The Interface Between an Alternating CG Motif and a Random Sequence Motif Displays Altered Nuclease Activity

Abstract

Previously we described the B-Z junctions produced in oligomers containing (5meCG)₄ segments in the presence of 5.0 M NaCl or 50 uM Co(NH₃)₆ ⁺³ Sheardy, R.D. & Winkle, S.A., Biochemistry 28, 720–725 (1989); Winkle, S. A., Aloyo, M.C., Morales, N., Zambrano, T.Y. & Sheardy, R.D., Biochemistry 30, 10601–10606 (1991)]. The circular dichroism spectra of an analogous unmethylated oligomer containing (CG)₄, termed BZ-IV, in 5.0 M NaCl and in 50 uM CO(NH₃)⁺³ suggest, however, that this oligomer does not form a B-Z hybrid. BZ-IV possesses Hha I sites (CGCG) in the (CG)₄ segment and an Mbo I site (GATC) at the terminus of the (CG)₄ segment BZ-IV is equally digestible in the presence and absence of cobalt hexamine by Hha I, further indicating that the structure of BZ-IV is fully B-like under these conditions. The Mbo I cleavage site at the juncture between the (CG)₄ segment and the adjacent random segment displays enhanced cleavage by both Mbo I and its isoschizomer Sau3A I in the presence of cobalt hexamine. In addition, exonuclease IH digestion of BZ-IV is inhibited at this juncture. Actinomycin inhibits Mbo I activity in the presence of cobalt hexamine but not in the absence. Together, these results suggest that enzymes recognize the interfaces of (CG)n and adjacent random sequences as altered substrates even in the absence of a B-Z junction formation.