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普茨格- NURF 核小体重塑复合物在黑腹果蝇的蜕皮激素受体信号转导和固有免疫中是必需的。

The Putzig-NURF nucleosome remodeling complex is required for ecdysone receptor signaling and innate immunity in Drosophila melanogaster.

机构信息

Institute of Genetics, University of Hohenheim, Stuttgart, Germany.

出版信息

Genetics. 2011 May;188(1):127-39. doi: 10.1534/genetics.111.127795. Epub 2011 Mar 8.

DOI:10.1534/genetics.111.127795
PMID:21385730
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3120143/
Abstract

Putzig (Pzg) was originally identified as being an integral component of the TRF2/DREF complex in Drosophila melanogaster, thereby regulating the transcriptional activation of replication-related genes. In a DREF-independent manner, Pzg was shown to mediate Notch target gene activation. This function of Pzg entails an association with the nucleosome remodeling factor complex NURF, which directly binds the ecdysone receptor EcR and coregulates targets of the EcR via the NURF-specific subunit Nurf-301. In contrast, Nurf-301 acts as a negative regulator of JAK/STAT signaling. Here, we provide evidence to show that Pzg is fundamental for these functions of NURF, apart from the regulation of Notch signaling activity. A jump-out mutagenesis provided us with a pzg null mutant displaying early larval lethality, defects in growth, and molting accompanied by aberrant feeding behavior. We show that Pzg is associated with EcR in vivo and required for the transcriptional induction of EcR target genes, whereas reduced ecdysteroid levels imply a NURF-independent function of Pzg. Moreover, pzg interferes with JAK/STAT-signaling activity by acting as a corepressor of Ken. Lamellocyte differentiation was consistently affected in a JAK/STAT mutant background and the expression level of defense response genes was elevated in pzg mutants, leading to the formation of melanotic tumors. Our results suggest that Pzg acts as an important partner of NURF in the regulation of EcR and JAK/STAT signaling.

摘要

普茨(Pzg)最初被鉴定为果蝇 TRF2/DREF 复合物的一个组成部分,从而调节与复制相关的基因的转录激活。以一种不依赖于 DREF 的方式,Pzg 被证明介导 Notch 靶基因的激活。Pzg 的这一功能需要与核小体重塑因子复合物 NURF 相关联,NURF 直接结合蜕皮激素受体 EcR,并通过 NURF 特异性亚基 Nurf-301 共同调节 EcR 的靶标。相比之下,Nurf-301 作为 JAK/STAT 信号的负调节剂。在这里,我们提供的证据表明,Pzg 除了调节 Notch 信号活性外,对于 NURF 的这些功能也是必不可少的。跳跃突变为我们提供了一个 pzg 缺失突变体,表现为早期幼虫致死、生长缺陷、蜕皮伴随着异常的摄食行为。我们表明,Pzg 与体内的 EcR 相关联,并且是 EcR 靶基因转录诱导所必需的,而降低的蜕皮激素水平暗示了 Pzg 的 NURF 独立功能。此外,pzg 通过作为 Ken 的核心抑制剂来干扰 JAK/STAT 信号活性。在 JAK/STAT 突变背景下,Lamellocyte 分化始终受到影响,并且在 pzg 突变体中防御反应基因的表达水平升高,导致黑色素瘤的形成。我们的结果表明,Pzg 在 EcR 和 JAK/STAT 信号的调节中作为 NURF 的一个重要伴侣发挥作用。

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本文引用的文献

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Genome-wide regulation of innate immunity by juvenile hormone and 20-hydroxyecdysone in the Bombyx fat body.保幼激素和 20-羟基蜕皮酮对家蚕脂肪体固有免疫的全基因组调控。
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A novel Pzg-NURF complex regulates Notch target gene activity.一种新型的 Pzg-NURF 复合物调节 Notch 靶基因活性。
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Genes of the ecdysone biosynthesis pathway are regulated by the dATAC histone acetyltransferase complex in Drosophila.蜕皮激素生物合成途径的基因受果蝇中 dATAC 组蛋白乙酰转移酶复合物的调控。
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ISWI regulates higher-order chromatin structure and histone H1 assembly in vivo.ISWI在体内调节高阶染色质结构和组蛋白H1组装。
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Mol Biol Cell. 2007 Oct;18(10):3733-40. doi: 10.1091/mbc.e07-03-0263. Epub 2007 Jul 18.