Parallel synthesis of H-pin polyamides by alkene metathesis on solid phase
Abstract
A small library of H-pin polyamides with variable aliphatic bridge lengths (CH(2))(n)(), where n = 4-8, connecting a central Py/Py pair was prepared via parallel synthesis with Ru-catalyzed alkene metathesis on solid phase as a complexity-generating cross-linking reaction. DNA binding affinities and sequence specificities were analyzed for each member of the library to determine the optimum linker length. An H-pin polyamide with a six-methylene bridge was found to have the highest affinity to its match site with high selectivity over a 1-bp mismatch site. The relationship between the number of methylenes in the linker (CH(2))(n)() and affinity is n = 6 > 4 > 7 > 5 > 8. These results indicate that 6 followed by 4 methylene-bridged polyamides represent the optimum spacer length for the H-pin motif in the DNA minor groove. Importantly, the H-pin is competitive with hairpin polyamides with respect to affinity and specificity. The metathesis-based convergent synthetic route to H-pin polyamides expands the scope of readily available DNA recognition motifs for small molecule-based gene regulation studies.
Additional Information
© 2003 American Chemical Society. Received November 1, 2002. Publication Date (Web): March 29, 2003. We thank the National Institutes of Health (GM-27681) for research support and a postdoctoral fellowship to B.O. (F32 GM-19788). C.J. is grateful to California Institute of Technology for a Summer Undergraduate Research Fellowship.Attached Files
Supplemental Material - ja0213221_s.pdf
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Additional details
- Eprint ID
- 66808
- DOI
- 10.1021/ja0213221
- Resolver ID
- CaltechAUTHORS:20160510-081357762
- NIH
- GM-27681
- NIH Postdoctoral Fellowship
- F32 GM-19788
- Caltech Summer Undergraduate Research Fellowship (SURF)
- Created
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2016-05-18Created from EPrint's datestamp field
- Updated
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2021-11-11Created from EPrint's last_modified field