DNA mismatches reveal conformational penalties in protein-DNA recognition.

Date
2020-11
Authors
Afek, Ariel
Shi, Honglue
Rangadurai, Atul
Sahay, Harshit
Senitzki, Alon
Xhani, Suela
Fang, Mimi
Salinas, Raul
Mielko, Zachery
Pufall, Miles A
Poon, Gregory MK
Haran, Tali E
Schumacher, Maria A
Al-Hashimi, Hashim M
Gordân, Raluca
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Abstract
Transcription factors recognize specific genomic sequences to regulate complex gene-expression programs. Although it is well-established that transcription factors bind to specific DNA sequences using a combination of base readout and shape recognition, some fundamental aspects of protein-DNA binding remain poorly understood1,2. Many DNA-binding proteins induce changes in the structure of the DNA outside the intrinsic B-DNA envelope. However, how the energetic cost that is associated with distorting the DNA contributes to recognition has proven difficult to study, because the distorted DNA exists in low abundance in the unbound ensemble3-9. Here we use a high-throughput assay that we term SaMBA (saturation mismatch-binding assay) to investigate the role of DNA conformational penalties in transcription factor-DNA recognition. In SaMBA, mismatched base pairs are introduced to pre-induce structural distortions in the DNA that are much larger than those induced by changes in the Watson-Crick sequence. Notably, approximately 10% of mismatches increased transcription factor binding, and for each of the 22 transcription factors that were examined, at least one mismatch was found that increased the binding affinity. Mismatches also converted non-specific sites into high-affinity sites, and high-affinity sites into 'super sites' that exhibit stronger affinity than any known canonical binding site. Determination of high-resolution X-ray structures, combined with nuclear magnetic resonance measurements and structural analyses, showed that many of the DNA mismatches that increase binding induce distortions that are similar to those induced by protein binding-thus prepaying some of the energetic cost incurred from deforming the DNA. Our work indicates that conformational penalties are a major determinant of protein-DNA recognition, and reveals mechanisms by which mismatches can recruit transcription factors and thus modulate replication and repair activities in the cell10,11.
Type
Journal article
Subject
Humans
DNA-Binding Proteins
Saccharomyces cerevisiae Proteins
Arabidopsis Proteins
Transcription Factors
Nucleic Acid Heteroduplexes
Crystallography, X-Ray
Nuclear Magnetic Resonance, Biomolecular
Binding Sites
Molecular Conformation
Base Pairing
Protein Binding
Mutation
Thermodynamics
Models, Molecular
Permalink
https://hdl.handle.net/10161/25100
Published Version (Please cite this version)
10.1038/s41586-020-2843-2
Publication Info
Afek, Ariel; Shi, Honglue; Rangadurai, Atul; Sahay, Harshit; Senitzki, Alon; Xhani, Suela; ... Gordân, Raluca (2020). DNA mismatches reveal conformational penalties in protein-DNA recognition. Nature, 587(7833). pp. 291-296. 10.1038/s41586-020-2843-2. Retrieved from https://hdl.handle.net/10161/25100.
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Scholars@Duke

Al-Hashimi

Hashim Al-Hashimi

Adjunct Professor in the Department of Biochemistry
Mielko

Zachery Mielko

Postdoctoral Associate
Salinas

Raul Salinas

Research Associate, Senior
Schumacher

Maria Anne Schumacher

Nanaline H. Duke Distinguished Professor of Biochemistry
Alphabetical list of authors with Scholars@Duke profiles.
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