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The Drosophila caspases Strica and Dronc function redundantly in programmed cell death during oogenesis.

机译:果蝇caspases Strica和Dronc在卵子发生过程中的程序性细胞死亡中多余地起作用。

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Programmed cell death (PCD) in the Drosophila ovary occurs either during mid-oogenesis, resulting in degeneration of the entire egg chamber or during late oogenesis, to facilitate the development of the oocyte. PCD during oogenesis is regulated by mechanisms different from those that control cell death in other Drosophila tissues. We have analyzed the role of caspases in PCD of the female germline by examining caspase mutants and overexpressing caspase inhibitors. Imprecise P-element excision was used to generate mutants of the initiator caspase strica. While null mutants of strica or another initiator caspase, dronc, display no ovary phenotype, we find that strica exhibits redundancy with dronc, during both mid- and late oogenesis. Ovaries of double mutants contain defective mid-stage egg chambers similar to those reported previously in dcp-1 mutants, and mature egg chambers with persisting nurse cell nuclei. In addition, the effector caspases drice and dcp-1 also display redundant functions during late oogenesis, resulting in persisting nurse cell nuclei. These findings indicate that caspases are required for nurse cell death during mid-oogenesis, and participate in developmental nurse cell death during late oogenesis. This reveals a novel pathway of cell death in the ovary that utilizes strica, dronc, dcp-1 and drice, and importantly illustrates strong redundancy among the caspases.
机译:果蝇卵巢中的程序性细胞死亡(PCD)发生在产卵中期,导致整个卵室变性或产卵后期,以促进卵母细胞的发育。卵子发生期间的PCD受与控制其他果蝇组织中细胞死亡的机制不同的机制调控。我们已经通过检查胱天蛋白酶突变体和过表达胱天蛋白酶抑制剂来分析胱天蛋白酶在雌性生殖系PCD中的作用。不精确的P元素切除用于生成启动子胱天蛋白酶条纹的突变体。虽然纹状体或另一个启动子胱天蛋白酶,dronc的无效突变体没有显示卵巢表型,但我们发现,在卵中期和晚期,纹状体在dronc上显示出冗余。双重突变体的卵巢包含与先前在dcp-1突变体中报道的相似的有缺陷的中期卵腔,以及具有持久性护士细胞核的成熟卵腔。此外,效应子胱天蛋白酶drice和dcp-1在后期卵子发生过程中也显示出多余的功能,导致护士细胞核持续存在。这些发现表明,胱天蛋白酶对于产卵中期的护士细胞死亡是必需的,并且参与后期卵生期间发育的护士细胞死亡。这揭示了利用条纹,dronc,dcp-1和drice的卵巢细胞死亡的新途径,并重要地说明了胱天蛋白酶之间的强冗余。

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