Efficient synthesis of carbopeptoid oligomers: insight into mimicry of β-peptide

Yoshitomo Suhara; Masaaki Kurihara; Atsushi Kittaka; Yoshitaka Ichikawa

doi:10.1016/j.tet.2006.05.080

Efficient synthesis of carbopeptoid oligomers: insight into mimicry of β-peptide

Yoshitomo Suhara, Masaaki Kurihara, Atsushi Kittaka, Yoshitaka Ichikawa

研究成果: Article › 査読

15 被引用数 (Scopus)

抄録

The ready access to a new class of carbohydrate mimetics was demonstrated by the synthesis of tetrameric carbopeptoids, in which glycosidic bonds were replaced with amide linkages. We herein describe the detailed synthetis method of β(1→2)- and β(1→6)-linked carbopeptoids starting from each d-glucosamine and d-glucose derivative. The building blocks were polymerized using BOP reagent and DIEA to form a homooligomer. These produced carbopeptoids are resistant to glycosidases and have interesting biological activity. With conformational analysis by molecular modeling calculation, β(1→2)-linked decamer showed a typical 16-helix form as a mimic of β-peptide. Therefore, our polysaccharide analogues have potential as peptide foldamers.

本文言語	English
ページ（範囲）	8207-8217
ページ数	11
ジャーナル	Tetrahedron
巻	62
号	34
DOI	https://doi.org/10.1016/j.tet.2006.05.080
出版ステータス	Published - 2006 8月 21
外部発表	はい

ASJC Scopus subject areas

生化学
創薬
有機化学

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10.1016/j.tet.2006.05.080

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title = "Efficient synthesis of carbopeptoid oligomers: insight into mimicry of β-peptide",

abstract = "The ready access to a new class of carbohydrate mimetics was demonstrated by the synthesis of tetrameric carbopeptoids, in which glycosidic bonds were replaced with amide linkages. We herein describe the detailed synthetis method of β(1→2)- and β(1→6)-linked carbopeptoids starting from each d-glucosamine and d-glucose derivative. The building blocks were polymerized using BOP reagent and DIEA to form a homooligomer. These produced carbopeptoids are resistant to glycosidases and have interesting biological activity. With conformational analysis by molecular modeling calculation, β(1→2)-linked decamer showed a typical 16-helix form as a mimic of β-peptide. Therefore, our polysaccharide analogues have potential as peptide foldamers.",

author = "Yoshitomo Suhara and Masaaki Kurihara and Atsushi Kittaka and Yoshitaka Ichikawa",

note = "Funding Information: The NMR studies were performed in the Biochemistry NMR Facility at Johns Hopkins University, which was established by a grant from the National Institute of Health (GM 27512) and a Biomedical Shared Instrumentation Grant (1S10-RR062620-0). A fellowship from Uehara Memorial Foundation (to Y.S.) is gratefully acknowledged.",

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AU - Suhara, Yoshitomo

AU - Kurihara, Masaaki

AU - Kittaka, Atsushi

AU - Ichikawa, Yoshitaka

N1 - Funding Information: The NMR studies were performed in the Biochemistry NMR Facility at Johns Hopkins University, which was established by a grant from the National Institute of Health (GM 27512) and a Biomedical Shared Instrumentation Grant (1S10-RR062620-0). A fellowship from Uehara Memorial Foundation (to Y.S.) is gratefully acknowledged.

PY - 2006/8/21

Y1 - 2006/8/21

N2 - The ready access to a new class of carbohydrate mimetics was demonstrated by the synthesis of tetrameric carbopeptoids, in which glycosidic bonds were replaced with amide linkages. We herein describe the detailed synthetis method of β(1→2)- and β(1→6)-linked carbopeptoids starting from each d-glucosamine and d-glucose derivative. The building blocks were polymerized using BOP reagent and DIEA to form a homooligomer. These produced carbopeptoids are resistant to glycosidases and have interesting biological activity. With conformational analysis by molecular modeling calculation, β(1→2)-linked decamer showed a typical 16-helix form as a mimic of β-peptide. Therefore, our polysaccharide analogues have potential as peptide foldamers.

AB - The ready access to a new class of carbohydrate mimetics was demonstrated by the synthesis of tetrameric carbopeptoids, in which glycosidic bonds were replaced with amide linkages. We herein describe the detailed synthetis method of β(1→2)- and β(1→6)-linked carbopeptoids starting from each d-glucosamine and d-glucose derivative. The building blocks were polymerized using BOP reagent and DIEA to form a homooligomer. These produced carbopeptoids are resistant to glycosidases and have interesting biological activity. With conformational analysis by molecular modeling calculation, β(1→2)-linked decamer showed a typical 16-helix form as a mimic of β-peptide. Therefore, our polysaccharide analogues have potential as peptide foldamers.

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Efficient synthesis of carbopeptoid oligomers: insight into mimicry of β-peptide

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