Syntheses of naturally occurring cytotoxic [7.7]paracyclophanes, (-)-cylindrocyclophane A and its enantiomer, and implications for biological activity

Hiroyuki Yamakoshi; Fumiya Ikarashi; Masataka Minami; Masatoshi Shibuya; Tsutomu Sugahara; Naoki Kanoh; Hisatsugu Ohori; Hiroyuki Shibata; Yoshiharu Iwabuchi

doi:10.1039/b909646a

Syntheses of naturally occurring cytotoxic [7.7]paracyclophanes, (-)-cylindrocyclophane A and its enantiomer, and implications for biological activity

Hiroyuki Yamakoshi, Fumiya Ikarashi, Masataka Minami, Masatoshi Shibuya, Tsutomu Sugahara, Naoki Kanoh, Hisatsugu Ohori, Hiroyuki Shibata, Yoshiharu Iwabuchi

Tohoku University

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

24 Citations (Scopus)

Abstract

The total syntheses of (-)-cylindrocyclophane A (1), a naturally occurring, cytotoxic [7.7]paracyclophane, and its enantiomer have been achieved in an enantiodivergent manner starting from a chiral propargyl alcohol building block using Smith's cross metathesis/ring-closing metathesis protocol as the key step. The biological evaluation of both enantiomers of cylindrocyclophane A (1 and ent-1) and its analogues indicated that the chirality of 1 is irrelevant to its cytotoxicity, which is attributed to the resorcinol motifs embedded in the robust [7.7]paracyclophane framework.

Original language	English
Pages (from-to)	3772-3781
Number of pages	10
Journal	Organic and Biomolecular Chemistry
Volume	7
Issue number	18
DOIs	https://doi.org/10.1039/b909646a
Publication status	Published - 2009

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abstract = "The total syntheses of (-)-cylindrocyclophane A (1), a naturally occurring, cytotoxic [7.7]paracyclophane, and its enantiomer have been achieved in an enantiodivergent manner starting from a chiral propargyl alcohol building block using Smith's cross metathesis/ring-closing metathesis protocol as the key step. The biological evaluation of both enantiomers of cylindrocyclophane A (1 and ent-1) and its analogues indicated that the chirality of 1 is irrelevant to its cytotoxicity, which is attributed to the resorcinol motifs embedded in the robust [7.7]paracyclophane framework.",

author = "Hiroyuki Yamakoshi and Fumiya Ikarashi and Masataka Minami and Masatoshi Shibuya and Tsutomu Sugahara and Naoki Kanoh and Hisatsugu Ohori and Hiroyuki Shibata and Yoshiharu Iwabuchi",

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AU - Yamakoshi, Hiroyuki

AU - Ikarashi, Fumiya

AU - Minami, Masataka

AU - Shibuya, Masatoshi

AU - Sugahara, Tsutomu

AU - Kanoh, Naoki

AU - Ohori, Hisatsugu

AU - Shibata, Hiroyuki

AU - Iwabuchi, Yoshiharu

PY - 2009

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AB - The total syntheses of (-)-cylindrocyclophane A (1), a naturally occurring, cytotoxic [7.7]paracyclophane, and its enantiomer have been achieved in an enantiodivergent manner starting from a chiral propargyl alcohol building block using Smith's cross metathesis/ring-closing metathesis protocol as the key step. The biological evaluation of both enantiomers of cylindrocyclophane A (1 and ent-1) and its analogues indicated that the chirality of 1 is irrelevant to its cytotoxicity, which is attributed to the resorcinol motifs embedded in the robust [7.7]paracyclophane framework.

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Syntheses of naturally occurring cytotoxic [7.7]paracyclophanes, (-)-cylindrocyclophane A and its enantiomer, and implications for biological activity

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