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Title: | Cγ(S/R)-Bimodal Peptide Nucleic Acids (Cγ-bm-PNA) Form Coupled Double Duplexes by Synchronous Binding to Two Complementary DNA Strands |
Authors: | BHINGARDEVE, PRAMOD Madhanagopal, Bharath Raj GANESH, KRISHNA N. Dept. of Chemistry |
Keywords: | Chemistry 2021-JAN-WEEK4 TOC-JAN-2021 2020 |
Issue Date: | Nov-2020 |
Publisher: | American Chemical Society |
Citation: | Journal of Organic Chemistry, 85(21), 13680-13693. |
Abstract: | Peptide nucleic acids (PNAs) are linear equivalents of DNA with a neutral acyclic polyamide backbone that has nucleobases attached via tert-amide link on repeating units of aminoethylglycine. They bind complementary DNA or RNA with sequence specificity to form hybrids that are more stable than the corresponding DNA/RNA self-duplexes. A new type of PNA termed bimodal PNA [Cγ(S/R)-bm-PNA] is designed to have a second nucleobase attached via amide spacer to a side chain at Cγ on the repeating aeg units of PNA oligomer. Cγ-bimodal PNA oligomers that have two nucleobases per aeg unit are demonstrated to concurrently bind two different complementary DNAs, to form duplexes from both tert-amide side and Cγ side. In such PNA:DNA ternary complexes, the two duplexes share a common PNA backbone. The ternary DNA 1:Cγ(S/R)-bm-PNA:DNA 2 complexes exhibit better thermal stability than the isolated duplexes, and the Cγ(S)-bm-PNA duplexes are more stable than Cγ(R)-bm-PNA duplexes. Bimodal PNAs are first examples of PNA analogues that can form DNA2:PNA:DNA1 double duplexes via recognition through natural bases. The conjoined duplexes of Cγ-bimodal PNAs can be used to generate novel higher-level assemblies. |
URI: | http://dr.iiserpune.ac.in:8080/xmlui/handle/123456789/5574 https://doi.org/10.1021/acs.joc.0c01853 |
ISSN: | 0022-3263 1520-6904 |
Appears in Collections: | JOURNAL ARTICLES |
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