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硝基咪唑类药物作为实体瘤缺氧调节剂的临床评价

Clinical evaluation of nitroimidazoles as modifiers of hypoxia in solid tumors.

作者信息

Overgaard J

机构信息

Danish Cancer Society, Department of Experimental Clinical Oncology, Radiumstationen, Aarhus.

出版信息

Oncol Res. 1994;6(10-11):509-18.

PMID:7620219
Abstract

Hypoxic modification by nitroimidazoles has been explored in a large number of clinical studies. Nine different drugs (misonidazole, metronidazole, benznidazole, desmethylmisonidazole, etanidazole, pimonidazole, nimorazole, ornidazole, and RSU 1069) have reached clinical evaluation. Phase I and II trials have demonstrated a relationship between drug tolerance and expected hypoxic modification. Thus, the most tolerable drugs, viz., 5-nitroimidazoles, are those with the smallest preclinical activity. However, they may be the most clinically active, due to higher plasma and tumor concentrations. The clinical evaluation of hypoxic modification is difficult, since clinically important hypoxia can be observed only indirectly. There is, however, indirect evidence of substantial hypoxia in human tumors, although with considerable heterogeneity among individual tumors. More than 7000 patients have been included in 50 randomized trials. A meta-analysis showed that modification of tumor hypoxia significantly improved the loco-regional tumor control after radiotherapy with an odds ratio of 1.17 (95% confidence limits 1.06 to 1.28). The treatment benefit could mostly be related to an improved response in head and neck with odds ratio 1.23 (95% confidence limits 1.09 to 1.37), and to a lesser extent in bladder tumors; no significant effect was observed in other tumor sites (cervix, lung, central nervous system, and esophagus). Similarly to the local control benefit, the overall survival rate was improved with an overall odds ratio of 1.13 (95% confidence limits 1.03 to 1.23). The clinical trials showed no evidence of significant chemosensitization or direct bioreductive effect. Although 50 randomized clinical trials were evaluated, the median number of patients was only 97 (range 17-620). Clinical trials of this size are not likely to detect the observed differences, which may explain the lack of significant improvement in most of the individual studies. However, the overall results indicate that the biological issue related to hypoxia appears to be a sound rationale, especially with regard to head and neck and bladder carcinoma. Future studies related to the hypoxic problem should therefore preferably be aimed towards such tumors.

摘要

大量临床研究探索了硝基咪唑类药物的低氧修饰作用。九种不同药物(米索硝唑、甲硝唑、苄硝唑、去甲基米索硝唑、依他硝唑、匹莫硝唑、尼莫唑、奥硝唑和RSU 1069)已进入临床评估阶段。I期和II期试验表明了药物耐受性与预期低氧修饰之间的关系。因此,最耐受的药物,即5-硝基咪唑类,是临床前活性最小的药物。然而,由于血浆和肿瘤浓度较高,它们可能是临床上活性最高的药物。低氧修饰的临床评估很困难,因为临床上重要的低氧只能间接观察到。然而,有间接证据表明人类肿瘤中存在大量低氧,尽管个体肿瘤之间存在相当大的异质性。50项随机试验纳入了7000多名患者。一项荟萃分析表明,肿瘤低氧修饰显著改善了放疗后的局部区域肿瘤控制,优势比为1.17(95%置信区间为1.06至1.28)。治疗益处主要与头颈部反应改善有关,优势比为1.23(95%置信区间为1.09至1.37),在膀胱肿瘤中程度较小;在其他肿瘤部位(子宫颈、肺、中枢神经系统和食管)未观察到显著效果。与局部控制益处类似,总生存率也有所提高,总体优势比为1.13(95%置信区间为1.03至1.23)。临床试验未显示出显著的化学增敏或直接生物还原作用的证据。尽管评估了50项随机临床试验,但患者中位数仅为97例(范围为17 - 620例)。这种规模的临床试验不太可能检测到观察到的差异,这可能解释了大多数个体研究中缺乏显著改善的原因。然而,总体结果表明,与低氧相关的生物学问题似乎是一个合理的理论基础,特别是对于头颈部和膀胱癌而言。因此,未来与低氧问题相关的研究最好针对此类肿瘤。

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