Alternative synthetic approach for (+)-phomopsidin via the highly stereoselective TADA reaction

Nobuyuki Hayashi; Takahiro Suzuki; Kenji Usui; Masahisa Nakada

doi:10.1016/j.tet.2008.11.030

Alternative synthetic approach for (+)-phomopsidin via the highly stereoselective TADA reaction

Nobuyuki Hayashi, Takahiro Suzuki, Kenji Usui, Masahisa Nakada^*

^*この研究の対応する著者

先進理工学部

研究成果: Article › 査読

16 被引用数 (Scopus)

抄録

This manuscript describes an alternative synthetic approach for (+)-phomopsidin, which shows strong inhibitory activity against the assembly of microtubule proteins. We observed that the TADA reaction of the macrolactone 5 with the reversed C11 configuration provided the desired cycloadduct 6 in 86% yield with excellent stereoselectivity (dr=16:1). Luche reduction of the ketone derived from the major product of the TADA reaction resulted in a 91% yield with excellent stereoselectivity (dr=21:1), and the major product was successfully converted to the known compound in the previously reported total synthesis of (+)-phomopsidin, thereby accomplishing the formal total synthesis of (+)-phomopsidin.

本文言語	English
ページ（範囲）	888-895
ページ数	8
ジャーナル	Tetrahedron
巻	65
号	4
DOI	https://doi.org/10.1016/j.tet.2008.11.030
出版ステータス	Published - 2009 1月 24

ASJC Scopus subject areas

生化学
創薬
有機化学

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10.1016/j.tet.2008.11.030

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abstract = "This manuscript describes an alternative synthetic approach for (+)-phomopsidin, which shows strong inhibitory activity against the assembly of microtubule proteins. We observed that the TADA reaction of the macrolactone 5 with the reversed C11 configuration provided the desired cycloadduct 6 in 86% yield with excellent stereoselectivity (dr=16:1). Luche reduction of the ketone derived from the major product of the TADA reaction resulted in a 91% yield with excellent stereoselectivity (dr=21:1), and the major product was successfully converted to the known compound in the previously reported total synthesis of (+)-phomopsidin, thereby accomplishing the formal total synthesis of (+)-phomopsidin.",

author = "Nobuyuki Hayashi and Takahiro Suzuki and Kenji Usui and Masahisa Nakada",

note = "Funding Information: This work was financially supported in part by a Waseda University Grant for Special Research Projects, a Grant-in-Aid for Scientific Research (B) and the Global COE program {\textquoteleft}Center for Practical Chemical Wisdom{\textquoteright} by MEXT. ",

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AU - Suzuki, Takahiro

AU - Usui, Kenji

AU - Nakada, Masahisa

N1 - Funding Information: This work was financially supported in part by a Waseda University Grant for Special Research Projects, a Grant-in-Aid for Scientific Research (B) and the Global COE program ‘Center for Practical Chemical Wisdom’ by MEXT.

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N2 - This manuscript describes an alternative synthetic approach for (+)-phomopsidin, which shows strong inhibitory activity against the assembly of microtubule proteins. We observed that the TADA reaction of the macrolactone 5 with the reversed C11 configuration provided the desired cycloadduct 6 in 86% yield with excellent stereoselectivity (dr=16:1). Luche reduction of the ketone derived from the major product of the TADA reaction resulted in a 91% yield with excellent stereoselectivity (dr=21:1), and the major product was successfully converted to the known compound in the previously reported total synthesis of (+)-phomopsidin, thereby accomplishing the formal total synthesis of (+)-phomopsidin.

AB - This manuscript describes an alternative synthetic approach for (+)-phomopsidin, which shows strong inhibitory activity against the assembly of microtubule proteins. We observed that the TADA reaction of the macrolactone 5 with the reversed C11 configuration provided the desired cycloadduct 6 in 86% yield with excellent stereoselectivity (dr=16:1). Luche reduction of the ketone derived from the major product of the TADA reaction resulted in a 91% yield with excellent stereoselectivity (dr=21:1), and the major product was successfully converted to the known compound in the previously reported total synthesis of (+)-phomopsidin, thereby accomplishing the formal total synthesis of (+)-phomopsidin.

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Alternative synthetic approach for (+)-phomopsidin via the highly stereoselective TADA reaction

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