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Publication : Structural basis for Hif-1 alpha /CBP recognition in the cellular hypoxic response.

First Author  Dames SA Year  2002
Journal  Proc Natl Acad Sci U S A Volume  99
Issue  8 Pages  5271-6
PubMed ID  11959977 Mgi Jnum  J:76075
Mgi Id  MGI:2178505 Doi  10.1073/pnas.082121399
Citation  Dames SA, et al. (2002) From the Cover: Structural basis for Hif-1alpha /CBP recognition in the cellular hypoxic response. Proc Natl Acad Sci U S A 99(8):5271-6
abstractText  The cellular response to low tissue oxygen concentrations is mediated by the hypoxia-inducible transcription factor HIF-1. Under hypoxic conditions, HIF-1 activates transcription of critical adaptive genes by recruitment of the general coactivators CBP/p300 through interactions with its alpha-subunit (Hif-1alpha). Disruption of the Hif-1alpha/p300 interaction has been linked to attenuation of tumor growth. To delineate the structural basis for this interaction, we have determined the solution structure of the complex between the carboxy-terminal activation domain (CAD) of Hif-1alpha and the zinc-binding TAZ1 (CH1) motif of cyclic-AMP response element binding protein (CREB) binding protein (CBP). Despite the overall similarity of the TAZ1 structure to that of the TAZ2 (part of the CH3) domain of CBP, differences occur in the packing of helices that can account for differences in specificity. The unbound CAD is intrinsically disordered and remains relatively extended upon binding, wrapping almost entirely around the TAZ1 domain in a groove through much of its surface. Three short helices are formed upon binding, stabilized by intermolecular interactions. The Asn-803 side chain, which functions as a hypoxic switch, is located on the second of these helices and is buried in the molecular interface. The third helix of the Hif-1alpha CAD docks in a deep hydrophobic groove in TAZ1, providing extensive intermolecular hydrophobic interactions that contribute to the stability of the complex. The structure of this complex provides new insights into the mechanism through which Hif-1alpha recruits CBP/p300 in response to hypoxia.
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