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Holo-repressor

The crystal structures of DtxR and IdeR provide a detailed picture of this protein family (Figure 3.7, Plate 5). The N-terminal domain (residues 1-73) containing a helix-turn-helix motif binds a recognition nucleotide sequence of about 21 base pairs, as is nicely shown in a cocrystal of DNA and DtxR (Pohl et al., 1999). The central domain (74-140) has a function in dimerization the role of the third carboxy-terminal domain (141-230) is uncertain. Although metal-binding sites have been defined in these crystal structures, the mechanism by which metal binding causes the structural changes between apo- and holo-repressor is not clear. [Pg.114]

The crystal structure of metal-ion activated DtxR suggests two, mutually nonexclusive, models for the mechanism of activation of this repressor. Comparison of the apo- and holo-repressors shows a conformational change between the two sub-... [Pg.363]

One of the first metalloregulatory proteins to be characterized extensively is the prokaryotic MerR transcription factor (1, 6, 7), which acts either as a repressor (apo-protein) or an activator (holo-protein) of the mer operon encoding mercury resistance proteins (Fig. Ic). The —35 and —10 sequence elements of the mer promoter, binding sites for the RNA polymerase initiation complex, are separated by an unusually long distance that results in poor constitutive transcription. Apo-MerR binds to the DNA between these sequences and bends the DNA, which results in a slight increase in repression on the suboptimal promoter. It also recruits the RNA polymerase to the transcription start site where it waits in a stalled complex. Upon binding of... [Pg.1080]

Pohl E, Holmes RK, Hoi WGJ. Motion of the DNA-binding domain with respect to the core of the diphtheria toxin repressor (DtxR) revealed in the crystal structures of apo- and holo-DtxR. J. Biol. Chem. 1998 273 22420-22427. [Pg.1088]


See other pages where Holo-repressor is mentioned: [Pg.362]    [Pg.365]    [Pg.368]    [Pg.450]    [Pg.362]    [Pg.365]    [Pg.368]    [Pg.450]    [Pg.211]    [Pg.1083]    [Pg.363]    [Pg.200]    [Pg.102]   
See also in sourсe #XX -- [ Pg.362 , Pg.365 , Pg.368 ]




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