Cyclic amplification and selection of targets (CASTing) for the myogenin consensus binding site.

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Mol Cell Biol. 1991 August; 11(8): 4104-4110

Cyclic amplification and selection of targets (CASTing) for the myogenin consensus binding site.

W E Wright, M Binder and W Funk

Department of Cell Biology and Neuroscience, University of Texas Southwestern Medical School, Dallas 75235.

ABSTRACT

The consensus binding site for the muscle regulatory factormyogenin was determined from an unbiased set of degenerate oligonucleotidesusing CASTing (cyclic amplification and selection of targets).Stretches of totally random sequence flanked by polymerase chainreaction priming sequences were mixed with purified myogeninor myotube nuclear extracts, DNA-protein complexes were immunoprecipitatedwith an antimyogenin antibody, and the DNA was amplified bypolymerase chain reaction. Specific binding was obtained afterfour to six cycles of CASTing. The population of selected bindingsites was then cloned, and a consensus was determined from sequencingindividual isolates. Starting from a pool with 14 random bases,purified myogenin yielded a consensus binding site of AACAG[T/C]TGTT,while nuclear extracts retrieved the sequence TTGCACCTGTTNNTTfrom a pool containing 35 random bases. The latter sequenceis consistent with that predicted from combining an E12/E47half-site (N[not T]CAC) with the purified myogenin half-site([T/C] TGTT). The presence of paired E boxes in many of thesequences isolated following CASTing with nuclear extracts provesthat myogenin can bind cooperatively with other E-box-bindingfactors.

Mol Cell Biol. 1991 August; 11(8): 4104-4110

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