Temperature-controlled Structural Alterations of an RNA Thermometer

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Abstract

Thermoresponsive structures in the 5′-untranslated region of mRNA are known to control translation of heat shock and virulence genes. Expression of many rhizobial heat shock genes is regulated by a conserved sequence element called ROSE for repression of heat shock gene expression. This cis-acting, untranslated mRNA is thought to prevent ribosome access at low temperature through an extended secondary structure, which partially melts when the temperature rises. We show here by a series of in vivo and in vitro approaches that ROSE is a sensitive thermometer responding in the physiologically relevant temperature range between 30 and 40 °C. Point mutations predicted to disrupt base pairing enhanced expression at 30 °C. Compensatory mutations restored repression, emphasizing the importance of secondary structures in the sensory RNA. Only moderate inducibility of a 5′-truncated ROSE variant suggests that interactions between individual stem loops coordinate temperature sensing. In the presence of a complementary oligonucleotide, the functionally important stem loop of ROSE was rendered susceptible to RNase H treatment at heat shock temperatures. Since major structural rearrangements were not observed during UV and CD spectroscopy, subtle structural changes involving the Shine-Dalgarno sequence are proposed to mediate translational control. Temperature perception by the sensory RNA is an ordered process that most likely occurs without the aid of accessory factors.

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Chowdhury, S., Ragaz, C., Kreuger, E., & Narberhaus, F. (2003). Temperature-controlled Structural Alterations of an RNA Thermometer. Journal of Biological Chemistry, 278(48), 47915–47921. https://doi.org/10.1074/jbc.M306874200

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