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首页> 外文期刊>The Journal of biological chemistry >The Chromatin Regulator DMAP1 Modulates Activity of the Nuclear Factor κB (NF-κB) Transcription Factor Relish in the Drosophila Innate Immune Response
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The Chromatin Regulator DMAP1 Modulates Activity of the Nuclear Factor κB (NF-κB) Transcription Factor Relish in the Drosophila Innate Immune Response

机译:染色质调节剂DMAP1调节核因子κB(NF-κB)转录因子的活性在果蝇天生免疫应答中

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The host defense of the model organism Drosophila is under the control of two major signaling cascades controlling transcription factors of the NF-κB family, the Toll and the immune deficiency (IMD) pathways. The latter shares extensive similarities with the mammalian TNF-R pathway and was initially discovered for its role in anti-Gram-negative bacterial reactions. A previous interactome study from this laboratory reported that an unexpectedly large number of proteins are binding to the canonical components of the IMD pathway. Here, we focus on DNA methyltransferase-associated protein 1 (DMAP1), which this study identified as an interactant of Relish, a Drosophila transcription factor reminiscent of the mammalian p105 NF-κB protein. We show that silencing of DMAP1 expression both in S2 cells and in flies results in a significant reduction of Escherichia coli-induced expression of antimicrobial peptides. Epistatic analysis indicates that DMAP1 acts in parallel or downstream of Relish. Co-immunoprecipitation experiments further reveal that, in addition to Relish, DMAP1 also interacts with Akirin and the Brahma-associated protein 55 kDa (BAP55). Taken together, these results reveal that DMAP1 is a novel nuclear modulator of the IMD pathway, possibly acting at the level of chromatin remodeling.
机译:模型生物体果蝇的主体防御是控制两种主要信号级联控制NF-κB家族的转录因子,损害和免疫缺陷(IMD)途径。后者与哺乳动物TNF-R途径共享广泛的相似性,并且最初被发现在抗革兰阴性细菌反应中的作用。来自该实验室的先前互乱的研究报告说,意外大量的蛋白质与IMD途径的规范组分结合。这里,我们专注于DNA甲基转移酶相关蛋白1(DMAP1),该研究鉴定为依赖哺乳动物的杂交酰序列,使得哺乳动物P105 NF-κB蛋白质中的果蝇转录因子。我们表明,在S2细胞和恒定中,DMAP1表达的沉默导致大肠杆菌诱导的抗微生物肽表达的显着降低。背景分析表明DMAP1在津津乐道的平行或下游作用。共免疫沉淀实验进一步揭示了,除了依赖外,DMAP1还与Akirin和Brahma相关蛋白55kDa(BAP55)相互作用。总之,这些结果表明,DMAP1是IMD途径的新型核调节剂,可能在染色质重塑的水平上作用。

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