Published June 15, 2015 | Version v1
Journal article Open

Intermolecular epistasis shaped the function and evolution of an ancient transcription factor and its DNA binding sites

  • 1. University of Oregon
  • 2. University of Chicago

Description

Complexes of specifically interacting molecules, such as transcription factor proteins (TFs) and the DNA response elements (REs) they recognize, control most biological processes, but little is known concerning the functional and evolutionary effects of epistatic interactions across molecular interfaces. We experimentally characterized all combinations of genotypes in the joint protein-DNA sequence space defined by an historical transition in TF-RE specificity that occurred some 500 million years ago in the DNA-binding domain of an ancient steroid hormone receptor. We found that rampant epistasis within and between the two molecules was essential to specific TF-RE recognition and to the evolution of a novel TF-RE complex with unique derived specificity. Permissive and restrictive epistatic mutations across the TF-RE interface opened and closed potential evolutionary paths accessible by the other, making the evolution of each molecule contingent on its partner's history and allowing a molecular complex with novel specificity to evolve.

Data availability

The following previously published data sets were used:

McKeown AN Bridgham JT Anderson DW Murphy MN Ortlund EA Thornton JW (2014) Ancestral Steroid Receptor 1 in complex with estrogen response element DNA Publicly available at RCSB Protein Data Bank (Accession No: 4OLN). http://www.rcsb.org/pdb/explore/explore.do?structureId=4OLN

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Additional details

Identifiers

DOI
10.7554/eLife.07864
Other
oai:uchicago.tind.io:9881

Funding

American Heart Association
11PRE7510085
National Institutes of Health
R01-GM104397
National Institutes of Health
5-T32-GM-7759-33
Howard Hughes Medical Institute
Early Career Scientist Award

UChicago Information

Division(s)
Biological Sciences Division
Department(s)
Ecology and Evolution, Human Genetics