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Disruption of small RNA signaling caused by competition for Hfq

Disruption of small RNA signaling caused by competition for Hfq Small RNAs (sRNAs) regulate diverse pathways, including stress responses, virulence, and metabolism in Escherichia coli. At the center of this large sRNA regulatory network is the Hfq protein. Hfq mediates the binding of sRNAs to their target mRNAs; without Hfq, most sRNAs cannot efficiently regulate target mRNA expression. Here, we show in vivo that Hfq can be a limiting factor for sRNA activity and that it can be easily depleted, causing disruption of the sRNA network. Depletion of the available Hfq can occur when sRNAs and target mRNAs are transcribed at high levels without their partners, resulting in the sequestration of Hfq into sRNA–Hfq and target mRNA–Hfq complexes. This can be avoided by coordinating the transcription of sRNAs with their target mRNAs so that they are turned on and off together to maximize duplex formation and minimize Hfq sequestration. Therefore, the limited availability of Hfq results in a highly interdependent sRNA network, wherein the activity of each sRNA depends on the activity of the other sRNAs and target mRNAs in the network. http://www.deepdyve.com/assets/images/DeepDyve-Logo-lg.png Proceedings of the National Academy of Sciences PNAS

Disruption of small RNA signaling caused by competition for Hfq

Disruption of small RNA signaling caused by competition for Hfq

Proceedings of the National Academy of Sciences , Volume 108 (3): 1110 – Jan 18, 2011

Abstract

Small RNAs (sRNAs) regulate diverse pathways, including stress responses, virulence, and metabolism in Escherichia coli. At the center of this large sRNA regulatory network is the Hfq protein. Hfq mediates the binding of sRNAs to their target mRNAs; without Hfq, most sRNAs cannot efficiently regulate target mRNA expression. Here, we show in vivo that Hfq can be a limiting factor for sRNA activity and that it can be easily depleted, causing disruption of the sRNA network. Depletion of the available Hfq can occur when sRNAs and target mRNAs are transcribed at high levels without their partners, resulting in the sequestration of Hfq into sRNA–Hfq and target mRNA–Hfq complexes. This can be avoided by coordinating the transcription of sRNAs with their target mRNAs so that they are turned on and off together to maximize duplex formation and minimize Hfq sequestration. Therefore, the limited availability of Hfq results in a highly interdependent sRNA network, wherein the activity of each sRNA depends on the activity of the other sRNAs and target mRNAs in the network.

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Publisher
PNAS
Copyright
Copyright ©2011 by the National Academy of Sciences
ISSN
0027-8424
eISSN
1091-6490
Publisher site
See Article on Publisher Site

Abstract

Small RNAs (sRNAs) regulate diverse pathways, including stress responses, virulence, and metabolism in Escherichia coli. At the center of this large sRNA regulatory network is the Hfq protein. Hfq mediates the binding of sRNAs to their target mRNAs; without Hfq, most sRNAs cannot efficiently regulate target mRNA expression. Here, we show in vivo that Hfq can be a limiting factor for sRNA activity and that it can be easily depleted, causing disruption of the sRNA network. Depletion of the available Hfq can occur when sRNAs and target mRNAs are transcribed at high levels without their partners, resulting in the sequestration of Hfq into sRNA–Hfq and target mRNA–Hfq complexes. This can be avoided by coordinating the transcription of sRNAs with their target mRNAs so that they are turned on and off together to maximize duplex formation and minimize Hfq sequestration. Therefore, the limited availability of Hfq results in a highly interdependent sRNA network, wherein the activity of each sRNA depends on the activity of the other sRNAs and target mRNAs in the network.

Journal

Proceedings of the National Academy of SciencesPNAS

Published: Jan 18, 2011

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