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Structural similarity between beta super(3)-peptides synthesized from beta super(3)-homo-amino acids and aspartic acid monomers
Formation of stable secondary structures by oligomers that mimic natural peptides is a key asset for enhanced biological response. Here we show that oligomeric beta super(3)-hexapeptides synthesized from l-aspartic acid monomers ( beta super(3)-peptides 1, 5a, and 6) or homologated beta super(3)-ami...
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| Published in: | Biopolymers 2014-07, Vol.102 (4), p.359-367 |
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| Main Authors: | , , |
| Format: | Article |
| Language: | English |
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| container_end_page | 367 |
| container_issue | 4 |
| container_start_page | 359 |
| container_title | Biopolymers |
| container_volume | 102 |
| creator | Ahmed, Sahar Sprules, Tara Kaur, Kamaljit |
| description | Formation of stable secondary structures by oligomers that mimic natural peptides is a key asset for enhanced biological response. Here we show that oligomeric beta super(3)-hexapeptides synthesized from l-aspartic acid monomers ( beta super(3)-peptides 1, 5a, and 6) or homologated beta super(3)-amino acids ( beta super(3)-peptide 2), fold into similar stable 14-helical secondary structures in solution, except that the former form right-handed 14-helix and the later form left-handed 14-helix. beta super(3)-Peptides from l-Asp monomers contain an additional amide bond in the side chains that provides opportunities for more hydrogen bonding. However, based on the NMR solution structures, we found that beta super(3)-peptide from l-Asp monomers (1) and from homologated amino acids (2) form similar structures with no additional side-chain interactions. These results suggest that the beta super(3)-peptides derived from l-Asp are promising peptide-mimetics that can be readily synthesized using l-Asp monomers as well as the right-handed 14-helical conformation of these beta super(3)-peptides (such as 1 and 6) may prove beneficial in the design of mimics for right-handed alpha -helix of alpha -peptides. copyright 2014 Wiley Periodicals, Inc. Biopolymers (Pept Sci) 102: 359-367, 2014. |
| doi_str_mv | 10.1002/bip.22510 |
| format | article |
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Here we show that oligomeric beta super(3)-hexapeptides synthesized from l-aspartic acid monomers ( beta super(3)-peptides 1, 5a, and 6) or homologated beta super(3)-amino acids ( beta super(3)-peptide 2), fold into similar stable 14-helical secondary structures in solution, except that the former form right-handed 14-helix and the later form left-handed 14-helix. beta super(3)-Peptides from l-Asp monomers contain an additional amide bond in the side chains that provides opportunities for more hydrogen bonding. However, based on the NMR solution structures, we found that beta super(3)-peptide from l-Asp monomers (1) and from homologated amino acids (2) form similar structures with no additional side-chain interactions. These results suggest that the beta super(3)-peptides derived from l-Asp are promising peptide-mimetics that can be readily synthesized using l-Asp monomers as well as the right-handed 14-helical conformation of these beta super(3)-peptides (such as 1 and 6) may prove beneficial in the design of mimics for right-handed alpha -helix of alpha -peptides. copyright 2014 Wiley Periodicals, Inc. 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These results suggest that the beta super(3)-peptides derived from l-Asp are promising peptide-mimetics that can be readily synthesized using l-Asp monomers as well as the right-handed 14-helical conformation of these beta super(3)-peptides (such as 1 and 6) may prove beneficial in the design of mimics for right-handed alpha -helix of alpha -peptides. copyright 2014 Wiley Periodicals, Inc. 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These results suggest that the beta super(3)-peptides derived from l-Asp are promising peptide-mimetics that can be readily synthesized using l-Asp monomers as well as the right-handed 14-helical conformation of these beta super(3)-peptides (such as 1 and 6) may prove beneficial in the design of mimics for right-handed alpha -helix of alpha -peptides. copyright 2014 Wiley Periodicals, Inc. Biopolymers (Pept Sci) 102: 359-367, 2014.</abstract><doi>10.1002/bip.22510</doi></addata></record> |
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| ispartof | Biopolymers, 2014-07, Vol.102 (4), p.359-367 |
| issn | 0006-3525 1097-0282 |
| language | eng |
| recordid | cdi_proquest_miscellaneous_1554954065 |
| source | Wiley |
| title | Structural similarity between beta super(3)-peptides synthesized from beta super(3)-homo-amino acids and aspartic acid monomers |
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