Total Synthesis of Isodaphlongamine H by Iridium-Catalyzed Reductive [3 + 2] Cycloaddition of N-Hydroxylactam

Sora Iwamoto; Reki Nakano; Keiji Sasaki; Shoichiro Kobayashi; Yuki Taira; Koya Takei; Reiji Kawakita; Ayako Tokuyama; Haruto Nakamura; Manato Tomoike; Ryota Kawahara; Akari Murase; Siro Simizu; Noritaka Chida; Toshitaka Okamura; Takaaki Sato

doi:10.1002/anie.202508062

Total Synthesis of Isodaphlongamine H by Iridium-Catalyzed Reductive [3 + 2] Cycloaddition of N-Hydroxylactam

Sora Iwamoto
, Reki Nakano
, Keiji Sasaki
, Shoichiro Kobayashi
, Yuki Taira
, Koya Takei
, Reiji Kawakita
, Ayako Tokuyama
, Haruto Nakamura
, Manato Tomoike
, Ryota Kawahara
, Akari Murase
, Siro Simizu
, Noritaka Chida
, Toshitaka Okamura
, Takaaki Sato

応用化学科

研究成果: Article › 査読

1 被引用数 (Scopus)

抄録

The total synthesis of isodaphlongamine H based on a lactam strategy, which enables quick access to complex cyclic amines, is described. The strategy begins with alkylation of a chiral lactam and subsequent N-oxidation via an imino ether to afford the N-hydroxylactam. For the key transformation to functionalize the amide carbonyl, an iridium-catalyzed reductive [3 + 2] cycloaddition of the N-hydroxylactam provides a tricyclic isoxazolidine in a one-pot process. After the coupling reaction with an allylic silane fragment, the total synthesis is accomplished through intramolecular Hosomi–Sakurai allylation to construct a pentacyclic core. The deoxygenated pentacyclic intermediate shows higher cytotoxicity against HeLa and U937 cell lines than isodaphlongamine H, and might become a lead compound for further biological study.

本文言語	English
論文番号	e202508062
ジャーナル	Angewandte Chemie - International Edition
巻	64
号	29
DOI	https://doi.org/10.1002/anie.202508062
出版ステータス	Published - 2025 7月 14

ASJC Scopus subject areas

触媒
化学一般

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10.1002/anie.202508062

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Iwamoto, S., Nakano, R., Sasaki, K., Kobayashi, S., Taira, Y., Takei, K., Kawakita, R., Tokuyama, A., Nakamura, H., Tomoike, M., Kawahara, R., Murase, A., Simizu, S., Chida, N., Okamura, T., & Sato, T. (2025). Total Synthesis of Isodaphlongamine H by Iridium-Catalyzed Reductive [3 + 2] Cycloaddition of N-Hydroxylactam. Angewandte Chemie - International Edition, 64(29), 記事 e202508062. https://doi.org/10.1002/anie.202508062

Iwamoto, S, Nakano, R, Sasaki, K, Kobayashi, S, Taira, Y, Takei, K, Kawakita, R, Tokuyama, A, Nakamura, H, Tomoike, M, Kawahara, R, Murase, A, Simizu, S, Chida, N, Okamura, T & Sato, T 2025, 'Total Synthesis of Isodaphlongamine H by Iridium-Catalyzed Reductive [3 + 2] Cycloaddition of N-Hydroxylactam', Angewandte Chemie - International Edition, vol. 64, no. 29, e202508062. https://doi.org/10.1002/anie.202508062

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abstract = "The total synthesis of isodaphlongamine H based on a lactam strategy, which enables quick access to complex cyclic amines, is described. The strategy begins with alkylation of a chiral lactam and subsequent N-oxidation via an imino ether to afford the N-hydroxylactam. For the key transformation to functionalize the amide carbonyl, an iridium-catalyzed reductive [3 + 2] cycloaddition of the N-hydroxylactam provides a tricyclic isoxazolidine in a one-pot process. After the coupling reaction with an allylic silane fragment, the total synthesis is accomplished through intramolecular Hosomi–Sakurai allylation to construct a pentacyclic core. The deoxygenated pentacyclic intermediate shows higher cytotoxicity against HeLa and U937 cell lines than isodaphlongamine H, and might become a lead compound for further biological study.",

keywords = "Amide, Daphniphyllum alkaloids, Iridium catalyst, Nitrone, Total synthesis",

author = "Sora Iwamoto and Reki Nakano and Keiji Sasaki and Shoichiro Kobayashi and Yuki Taira and Koya Takei and Reiji Kawakita and Ayako Tokuyama and Haruto Nakamura and Manato Tomoike and Ryota Kawahara and Akari Murase and Siro Simizu and Noritaka Chida and Toshitaka Okamura and Takaaki Sato",

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AU - Iwamoto, Sora

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AU - Sasaki, Keiji

AU - Kobayashi, Shoichiro

AU - Taira, Yuki

AU - Takei, Koya

AU - Kawakita, Reiji

AU - Tokuyama, Ayako

AU - Nakamura, Haruto

AU - Tomoike, Manato

AU - Kawahara, Ryota

AU - Murase, Akari

AU - Simizu, Siro

AU - Chida, Noritaka

AU - Okamura, Toshitaka

AU - Sato, Takaaki

PY - 2025/7/14

Y1 - 2025/7/14

N2 - The total synthesis of isodaphlongamine H based on a lactam strategy, which enables quick access to complex cyclic amines, is described. The strategy begins with alkylation of a chiral lactam and subsequent N-oxidation via an imino ether to afford the N-hydroxylactam. For the key transformation to functionalize the amide carbonyl, an iridium-catalyzed reductive [3 + 2] cycloaddition of the N-hydroxylactam provides a tricyclic isoxazolidine in a one-pot process. After the coupling reaction with an allylic silane fragment, the total synthesis is accomplished through intramolecular Hosomi–Sakurai allylation to construct a pentacyclic core. The deoxygenated pentacyclic intermediate shows higher cytotoxicity against HeLa and U937 cell lines than isodaphlongamine H, and might become a lead compound for further biological study.

AB - The total synthesis of isodaphlongamine H based on a lactam strategy, which enables quick access to complex cyclic amines, is described. The strategy begins with alkylation of a chiral lactam and subsequent N-oxidation via an imino ether to afford the N-hydroxylactam. For the key transformation to functionalize the amide carbonyl, an iridium-catalyzed reductive [3 + 2] cycloaddition of the N-hydroxylactam provides a tricyclic isoxazolidine in a one-pot process. After the coupling reaction with an allylic silane fragment, the total synthesis is accomplished through intramolecular Hosomi–Sakurai allylation to construct a pentacyclic core. The deoxygenated pentacyclic intermediate shows higher cytotoxicity against HeLa and U937 cell lines than isodaphlongamine H, and might become a lead compound for further biological study.

KW - Amide

KW - Daphniphyllum alkaloids

KW - Iridium catalyst

KW - Nitrone

KW - Total synthesis

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Total Synthesis of Isodaphlongamine H by Iridium-Catalyzed Reductive [3 + 2] Cycloaddition of N-Hydroxylactam

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