亚叶酸钙和α-2a干扰素联合调节氟嘧啶介导的生长抑制作用。
Combined modulation by leucovorin and alpha-2a interferon of fluoropyrimidine mediated growth inhibition.
作者信息
Sinnige H A, Timmer-Bosscha H, Peters G F, De Vries E G, Mulder N H
机构信息
Department of Medical Oncology, University Hospital Groningen, The Netherlands.
出版信息
Anticancer Res. 1993 Sep-Oct;13(5A):1335-40.
UNLABELLED
One way to improve fluoropyrimidine activity is the use of leucovorin (LV). Another way is the use of alpha-2a interferon (alpha-IF). The mechanism of the alpha-IF effect on fluoropyrimidines has not yet been elucidated. Besides, only limited data area available on double modulation (LV and alpha-IF) of fluoropyrimidines. Therefore, the modulating capacity of both drugs was tested in a fluoropyrimidine resistant (COLO 320) and a sensitive (SW 948) cell line. Also, the binding capacity of thymidylate synthase (TS) to 5-fluoro-2'-deoxyuridine-5'-monophosphate (FdUMP) and TS catalytic activity were studied in both cell lines as well as the effects of 5-fluorouracil (5-FU) and alpha IF on enzyme activity. COLO 320 had, compared to SW 948, a 7.5 fold higher FdUMP binding capacity to TS. TS activity was 4.4 and 11.3 fold higher at 10 and 1 mM substrate, respectively. In COLO 320 enhancement of 5-FU, either by LV or by alpha-IF, was not possible. Since LV did enhance 5-fluoro-2' deoxyuridine (FUdR) activity, it is conceivable that 5-FU mediated growth inhibition in COLO 320 is not TS mediated. SW 948 was sensitive to both modulating agents with a 2.4 fold lower IC50 for 5-FU/LV, 6.8 fold lower IC50 for 5-FU/alpha-IF and a 11.2 fold lower IC50 for 5-FU/LV/alpha-IF. Effects of LV and alpha-IF on FUdR were comparable but less pronounced, with a 3.4 fold lower IC50 for FUdR/LV/alpha-IF compared with FUdR alone. Thymidine, which circumvents TS inhibition, neutralized the synergistic effects of alpha-IF, indicating that alpha-IF enhancement is mediated via inhibition of DNA synthesis. However, no direct effects of alpha-IF on FdUMP binding or catalytic activity could be demonstrated.
IN CONCLUSION
alpha-IF can increase 5-FU/LV mediated growth inhibition in fluoropyrimidine sensitive colorectal cancer cells. FdUMP binding capacity and catalytic activity of TS may predict sensitivity to (modulation of) fluoropyrimidines.
未标记
提高氟嘧啶活性的一种方法是使用亚叶酸(LV)。另一种方法是使用α-2a干扰素(α-IF)。α-IF对氟嘧啶作用的机制尚未阐明。此外,关于氟嘧啶的双重调节(LV和α-IF)仅有有限的数据。因此,在氟嘧啶耐药(COLO 320)和敏感(SW 948)细胞系中测试了这两种药物的调节能力。同时,在这两种细胞系中研究了胸苷酸合成酶(TS)与5-氟-2'-脱氧尿苷-5'-单磷酸(FdUMP)的结合能力、TS催化活性以及5-氟尿嘧啶(5-FU)和α-IF对酶活性的影响。与SW 948相比,COLO 320中FdUMP与TS的结合能力高7.5倍。在底物浓度为10和1 mM时,TS活性分别高4.4倍和11.3倍。在COLO 320中,无论是LV还是α-IF都无法增强5-FU的作用。由于LV确实增强了5-氟-2'-脱氧尿苷(FUdR)的活性,可以推测COLO 320中5-FU介导的生长抑制不是由TS介导的。SW 948对两种调节药物均敏感,5-FU/LV的IC50低2.4倍,5-FU/α-IF的IC50低6.8倍,5-FU/LV/α-IF的IC50低11.2倍。LV和α-IF对FUdR的作用相当但不太明显,与单独的FUdR相比,FUdR/LV/α-IF的IC50低3.4倍。胸苷可规避TS抑制,中和了α-IF的协同作用,表明α-IF的增强作用是通过抑制DNA合成介导的。然而,未证实α-IF对FdUMP结合或催化活性有直接影响。
结论
α-IF可增强氟嘧啶敏感的结直肠癌细胞中5-FU/LV介导的生长抑制。TS的FdUMP结合能力和催化活性可预测对氟嘧啶(调节)的敏感性。
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