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Specific requirement of DRB4 a dsRNA-binding protein for the in vitro dsRNA-cleaving activity of Arabidopsis Dicer-like 4

机译:dsRNA结合蛋白DRB4对拟南芥Dicer-like 4的体外dsRNA裂解活性的特殊要求

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摘要

Arabidopsis thaliana Dicer-like 4 (DCL4) produces 21-nt small interfering RNAs from both endogenous and exogenous double-stranded RNAs (dsRNAs), and it interacts with DRB4, a dsRNA-binding protein, in vivo and in vitro. However, the role of DRB4 in DCL4 activity remains unclear because the dsRNA-cleaving activity of DCL4 has not been characterized biochemically. In this study, we biochemically characterize DCL4's Dicer activity and establish that DRB4 is required for this activity in vitro. Crude extracts from Arabidopsis seedlings cleave long dsRNAs into 21-nt small RNAs in a DCL4/DRB4-dependent manner. Immunoaffinity-purified DCL4 complexes produce 21-nt small RNAs from long dsRNA, and these complexes have biochemical properties similar to those of known Dicer family proteins. The DCL4 complexes purified from drb4-1 do not cleave dsRNA, and the addition of recombinant DRB4 to drb4-1 complexes specifically recovers the 21-nt small RNA generation. These results reveal that DCL4 requires DRB4 to cleave long dsRNA into 21-nt small RNAs in vitro. Amino acid substitutions in conserved dsRNA-binding domains (dsRBDs) of DRB4 impair three activities: binding to dsRNA, interacting with DCL4, and facilitating DCL4 activity. These observations indicate that the dsRBDs are critical for DRB4 function. Our biochemical approach and observations clearly show that DRB4 is specifically required for DCL4 activity in vitro.
机译:拟南芥Dicer-like 4(DCL4)从内源性和外源性双链RNA(dsRNA)产生21 nt小干扰RNA,并且在体内和体外与dsB结合蛋白DRB4相互作用。但是,DRB4在DCL4活性中的作用仍不清楚,因为DCL4的dsRNA裂解活性尚未进行生化表征。在这项研究中,我们对DCL4的Dicer活性进行了生化表征,并确定DRB4在体外是该活性所必需的。拟南芥幼苗的粗提物以DCL4 / DRB4依赖性的方式将长dsRNA裂解为21 nt小RNA。免疫亲和纯化的DCL4复合物从长dsRNA产生21 nt的小RNA,这些复合物的生化特性与已知的Dicer家族蛋白相似。从drb4-1纯化的DCL4复合物不切割dsRNA,并且将重组DRB4添加到drb4-1复合物可特异性地恢复21 nt小RNA的产生。这些结果表明,DCL4需要DRB4在体外将长dsRNA裂解为21 nt小RNA。 DRB4的保守dsRNA结合域(dsRBDs)中的氨基酸取代会削弱三种活性:与dsRNA结合,与DCL4相互作用以及促进DCL4活性。这些观察结果表明,dsRBD对于DRB4功能至关重要。我们的生化方法和观察结果清楚地表明,DRB4是体外DCL4活性所特有的。

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