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作为血红蛋白修饰剂和肿瘤放射增敏剂的氯苯氧基乙酸衍生物

Chlorophenoxy acetic acid derivatives as hemoglobin modifiers and tumor radiosensitizers.

作者信息

Hirst D G, Wood P J

机构信息

Department of Radiation Oncology, Stanford University School of Medicine, CA 94305.

出版信息

Int J Radiat Oncol Biol Phys. 1989 May;16(5):1183-6. doi: 10.1016/0360-3016(89)90279-4.

Abstract

We have studied the influence of the antilipidemia drug, clofibrate, and several structurally related analogs on the binding affinity of hemoglobin for oxygen and the radiation sensitivity of the SCCVII/St carcinoma in the mouse. Several compounds in this class reduced hemoglobin affinity in vivo; and two of these, ML1024 (etophyline clofibrate) and ML1037, were at least as effective as clofibrate at reducing hemoglobin affinity and much less toxic. When given orally at a dose of 4.1 m mole/Kg, 1/2-2 hrs before 20 Gy X rays, clofibrate gave radiosensitization in the SCCVII/St tumor equivalent to a 40-fold reduction in hypoxic fraction. ML1024 and ML1037 at a dose (3.0 m mole/Kg), which had a similar effect on hemoglobin, gave much less sensitization of the tumor. Only ML1024 produced a statistically significant effect, equivalent to a four-fold reduction in hypoxic fraction. We conclude that there are several clofibrate analogs which in relation to their toxicity are much better hemoglobin modifiers than the parent compound. They do not, however, show the same radiosensitizing effects, leading us to believe that mechanisms other than changes in hemoglobin/oxygen binding must also be involved.

摘要

我们研究了抗血脂药物氯贝丁酯以及几种结构相关类似物对小鼠血红蛋白与氧结合亲和力和SCCVII/St癌辐射敏感性的影响。该类中的几种化合物在体内降低了血红蛋白亲和力;其中两种,ML1024(氯贝茶碱)和ML1037,在降低血红蛋白亲和力方面至少与氯贝丁酯一样有效,且毒性小得多。在20 Gy X射线照射前1/2 - 2小时以4.1毫摩尔/千克的剂量口服时,氯贝丁酯使SCCVII/St肿瘤产生的放射增敏作用相当于缺氧分数降低40倍。ML1024和ML1037以对血红蛋白有类似作用的剂量(3.0毫摩尔/千克)给药时,肿瘤的增敏作用小得多。只有ML1024产生了统计学上显著的效果,相当于缺氧分数降低四倍。我们得出结论,有几种氯贝丁酯类似物,就其毒性而言,是比母体化合物更好的血红蛋白调节剂。然而,它们并未表现出相同的放射增敏作用,这使我们相信除了血红蛋白/氧结合的变化之外,一定还涉及其他机制。

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