TX - 1877:作为一种BRM功能型缺氧细胞放射增敏剂的设计、合成及生物学活性
TX-1877: design, synthesis, and biological activities as a BRM-functional hypoxic cell radiosensitizer.
作者信息
Kasai S, Nagasawa H, Kuwasaka H, Oshodani T, Nishioka A, Ogawa Y, Yoshida S, Inayama S, Inomata T, Hori H
机构信息
Department of Biological Science and Technology, Faculty of Engineering, The University of Tokushima, Japan.
出版信息
Int J Radiat Oncol Biol Phys. 1998 Nov 1;42(4):799-802. doi: 10.1016/s0360-3016(98)00328-9.
PURPOSE
2-Nitroimidazole acetamide TX-1877 and its derivatives (TX-1877 analogs) were designed, synthesized, and evaluated by their in vitro and in vivo radiosensitization, tumor growth control, suppression of lung metastasis, and immunopotentiation, as biological response modifier (BRM)-functional hypoxic cell radiosensitizers.
MATERIALS AND METHODS
TX-1877 analogs were designed and synthesized in our laboratory. In vitro radiosensitizing ability was estimated using EMT6/KU cells under hypoxic conditions. In vivo radiosensitization, antimetastasis, and immunopotentiation were evaluated using female C3H/He mice bearing the SCCVII tumor. Days (15 or 10) after the inoculation of 10(5) SCCVII tumor cells into the hinder thigh, a drug (0.4 mg/g) was administered i.p. and local irradiation of 30 Gy was given at 30 min after its administration. Tumor growth was observed for 20 days and mice were euthanized to count the number of metastatic nodules on the surface of the lungs. Tumor tissues were extirpated and stained by the ABC method at 1, 2, and 3 weeks after treatment for immunological evaluation.
RESULTS
Novel types of bifunctional radiosensitizers, TX-1877 and its analogs possessing BRM-functions (i.e., antimetastatic and immunopotentiation effects) were developed. In vitro radiosensitizing abilities of TX-1877 and its analogs, with their partition coefficient values of more than 0.050, were comparable to misonidazole (MISO) at their doses of 1 mM. Tumor regrowth was suppressed evidently 20 days after the treatment in the irradiated group with TX-1877 (TX-1877 plus R) and with KIN-806 (KIN-806 plus R). The former group reduced markedly the mean number of metastatic lung nodules regardless of radiation therapy. TX-1877 and KIN-806 plus R induced helper T lymphocytes. The TX-1877, TX-1877 plus R, KIN-806, and KIN-806 plus R enhanced macrophage infiltration for 3 weeks after treatment.
CONCLUSION
TX-1877 is an excellent BRM-functional hypoxic cell radiosensitizer, expected to be useful for clinical use.
目的
设计、合成了2-硝基咪唑乙酰胺TX-1877及其衍生物(TX-1877类似物),并通过其体外和体内放射增敏作用、肿瘤生长控制、肺转移抑制及免疫增强作用进行评估,作为生物反应调节剂(BRM)功能性缺氧细胞放射增敏剂。
材料与方法
TX-1877类似物在我们实验室设计并合成。在缺氧条件下使用EMT6/KU细胞评估体外放射增敏能力。使用荷SCCVII肿瘤的雌性C3H/He小鼠评估体内放射增敏、抗转移及免疫增强作用。将10⁵个SCCVII肿瘤细胞接种到后肢大腿15或10天后,腹腔注射药物(0.4mg/g),给药后30分钟进行30Gy的局部照射。观察肿瘤生长20天,对小鼠实施安乐死以计数肺表面转移结节的数量。治疗后1、2和3周切除肿瘤组织并用ABC法染色进行免疫学评估。
结果
开发了新型双功能放射增敏剂TX-1877及其具有BRM功能(即抗转移和免疫增强作用)的类似物。TX-1877及其类似物的体外放射增敏能力,其分配系数值大于0.050,在1mM剂量下与米索硝唑(MISO)相当。在接受TX-1877(TX-1877加R)和KIN-806(KIN-806加R)照射的组中,治疗20天后肿瘤再生长明显受到抑制。前一组无论是否进行放射治疗,均显著减少了肺转移结节的平均数量。TX-1877和KIN-806加R诱导辅助性T淋巴细胞。TX-1877、TX-1877加R、KIN-806和KIN-806加R在治疗后3周增强巨噬细胞浸润。
结论
TX-1877是一种优秀的BRM功能性缺氧细胞放射增敏剂,有望用于临床。
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