AI Article Synopsis

  • The prokaryotic transcription factor CRP serves as a model to study protein allostery and the different effects of cyclic nucleotides cAMP and cGMP.
  • Crystal structures of inactive CRP forms provide insights into how these nucleotides induce conformational changes, demonstrating negative cooperativity in their binding.
  • cGMP, in particular, prompts an inhibitory change in CRP's structure, suggesting its potential role in regulating CRP-like proteins in prokaryotes.

Article Abstract

The prokaryotic global transcription factor CRP has been considered to be an ideal model for in-depth study of both the allostery of the protein and the differential utilization of the homologous cyclic nucleotide second messengers cAMP and cGMP. Here, atomic details from the crystal structures of two inactive CRP species, an apo form and a cGMP-bound form, in comparison with a known active conformation, the cAMP-CRP complex, provide macroscopic and microscopic insights into CRP allostery, which is coupled to specific discrimination between the two effectors. The cAMP-induced conformational transition, including dynamic fluctuations, can be driven by the fundamental folding forces that cause water-soluble globular proteins to construct an optimized hydrophobic core, including secondary-structure formation. The observed conformational asymmetries underlie a negative cooperativity in the sequential binding of cyclic nucleotides and a stepwise manner of binding with discrimination between the effector molecules. Additionally, the finding that cGMP, which is specifically recognized in a syn conformation, induces an inhibitory conformational change, rather than a null effect, on CRP supports the intriguing possibility that cGMP signalling could be widely utilized in prokaryotes, including in aggressive inhibition of CRP-like proteins.

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Source
http://dx.doi.org/10.1107/S139900471400724XDOI Listing

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