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Silencing of RpATG6 impaired the yolk accumulation and the biogenesis of the yolk organelles in the insect vector R. prolixus

机译:RpATG6的沉默削弱了昆虫载体R. prolixus中的卵黄积累和卵黄细胞器的生物发生。

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摘要

In oviparous animals, the egg yolk is synthesized by the mother in a major metabolic challenge, where the different yolk components are secreted to the hemolymph and delivered to the oocytes mostly by endocytosis. The yolk macromolecules are then stored in a wide range of endocytic-originated vesicles which are collectively referred to as yolk organelles and occupy most of the mature oocytes cytoplasm. After fertilization, the contents of these organelles are degraded in a regulated manner to supply the embryo cells with fundamental molecules for de novo synthesis. Yolk accumulation and its regulated degradation are therefore crucial for successful development, however, most of the molecular mechanisms involved in the biogenesis, sorting and degradation of targeted yolk organelles are still poorly understood. ATG6 is part of two PI3P-kinase complexes that can regulate the recruitment of the endocytic or the autophagy machineries. Here, we investigate the role of RpATG6 in the endocytosis of the yolk macromolecules and in the biogenesis of the yolk organelles in the insect vector Rhodnius prolixus. We found that vitellogenic females express high levels of RpATG6 in the ovaries, when compared to the levels detected in the midgut and fat body. RNAi silencing of RpATG6 resulted in yolk proteins accumulated in the vitellogenic hemolymph, as a consequence of poor uptake by the oocytes. Accordingly, the silenced oocytes are unviable, white (contrasting to the control pink oocytes), smaller (62% of the control oocyte volume) and accumulate only 40% of the yolk proteins, 80% of the TAG and 50% of the polymer polyphosphate quantified in control oocytes. The cortex of silenced oocytes present atypical smaller vesicles indicating that the yolk organelles were not properly formed and/or sorted, which was supported by the lack of endocytic vesicles near the plasma membrane of silenced oocytes as seen by TEM. Altogether, we found that RpATG6 is central for the mechanisms of yolk accumulation, emerging as an important target for further investigations on oogenesis and, therefore, reproduction of this vector.
机译:在卵生动物中,蛋黄是母亲在主要的代谢挑战中合成的,卵黄中的不同蛋黄成分分泌到血淋巴中,主要通过内吞作用传递到卵母细胞。卵黄大分子然后存储在广泛的内吞起源的囊泡中,这些囊泡统称为卵黄细胞器,并占据大多数成熟卵母细胞的细胞质。受精后,这些细胞器的内容物以受控方式降解,为胚胎细胞提供从头合成的基本分子。因此,卵黄积累及其受调节的降解对于成功发育至关重要,但是,对靶向卵黄细胞器的生物发生,分选和降解的大多数分子机制仍知之甚少。 ATG6是两个PI3P激酶复合物的一部分,可以调节内吞或自噬机制的募集。在这里,我们研究了RpATG6在卵黄大分子内吞作用和昆虫载体Rhodnius prolixus中卵黄细胞器的生物发生中的作用。我们发现,与中肠和脂肪体内检测到的水平相比,卵黄形成的雌性在卵巢中表达高水平的RpATG6。 RpATG6的RNAi沉默导致卵黄蛋白在卵黄蛋白形成的血淋巴中积累,这是卵母细胞摄取不良的结果。因此,沉默的卵母细胞是不存活的,白色(与对照粉红色卵母细胞相反),较小(占对照卵母细胞体积的62%),并且仅积累40%的卵黄蛋白,80%的TAG和50%的聚合物多磷酸盐在对照卵母细胞中定量。沉默卵母细胞的皮层呈现非典型的较小囊泡,表明卵黄细胞器未正确形成和/或分选,这由TEM观察到的沉默卵母细胞质膜附近缺乏内吞性囊泡所支持。总的来说,我们发现RpATG6是卵黄积累机制的核心,正在成为进一步研究卵子发生和因此复制该载体的重要靶标。

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