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Drosophila Lin-52 Acts in Opposition to Repressive Components of the Myb-MuvB/dREAM Complex

机译:果蝇林52反对Myb-MuvB / dREAM复杂的压迫性成分。

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摘要

The Drosophila melanogaster Myb-MuvB/dREAM complex (MMB/dREAM) participates in both the activation and repression of developmentally regulated genes and origins of DNA replication. Mutants in MMB subunits exhibit diverse phenotypes, including lethality, eye defects, reduced fecundity, and sterility. Here, we used P-element excision to generate mutations in lin-52, which encodes the smallest subunit of the MMB/dREAM complex. lin-52 is required for viability, as null mutants die prior to pupariation. The generation of somatic and germ line mutant clones indicates that lin-52 is required for adult eye development and for early embryogenesis via maternal effects. Interestingly, the maternal-effect embryonic lethality, larval lethality, and adult eye defects could be suppressed by mutations in other subunits of the MMB/dREAM complex. These results suggest that a partial MMB/dREAM complex is responsible for the lethality and eye defects of lin-52 mutants. Furthermore, these findings support a model in which the Lin-52 and Myb proteins counteract the repressive activities of the other members of the MMB/dREAM complex at specific genomic loci in a developmentally controlled manner.
机译:果蝇Myb-MuvB / dREAM复合体(MMB / dREAM)参与激活和抑制发育调控基因和DNA复制的起源。 MMB亚基中的突变体表现出多种表型,包括致死性,眼缺陷,繁殖力降低和不育。在这里,我们使用P元素切除在lin-52中生成突变,该突变编码MMB / dREAM复合体的最小亚基。 lin-52是生存力所必需的,因为无效突变体会在粉碎之前死亡。体细胞和种系突变体克隆的产生表明,lin-52是成年眼睛发育和通过母体作用早期胚胎发生所必需的。有趣的是,MMB / dREAM复合体其他亚基的突变可以抑制母体效应的胚胎致死率,幼虫致死率和成年眼缺陷。这些结果表明,部分MMB / dREAM复合物负责lin-52突变体的致死性和眼缺陷。此外,这些发现支持了一个模型,其中Lin-52和Myb蛋白以发育受控的方式抵消了MMB / dREAM复合体其他成员在特定基因组位点的抑制活性。

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