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NF-kappaB p52:RelB heterodimer recognizes two classes of kappaB sites with two distinct modes

by Wang, Vivien Ya-Fan , Miller, Dustyn , Vu, Don , Fusco, Amanda J , Ghosh, Gourisankar , Huang, De-Bin

in Amino Acid Sequence / Amino Acid Substitution / Animals / Base Composition / Crystallography, X-Ray / Dimerization / DNA - chemistry / DNA - metabolism / Humans / Mice / Models, Molecular / Molecular Sequence Data / NF-kappa B p52 Subunit - chemistry / Point Mutation / Protein Binding / Protein Interaction Mapping / Protein Structure, Tertiary / Sequence Alignment / Structure-Activity Relationship / Substrate Specificity / Transcription Factor RelB - chemistry / Transcription, Genetic

2009

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NF-kappaB p52:RelB heterodimer recognizes two classes of kappaB sites with two distinct modes

by Wang, Vivien Ya-Fan , Miller, Dustyn , Vu, Don , Fusco, Amanda J , Ghosh, Gourisankar , Huang, De-Bin

2009

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NF-kappaB p52:RelB heterodimer recognizes two classes of kappaB sites with two distinct modes

by Wang, Vivien Ya-Fan , Miller, Dustyn , Vu, Don , Fusco, Amanda J , Ghosh, Gourisankar , Huang, De-Bin

2009

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Journal Article

NF-kappaB p52:RelB heterodimer recognizes two classes of kappaB sites with two distinct modes

Wang, Vivien Ya-Fan,

Miller, Dustyn,

Vu, Don,

Fusco, Amanda J,

Ghosh, Gourisankar,

Huang, De-Bin

2009

Overview

The X-ray structure of the nuclear factor-kappaB (NF-kappaB) p52:RelB:kappaB DNA complex reveals a new recognition feature not previously seen in other NF-kappaB:kappaB DNA complexes. Arg 125 of RelB is in contact with an additional DNA base pair. Surprisingly, the p52:RelB R125A mutant heterodimer shows defects both in DNA binding and in transcriptional activity only to a subclass of kappaB sites. We found that the Arg 125-sensitive kappaB sites contain more contiguous and centrally located A:T base pairs than do the insensitive sites. A protein-induced kink observed in this complex, which used an AT-rich kappaB site, might allow the DNA contact by Arg 125; such a kink might not be possible in complexes with non-AT-rich kappaB sites. Furthermore, we show that the p52:RelB heterodimer binds to a broader spectrum of kappaB sites when compared with the p50:RelA heterodimer. We suggest that the p52:RelB heterodimer is more adaptable to complement sequence and structural variations in kappaB sites when compared with other NF-kappaB dimers.

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Subject

Amino Acid Sequence

/ Amino Acid Substitution

/ Animals

/ Base Composition

/ Crystallography, X-Ray

/ Dimerization

/ DNA - chemistry

/ DNA - metabolism

/ Humans