摘要
Tumor hypoxia has been widely explored over the years as a diagnostic and therapeutic marker. Herein, we designed, optimized and synthesized a new multifunctional bioreductive linker (12) containing an alkynyl group (potential click chemistry fragment); the linker is based on 2-nitroimidazole which was expected to simultaneously overcome the drawbacks of hypoxia-activated prodrugs (poor selectivity and unsatisfactory water solubility). Furthermore, a hypoxia-activated, water-soluble SN-38 prodrug was obtained, and it was stable under physiological conditions and was rapidly released as an active drug under hypoxic conditions.
| 源语言 | 英语 |
|---|---|
| 文章编号 | 103975 |
| 期刊 | Bioorganic Chemistry |
| 卷 | 101 |
| DOI | |
| 出版状态 | 已出版 - 8月 2020 |
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