The Human SWI-SNF Complex Protein p270 Is an ARID Family Member with Non-Sequence-Specific DNA Binding Activity

doi:10.1128/MCB.20.9.3137-3146.2000

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Molecular and Cellular Biology, May 2000, p. 3137-3146, Vol. 20, No. 9
0270-7306/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

The Human SWI-SNF Complex Protein p270 Is an ARID Family Member with Non-Sequence-Specific DNA Binding Activity

Peter B. Dallas,¹^, Stephen Pacchione,¹ Deborah Wilsker,¹ Valerie Bowrin,¹ Ryuji Kobayashi,² and Elizabeth Moran¹^,^*

Fels Institute for Cancer Research and Molecular Biology, Temple University School of Medicine, Philadelphia, Pennsylvania 19140,¹ and Cold Spring Harbor Laboratory, Cold Spring Harbor, New York 11724²

Received 10 January 2000/Returned for modification 31 January 2000/Accepted 3 February 2000

p270 is an integral member of human SWI-SNF complexes, first identified through its shared antigenic specificity with p300and CREB binding protein. The deduced amino acid sequence of p270reported here indicates that it is a member of an evolutionarilyconserved family of proteins distinguished by the presence ofa DNA binding motif termed ARID (AT-rich interactive domain).The ARID consensus and other structural features are common toboth p270 and yeast SWI1, suggesting that p270 is a human counterpartof SWI1. The approximately 100-residue ARID sequence is presentin a series of proteins strongly implicated in the regulationof cell growth, development, and tissue-specific gene expression.Although about a dozen ARID proteins can be identified from databasesearches, to date, only Bright (a regulator of B-cell-specificgene expression), dead ringer (a Drosophila melanogaster geneproduct required for normal development), and MRF-2 (which repressesexpression from the cytomegalovirus enhancer) have been analyzeddirectly in regard to their DNA binding properties. Each bindspreferentially to AT-rich sites. In contrast, p270 shows no sequencepreference in its DNA binding activity, thereby demonstratingthat AT-rich binding is not an intrinsic property of ARID domainsand that ARID family proteins may be involved in a wider rangeof DNAinteractions.

^* Corresponding author. Mailing address: Fels Institute for Cancer Research and Molecular Biology, Temple University Schoolof Medicine, Philadelphia, PA. Phone: (215) 707-7313. Fax: (215)707-6989. E-mail: betty{at}unix.temple.edu.

Present address: Institute for Child Health Research, University of Western Australia, West Perth, Western Australia,Australia.

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