Combinatorial Solid-Phase Synthesis and Biological Evaluation of Cyclodepsipeptide Destruxin B as a Negative Regulator for Osteoclast Morphology

Hiroshi Sato; Masahito Yoshida; Hayato Murase; Hiroshi Nakagawa; Takayuki Doi

doi:10.1021/acscombsci.6b00076

Combinatorial Solid-Phase Synthesis and Biological Evaluation of Cyclodepsipeptide Destruxin B as a Negative Regulator for Osteoclast Morphology

Hiroshi Sato, Masahito Yoshida, Hayato Murase, Hiroshi Nakagawa, Takayuki Doi

Research output: Contribution to journal › Article › peer-review

7 Citations (Scopus)

Abstract

Combinatorial synthesis and biological evaluation of cyclodepsipeptide destruxin B have been achieved. The cyclization precursors were prepared by solid-phase peptide synthesis via a split and pool method utilizing SynPhase lanterns with colored tags and cogs, followed by cleavage from the polymer-support. Macrolactonization utilizing MNBA-DMAPO in solution-phase was successfully performed in parallel to afford the desired 64-member destruxin analogues in moderate to good yields. Biological evaluation of the synthesized analogues indicated that a MeAla residue for the building block A is required to induce the desired morphological changes in osteoclast-like multinuclear cells (OCLs), and introduction of the substituent at the R⁴ position of a proline moiety is tolerated by the morphology and may enable the preparation of a molecular probe for the target identification in the osteoclasts.

Original language	English
Pages (from-to)	590-595
Number of pages	6
Journal	ACS Combinatorial Science
Volume	18
Issue number	9
DOIs	https://doi.org/10.1021/acscombsci.6b00076
Publication status	Published - 2016 Sept 12

Keywords

combinatorial library
cyclic peptides
cyclodepsipeptides
osteoclasts
solid-phase synthesis

ASJC Scopus subject areas

Chemistry(all)

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10.1021/acscombsci.6b00076

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title = "Combinatorial Solid-Phase Synthesis and Biological Evaluation of Cyclodepsipeptide Destruxin B as a Negative Regulator for Osteoclast Morphology",

abstract = "Combinatorial synthesis and biological evaluation of cyclodepsipeptide destruxin B have been achieved. The cyclization precursors were prepared by solid-phase peptide synthesis via a split and pool method utilizing SynPhase lanterns with colored tags and cogs, followed by cleavage from the polymer-support. Macrolactonization utilizing MNBA-DMAPO in solution-phase was successfully performed in parallel to afford the desired 64-member destruxin analogues in moderate to good yields. Biological evaluation of the synthesized analogues indicated that a MeAla residue for the building block A is required to induce the desired morphological changes in osteoclast-like multinuclear cells (OCLs), and introduction of the substituent at the R4 position of a proline moiety is tolerated by the morphology and may enable the preparation of a molecular probe for the target identification in the osteoclasts.",

keywords = "combinatorial library, cyclic peptides, cyclodepsipeptides, osteoclasts, solid-phase synthesis",

author = "Hiroshi Sato and Masahito Yoshida and Hayato Murase and Hiroshi Nakagawa and Takayuki Doi",

note = "Funding Information: Financial contribution from JSPS KAKENHI Grant Numbers JP15H05837 in Middle Molecular Strategy, JP26282208, and the Platform Project for Supporting in Drug Discovery and Life Science Research from Japan Agency for Medical Research and Development (AMED) are gratefully acknowledged. Publisher Copyright: {\textcopyright} 2016 American Chemical Society. Copyright: Copyright 2016 Elsevier B.V., All rights reserved.",

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doi = "10.1021/acscombsci.6b00076",

language = "English",

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AU - Sato, Hiroshi

AU - Yoshida, Masahito

AU - Murase, Hayato

AU - Nakagawa, Hiroshi

AU - Doi, Takayuki

N1 - Funding Information: Financial contribution from JSPS KAKENHI Grant Numbers JP15H05837 in Middle Molecular Strategy, JP26282208, and the Platform Project for Supporting in Drug Discovery and Life Science Research from Japan Agency for Medical Research and Development (AMED) are gratefully acknowledged. Publisher Copyright: © 2016 American Chemical Society. Copyright: Copyright 2016 Elsevier B.V., All rights reserved.

PY - 2016/9/12

Y1 - 2016/9/12

N2 - Combinatorial synthesis and biological evaluation of cyclodepsipeptide destruxin B have been achieved. The cyclization precursors were prepared by solid-phase peptide synthesis via a split and pool method utilizing SynPhase lanterns with colored tags and cogs, followed by cleavage from the polymer-support. Macrolactonization utilizing MNBA-DMAPO in solution-phase was successfully performed in parallel to afford the desired 64-member destruxin analogues in moderate to good yields. Biological evaluation of the synthesized analogues indicated that a MeAla residue for the building block A is required to induce the desired morphological changes in osteoclast-like multinuclear cells (OCLs), and introduction of the substituent at the R4 position of a proline moiety is tolerated by the morphology and may enable the preparation of a molecular probe for the target identification in the osteoclasts.

AB - Combinatorial synthesis and biological evaluation of cyclodepsipeptide destruxin B have been achieved. The cyclization precursors were prepared by solid-phase peptide synthesis via a split and pool method utilizing SynPhase lanterns with colored tags and cogs, followed by cleavage from the polymer-support. Macrolactonization utilizing MNBA-DMAPO in solution-phase was successfully performed in parallel to afford the desired 64-member destruxin analogues in moderate to good yields. Biological evaluation of the synthesized analogues indicated that a MeAla residue for the building block A is required to induce the desired morphological changes in osteoclast-like multinuclear cells (OCLs), and introduction of the substituent at the R4 position of a proline moiety is tolerated by the morphology and may enable the preparation of a molecular probe for the target identification in the osteoclasts.

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Combinatorial Solid-Phase Synthesis and Biological Evaluation of Cyclodepsipeptide Destruxin B as a Negative Regulator for Osteoclast Morphology

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Keywords

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