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A Qrr Noncoding RNA Deploys Four Different Regulatory Mechanisms to Optimize Quorum-Sensing Dynamics

机译:Qrr非编码RNA部署四种不同的调控机制来优化群体感应动力学

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摘要

Quorum sensing is a cell-cell communication process that bacteria use to transition between individual and social lifestyles. In vibrios, homologous small RNAs called the Qrr sRNAs function at the center of quorum-sensing pathways. The Qrr sRNAs regulate multiple mRNA targets including those encoding the quorum-sensing regulatory components luxR, luxO, luxM, and aphA. We show that a representative Qrr, Qrr3, uses four distinct mechanisms to control its particular targets: the Qrr3 sRNA represses luxR through catalytic degradation, represses luxM through coupled degradation, represses luxO through sequestration, and activates aphA by revealing the ribosome binding site while the sRNA itself is degraded. Qrr3 forms different base-pairing interactions with each mRNA target, and the particular pairing strategy determines which regulatory mechanism occurs. Combined mathematicalmodeling and experiments show that the specific Qrr regulatory mechanism employed governs the potency, dynamics, and competition of target mRNA regulation, which in turn, defines the overall quorum-sensing response.
机译:群体感应是细菌用于在个人和社交生活方式之间转换的细胞间通信过程。在弧菌中,称为Qrr sRNA的同源小RNA在群体感应途径的中心起作用。 Qrr sRNA调节多个mRNA靶标,包括编码群体感应调节成分luxR,luxO,luxM和aphA的靶标。我们显示出代表性的Qrr,Qrr3,使用四种不同的机制来控制其特定靶标:Qrr3 sRNA通过催化降解抑制luxR,通过偶联降解抑制luxM,通过螯合抑制luxO,并通过揭示核糖体结合位点激活aphA。 sRNA本身被降解。 Qrr3与每个mRNA靶标形成不同的碱基配对相互作用,并且特定的配对策略决定了发生哪种调控机制。结合的数学模型和实验表明,采用的特定Qrr调控机制控制着目标mRNA调控的效价,动力学和竞争,进而定义了总体群体感应反应。

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