Towards mixed sequence recognition by triple helix formation
The formation of intermolecular DNA triple helices offers the possibility of designing
compounds with extensive sequence recognition properties which may be useful as
antigene agents or tools in molecular biology. One major limitation of this approach is that
these structures are generally restricted to homopurine homopyrimidine target sites. This
review describes the strategies that have been employed to overcome this drawback and
outlines the potential for triplex formation at mixed sequence DNA targets.
compounds with extensive sequence recognition properties which may be useful as
antigene agents or tools in molecular biology. One major limitation of this approach is that
these structures are generally restricted to homopurine homopyrimidine target sites. This
review describes the strategies that have been employed to overcome this drawback and
outlines the potential for triplex formation at mixed sequence DNA targets.
Abstract
The formation of intermolecular DNA triple helices offers the possibility of designing compounds with extensive sequence recognition properties which may be useful as antigene agents or tools in molecular biology. One major limitation of this approach is that these structures are generally restricted to homopurine homopyrimidine target sites. This review describes the strategies that have been employed to overcome this drawback and outlines the potential for triplex formation at mixed sequence DNA targets.
Oxford University Press