一类新型抗肿瘤前药,1-(2'-氧代丙基)-5-氟尿嘧啶(OFU001),在缺氧照射时释放5-氟尿嘧啶。
A novel class of antitumor prodrug, 1-(2'-oxopropyl)-5-fluorouracil (OFU001), that releases 5-fluorouracil upon hypoxic irradiation.
作者信息
Shibamoto Y, Zhou L, Hatta H, Mori M, Nishimoto S
机构信息
Department of Oncology, Institute for Frontier Medical Sciences, Kyoto University, Kyoto 606-8507, Japan.
出版信息
Jpn J Cancer Res. 2000 Apr;91(4):433-8. doi: 10.1111/j.1349-7006.2000.tb00963.x.
We have been developing prodrugs of anticancer agents such as 5-fluorouracil (5-FU) that are activated by irradiation under hypoxic conditions via one-electron reduction. Among them, OFU001 [1-(2'-oxopropyl)-5-fluorouracil] is a prototype radiation-activated prodrug. In this study, we investigated the radiation chemical reactivity and the biological effects of OFU001. This prodrug is presumed to release 5-FU through incorporation of hydrated electrons into the antibonding sigma * orbital of the C(1')-N(1) bond. Hydrated electrons are active species derived from radiolysis of water, but are readily deactivated by O(2) into superoxide anion radicals (O(2).(-)) under conditions of aerobic irradiation. Therefore, 5-FU release occurs highly specifically upon irradiation under hypoxic conditions. OFU001 dissolved in phosphate buffer released 5-FU with a G-value (mol number of molecules that are decomposed or produced by 1 J of absorbed radiation energy) of 1.9 x 10(-7) mol / J following hypoxic irradiation, while the G-value for 5-FU release was 1.0 x 10(-8) mol/J following aerobic irradiation. However, the G-values for decomposition of OFU001 were almost the same, i.e., 3.4 x 10(-7) mol/J following hypoxic irradiation and 2. 5 x 10(-7) mol / J following aerobic irradiation. When hypoxically irradiated (7.5 - 30 Gy) OFU001 was added to murine SCCVII cells for 1 - 24 h, a significant cell-killing effect was observed. The degree of this cytotoxicity was consistent with that of authentic 5-FU at the corresponding concentrations. On the other hand, cytotoxicity was minimal when the cells were treated with aerobically irradiated or unirradiated OFU001. This compound had no radiosensitizing effect against SCCVII cells under either aerobic or hypoxic conditions when the drug was removed immediately after irradiation. Since hypoxia is generally most marked in tumors and irradiation is applied at the tumor site, this concept of prodrug design appears to be potentially useful for selective tumor treatment with minimal adverse effects of anticancer agents.
我们一直在研发抗癌药物的前体药物,比如5-氟尿嘧啶(5-FU),其可在缺氧条件下通过单电子还原经辐射激活。其中,OFU001 [1-(2'-氧代丙基)-5-氟尿嘧啶] 是一种辐射激活前体药物的原型。在本研究中,我们研究了OFU001的辐射化学反应性和生物学效应。据推测,这种前体药物通过水合电子并入C(1')-N(1)键的反键σ*轨道来释放5-FU。水合电子是水辐射分解产生的活性物质,但在有氧辐射条件下很容易被O(2)失活转化为超氧阴离子自由基(O(2).(-))。因此,5-FU的释放在缺氧条件下辐射时具有高度特异性。缺氧辐射后,溶解在磷酸盐缓冲液中的OFU001释放5-FU的G值(每1焦耳吸收辐射能量分解或产生的分子摩尔数)为1.9×10(-7) mol / J,而有氧辐射后5-FU释放的G值为1.0×10(-8) mol/J。然而,OFU001分解的G值几乎相同,即缺氧辐射后为3.4×10(-7) mol/J,有氧辐射后为2.5×10(-7) mol / J。当将缺氧辐射(7.5 - 30 Gy)的OFU001添加到小鼠SCCVII细胞中1 - 24小时时,观察到显著的细胞杀伤作用。这种细胞毒性的程度与相应浓度的纯5-FU一致。另一方面,当细胞用有氧辐射或未辐射的OFU001处理时,细胞毒性最小。当辐射后立即去除药物时,该化合物在有氧或缺氧条件下对SCCVII细胞均无放射增敏作用。由于缺氧在肿瘤中通常最为明显,且辐射应用于肿瘤部位,这种前体药物设计理念似乎对于以最小的抗癌药物副作用进行选择性肿瘤治疗具有潜在的用途。
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