼠成熟蛋白。基于BMP-15的生物学作用,小鼠BMP-15成熟蛋白生产中的缺陷可能与在小鼠中观察到的高排卵量和窝产仔数有关。

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