Total Synthesis of Calicheamicin γ1I. 3. The Final Stages

K. C. Nicolaou; C. W. Hummel; M. Nakada; K. Shibayama; E. N. Pitsinos; H. Saimoto; Y. Mizuno; K. U. Baldenius; A. L. Smith

doi:10.1021/ja00070a006

Total Synthesis of Calicheamicin γ₁^I. 3. The Final Stages

K. C. Nicolaou, C. W. Hummel, M. Nakada, K. Shibayama, E. N. Pitsinos, H. Saimoto, Y. Mizuno, K. U. Baldenius, A. L. Smith

研究成果: Article › 査読

120 被引用数 (Scopus)

抄録

The first total synthesis of calicheamicin γ₁^I (1) has been achieved. The stereoselective glycosidation, joining the appropriately functionalized aglycon 3 with the oligosaccharide fragment 2, was realized using Schmidt’s trichloroacetimidate methodology. Segment 4, equipped with the photolabile 2-nitrobenzyl group at the reducing end, was synthesized using similar chemistry to that applied to the synthesis of its methyl glycoside counterpart (see accompanying paper). Stereoselective reduction of oxime 31, obtained from the coupling product, with NaCNBH₃ in the presence of BF₃-OEt₂, late in the synthetic scheme, generated the desired alkoxylamine 32 and its A-4 isomer 32-epi. Installment of the allylic trisulfide and appropriate deprotections allowed transformation of 32 and 32-epi to calicheamicin γ₁^I (1) and its A-4 epimer 1-epi, respectively.

本文言語	English
ページ（範囲）	7625-7635
ページ数	11
ジャーナル	Journal of the American Chemical Society
巻	115
号	17
DOI	https://doi.org/10.1021/ja00070a006
出版ステータス	Published - 1993 8 1
外部発表	はい

ASJC Scopus subject areas

Catalysis
Chemistry(all)
Biochemistry
Colloid and Surface Chemistry

文献へのアクセス

10.1021/ja00070a006

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引用スタイル

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abstract = "The first total synthesis of calicheamicin γ1I (1) has been achieved. The stereoselective glycosidation, joining the appropriately functionalized aglycon 3 with the oligosaccharide fragment 2, was realized using Schmidt{\textquoteright}s trichloroacetimidate methodology. Segment 4, equipped with the photolabile 2-nitrobenzyl group at the reducing end, was synthesized using similar chemistry to that applied to the synthesis of its methyl glycoside counterpart (see accompanying paper). Stereoselective reduction of oxime 31, obtained from the coupling product, with NaCNBH3 in the presence of BF3-OEt2, late in the synthetic scheme, generated the desired alkoxylamine 32 and its A-4 isomer 32-epi. Installment of the allylic trisulfide and appropriate deprotections allowed transformation of 32 and 32-epi to calicheamicin γ1I (1) and its A-4 epimer 1-epi, respectively.",

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AU - Hummel, C. W.

AU - Nakada, M.

AU - Shibayama, K.

AU - Pitsinos, E. N.

AU - Saimoto, H.

AU - Mizuno, Y.

AU - Baldenius, K. U.

AU - Smith, A. L.

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