Structural and dynamical characterization of the Miz-1 zinc fingers 5-8 by solution-state NMR.
 

Structural and dynamical characterization of the Miz-1 zinc fingers 5-8 by solution-state NMR.

http://www.bionmr.com//www.ncbi.nlm....ringerlink.gif Related Articles Structural and dynamical characterization of the Miz-1 zinc fingers 5-8 by solution-state NMR.

J Biomol NMR. 2013 Aug 24;

Authors: Bernard D, Bédard M, Bilodeau J, Lavigne P

Abstract
Myc-interacting zinc finger protein-1 (Miz-1) is a BTB/POZ transcription factor that activates the transcription of cytostatic genes, such as p15(INK4B) or p21(CIP1). The C-terminus of Miz-1 contains 13 consensus C2H2 zinc finger domains (ZF). ZFs 1-4 have been shown to interact with SMAD3/4, while the remaining ZFs are expected to bind the promoters of target genes. We have noted unusual features in ZF 5 and the linker between ZFs 5 and 6. Indeed, a glutamate is found instead of the conserved basic residue two positions before the second zinc-coordinating histidine on the ZF 5 helix, and the linker sequence is DTDKE in place of the classical TGEKP sequence. In a canonical ??? fold, such unusual primary structure elements should cause severe electrostatic repulsions. In this context, we have characterized the structure and the dynamics of a Miz-1 construct comprising ZFs 5-8 (Miz 5-8) by solution-state NMR. Whilst ZFs 5, 7 and 8 were shown to adopt the classical ??? fold for C2H2 ZFs, the number of long-range NOEs was insufficient to define a classical fold for ZF 6. We show by using (15)N-relaxation dispersion experiments that this lack of NOEs is due to the presence of extensive motions on the ?s-ms timescale. Since this negatively charged region would have to be located near the phosphodiester backbone in a DNA complex, we propose that in addition to promoting conformational searches, it could serve as a hinge region to keep ZFs 1-4 away from DNA.


PMID: 23975355 [PubMed - as supplied by publisher]



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