Literature DB >> 23035121

The N-terminal capping propensities of the D-helix modulate the allosteric activation of the Escherichia coli cAMP receptor protein.

Shaoning Yu1, Rodrigo A Maillard, Alexey V Gribenko, J Ching Lee.   

Abstract

Transduction of biological signals at the molecular level involves the activation and/or inhibition of allosteric proteins. In the transcription factor cAMP receptor protein (CRP) from Escherichia coli, the allosteric activation, or apo-holo transition, involves rigid body motions of domains and structural rearrangements within the hinge region connecting the cAMP- and DNA-binding domains. During this apo-holo transition, residue 138 is converted as part of the elongated D-helix to the position of the N-terminal capping residue of a shorter D-helix. The goal of the current study is to elucidate the role of residue 138 in modulating the allostery between cAMP and DNA binding. By systematically mutating residue 138, we found that mutants with higher N-terminal capping propensities lead to increased cooperativity of cAMP binding and a concomitant increase in affinity for lac-DNA. Furthermore, mutants with higher N-terminal capping propensity correlate with properties characteristic of holo-CRP, particularly, increase in protein structural dynamics. Overall, our results provide a quantitative characterization of the role of residue 138 in the isomerization equilibrium between the apo and holo forms of CRP, and in turn the thermodynamic underpin to the molecular model of allostery revealed by the high resolution structural studies.

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Year:  2012        PMID: 23035121      PMCID: PMC3501046          DOI: 10.1074/jbc.M112.404806

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  39 in total

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9.  Differential perturbation of intersubunit and interdomain communications by glycine 141 mutation in Escherichia coli CRP.

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Journal:  Biochemistry       Date:  1998-01-06       Impact factor: 3.162

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Authors:  Rati Chkheidze; Wilfredo Evangelista; Mark A White; Y Whitney Yin; J Ching Lee
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Review 5.  Cyclic-AMP and bacterial cyclic-AMP receptor proteins revisited: adaptation for different ecological niches.

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6.  cAMP is an allosteric modulator of DNA binding specificity in cAMP receptor protein from Mycobacterium tuberculosis.

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7.  Theoretical analysis of inducer and operator binding for cyclic-AMP receptor protein mutants.

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