1RNL
THE NITRATE/NITRITE RESPONSE REGULATOR PROTEIN NARL FROM NARL
Summary for 1RNL
| Entry DOI | 10.2210/pdb1rnl/pdb |
| Descriptor | NITRATE/NITRITE RESPONSE REGULATOR PROTEIN NARL, PLATINUM (II) ION, GLYCEROL, ... (4 entities in total) |
| Functional Keywords | response regulators, two-component systems, signal transduction protein |
| Biological source | Escherichia coli str. K12 substr. |
| Total number of polymer chains | 1 |
| Total formula weight | 25275.37 |
| Authors | Baikalov, I.,Schroder, I.,Kaczor-Grzeskowiak, M.,Grzeskowiak, K.,Gunsalus, R.P.,Dickerson, R.E. (deposition date: 1996-04-17, release date: 1996-11-08, Last modification date: 2024-02-14) |
| Primary citation | Baikalov, I.,Schroder, I.,Kaczor-Grzeskowiak, M.,Grzeskowiak, K.,Gunsalus, R.P.,Dickerson, R.E. Structure of the Escherichia coli response regulator NarL. Biochemistry, 35:11053-11061, 1996 Cited by PubMed Abstract: The crystal structure analysis of the NarL protein provides a first look at interactions between receiver and effector domains of a full-length bacterial response regulator. The N-terminal receiver domain, with 131 amino acids, is folded into a 5-strand beta sheet flanked by 5 alpha helices, as seen in CheY and in the N-terminal domain of NTRC. The C-terminal DNA-binding domain, with 62 amino acids, is a compact bundle of 4 alpha helices, of which the middle 2 form a helix-turn-helix motif closely related to that of Drosophila paired protein and other H-T-H DNA-binding proteins. The 2 domains are connected by an alpha helix of 10 amino acids and a 13-residue flexible tether that is not visible and presumably disordered in the X-ray structure. In this unphosphorylated form of NarL, the C-terminal domain is turned against the receiver domain in a manner that would preclude DNA binding. Activation of NarL via phosphorylation of Asp59 must involve transfer of information to the interdomain interface and either rotation or displacement of the DNA-binding C-terminal domain. Docking of a B-DNA duplex against the isolated C-terminal domain in the manner observed in paired protein and other H-T-H proteins suggests a stereochemical basis for DNA sequence preference: T-R-C-C-Y (high affinity) or T-R-C-T-N (low affinity), which is close to the experimentally observed consensus sequence: T-A-C-Y-N. The NarL structure is a model for other members of the FixJ or LuxR family of bacterial transcriptional activators, and possibly to the more distant OmpR and NtrC families as well. PubMed: 8780507DOI: 10.1021/bi960919o PDB entries with the same primary citation |
| Experimental method | X-RAY DIFFRACTION (2.4 Å) |
Structure validation
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