Synthesis and Biological Evaluation of Quinocarcin Derivatives

Hiromitsu SAITO; Shigeru KOBAYASHI; Youichi UOSAKI; Akira SATO; Kazuhisa FUJIMOTO; Katunori MIYOSHI; Tadashi ASHIZAWA; Makoto MORIMOTO; Tadashi HIRATA

doi:10.1248/cpb.38.1278

斉藤博満, 小林茂, 宇於崎洋一, 佐藤章, 藤本和久, 三好勝則, 芦沢忠, 森本眞, 平田正

著者情報

キーワード: quinocarcin, 10-halo quinocarcin derivative, DX-52-1, 10-substituted DX-52-1 analog, cyanation, electrophilic substitution, antitumor activity

ジャーナルフリー

1990 年 38 巻 5 号 p. 1278-1285

DOI https://doi.org/10.1248/cpb.38.1278

詳細

抄録

Cyanation of quinocarcin readily opened the oxazolidine ring to provide DX-52-1 (2), which was a key compound in the synthesis of quinocarcin derivatives. Various electrophilic reactions toward aromatic ring of DX-52-1 were examined, and 10-substituted (e.g., halogen, nitro, formyl, cyano, hydroxy, etc.) analogs were prepared. Dehydrocyanation of the derivatives could be achieved to reproduce the oxazolidine ring upon treatment with HCl or AgNO₃. 10-Chloride 10 and 10-bromide 11 were the most promising among the derivatives prepared. Antitumor activity of 10 was extended to B-16 melanoma.

責任著者(Corresponding author)

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