Eight-ring cyclic polyamides containing pyrrole (Py), imidazole (Im), and h
ydroxypyrrole (Hp) aromatic amino acids recognize predetermined six base pa
ir sites in the minor groove of DNA. Two four-ring polyamide subunits linke
d by (R)-2,4-diaminobutyric acid [(R)(H2N)gamma] residue form hairpin polya
mide structures with enhanced DNA binding properties. In hairpin poly amide
s, substitution of Hp/Py for Py/Py pairs enhances selectivity for T.A base
pairs but compromises binding affinity for specific sequences. In an effort
to enhance the binding properties of polyamides containing Hp/Py pairings,
four eight ring cyclic polyamides were synthesized and analyzed on a DNA r
estriction fragment containing three 6-bp sites 5'-tAGNNCTt-3', where NN =
AA, TA, or AT. Quantitative footprint titration experiments demonstrate tha
t contiguous placement of Hp/Py pairs in cy clo-(gamma -ImPyPyPy-(R)(H2N)ga
mma -ImHpHpPy-) (1) provides a 20-fold increase in affinity for the 5'-tAGA
ACTt-3' site (K-a = 7.5 x 10(7) M-1) relative to ImPyPyPy-(R)(H2N)gamma -Im
HpHpPy-C3-OH (2). A cyclic polyamide of sequence composition cyclo-(gamma -
ImHpPyPy-(R)(H2N)gamma -ImHpPyPy-) (3) binds a 5'-tAGTACTt-3' site with an
equilibrium association constant K-a = 3.2 x 10(9) M-1, representing a five
fold increase relative to the hairpin analogue ImHpPyPy-(R)(H2N)gamma -ImHp
PyPy-C3-OH (4). Arrangement of Hp/Py pairs in a 3'stagger regulates specifi
city of cyclo-(ImPyHpPy-(R)(H2N)gamma -ImPyHpPy-) (5) for the 5'-tAGATCT(t-
3') site (K-a=7.5x 10(7) M-1), threefold increase in affinity relative to t
he hairpin analogue ImPyHpPy-(R)(H2N)gamma -ImPyHpPy-C3-OH (6), respectivel
y. This study identifies cyclic polyamides as a viable motif for restoring
recognition properties of polyamides containing Hp/Py pairs.