2016
DOI: 10.1002/prot.24990
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A genetic and physical study of the interdomain linker ofE. ColiAraC protein-atrans-subunit communication pathway

Abstract: Genetic experiments with full length AraC and biophysical experiments with its dimerization domain plus linker suggest that arabinose binding to the dimerization domain changes the properties of the inter-domain linker which connects the dimerization domain to the DNA binding domain via interactions that do not depend on the DNA binding domain. Normal AraC function was found to tolerate considerable linker sequence alteration excepting proline substitutions. The proline substitutions partially activate transcr… Show more

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Cited by 8 publications
(15 citation statements)
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“…The interacting residues (green) are shown bonding (dotted lines) with the ligand. -López et al, 2015;Malaga et al, 2016). Table 11 presents the best results against AraC family transcriptional regulator (melR) where ZINC71781167 was predicted as top lead compound as shown in Figure 9.…”
Section: Zinc Idmentioning
confidence: 99%
“…The interacting residues (green) are shown bonding (dotted lines) with the ligand. -López et al, 2015;Malaga et al, 2016). Table 11 presents the best results against AraC family transcriptional regulator (melR) where ZINC71781167 was predicted as top lead compound as shown in Figure 9.…”
Section: Zinc Idmentioning
confidence: 99%
“…One demonstration of linker conformation effects on transcription is the AraC bacterial transcriptional regulator. In one conformation (suspected to be a random coil) AraC forms a repressive loop between distant molecules bound to DNA, whereas a change in linker conformation (proposed to be an increase in helicity) reorients the AraC dimer, and it binds to adjacent, activating sites on DNA (44). Recent studies have discovered that disordered proteins are abundant in proteomes across all domains of life and functionally significant.…”
Section: Elimination Of H-ns Binding Does Not Affect Nucleoid Compactmentioning
confidence: 99%
“…However, the structure of effector‐bound ToxT is monomeric 29 . Thus, information about inter‐domain and inter‐monomer contacts in full‐length AraC/XylS homodimers have largely been inferred from substitution experiments that diminish or enhance activity 31‐39 …”
Section: Figurementioning
confidence: 99%