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DWA1 and DWA2 Two Arabidopsis DWD Protein Components of CUL4-Based E3 Ligases Act Together as Negative Regulators in ABA Signal Transduction

机译:DWA1和DWA2基于CUL4的E3 Ligas的两个拟南芥DWD蛋白成分在ABA信号转导中共同起负调控作用

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摘要

To elucidate potential roles of CUL4-DDB1-DWD (for Cullin 4-Damaged DNA Binding1-DDB1 binding WD40) E3 ligases in abscisic acid (ABA) signaling, we examined ABA sensitivities of T-DNA mutants of a number of Arabidopsis thaliana DWD genes, which encode substrate receptors for CUL4 E3 ligases. Mutants in two DWD genes, DWA1 and DWA2 (DWD hypersensitive to ABA1 and 2), had ABA-hypersensitive phenotypes. Both proteins interacted with DDB1 in yeast two-hybrid assays and associated with DDB1 and CUL4 in vivo, implying they could form CUL4-based complexes. Several ABA-responsive genes were hyperinduced in both mutants, and the ABA-responsive transcription factors ABA INSENSITIVE 5 (ABI5) and MYC2 accumulated to high levels in the mutants after ABA treatment. Moreover, ABI5 interacted with DWA1 and DWA2 in vivo. Cell-free degradation assays showed ABI5 was degraded more slowly in dwa1 and dwa2 than in wild-type cell extracts. Therefore, DWA1 and/or DWA2 may be the substrate receptors for a CUL4 E3 ligase that targets ABI5 for degradation. Our data indicate that DWA1 and DWA2 can directly interact with each other, and their double mutants exhibited enhanced ABA and NaCl hypersensitivities, implying they can act together. This report thus describes a previously unknown heterodimeric cooperation between two independent substrate receptors for CUL4-based E3 ligases.
机译:为了阐明CUL4-DDB1-DWD(对于结合Cullin 4的DNA损伤1-DDB1的WD40)E3连接酶在脱落酸(ABA)信号传导中的潜在作用,我们检查了许多拟南芥DWD基因T-DNA突变体的ABA敏感性。 ,它编码CUL4 E3连接酶的底物受体。两个DWD基因DWA1和DWA2(对ABA1和2高度敏感的DWD)的突变体具有ABA超敏感表型。两种蛋白在酵母双杂交检测中均与DDB1相互作用,并在体内与DDB1和CUL4相关,这意味着它们可以形成基于CUL4的复合物。在这两个突变体中都诱导了几个ABA反应性基因的过度诱导,并且在ABA处理后,ABA反应性转录因子ABA INSENSITIVE 5(ABI5)和MYC2积累到高水平。此外,ABI5在体内与DWA1和DWA2相互作用。无细胞降解试验表明,dwa1和dwa2中ABI5的降解速度比野生型细胞提取物中的降解慢。因此,DWA1和/或DWA2可能是靶向ABI5降解的CUL4 E3连接酶的底物受体。我们的数据表明DWA1和DWA2可以直接相互影响,并且它们的双突变体表现出增强的ABA和NaCl超敏性,这意味着它们可以一起起作用。因此,该报告描述了基于CUL4的E3连接酶的两个独立底物受体之间以前未知的异二聚体合作。

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