The type IIS restriction enzyme MmeI can cut across a double-strand break

BackgroundType-IIS restriction enzymes cut outside their recognition sites, allowing them to remove their binding sites upon digestion. This feature has resulted in their wide application in molecular biology techniques, including seamless cloning methods, enzymatic CRISPR library generation, and others. We studied the ability of the Type-IIS restriction enzyme MmeI, which recognizes an asymmetric sequence TCCRAC and cuts 20 bp downstream, to cut across a double-strand break (DSB).Methods and resultsWe used synthetic double-stranded oligos with MmeI recognition sites close to 5 ' end and different overhang lengths to measure digestion after different periods of time and at different temperatures. We found that the MmeI binding and cutting sites can be situated on opposite sides of a DSB if the edges of the DNA molecules are held together by transient base-pairing interactions between compatible overhangs.ConclusionWe found that MmeI can cut across a DSB, and the efficiency of the cutting depends on both overhang length and temperature.

Automated summary

In this study, it was found that the Type-IIS restriction enzyme MmeI, which recognizes the asymmetric sequence TCCRAC, can cut across a double-strand break (DSB). The efficiency of cutting depends on both overhang length and temperature.