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[辐射增敏剂:特别提及乏氧细胞增敏剂]

[Radiation sensitizers: with special reference to hypoxic cell sensitizers].

作者信息

Onoyama Y, Nakajima T, Tanaka M

出版信息

Gan To Kagaku Ryoho. 1986 Apr;13(4 Pt 1):894-903.

PMID:3963856
Abstract

Recent advances in radiation chemistry and radiation biology have led to the combined use of radiosensitizing agents with radiation in the treatment of radioresistant tumors. Various chemicals, including cancerocidal drugs, are used, although radiation sensitizers are defined as drugs which can increase cellular radiosensitivity but have no direct cancerocidal effect. At least four classes of agents, pyrimidine analogues, hypoxic cell sensitizers, PLDR inhibitors and thiol-depleting agents, can modify radiosensitivity and have potential for differential sensitization. Pyrimidine analogues are incorporated into DNA in replicating tumor cells, and can sensitize these cells to radiation up to a factor of 3. Results of clinical trials of intra-arterial infusion of BUdR have not proved satisfactory, especially with regard to long-term survival, possibly because of the existence of non-replicating cells in the tumor. The latter two are still in the experimental stage of study. The radioresistance of hypoxic cells in tumor has been regarded as one of the limiting factors in the local control of cancer by radiation. Attempts to improve the situation involve high-LET radiation and combined use of chemicals, such as oxygen, prefluorochemicals and electron-affinic compounds, with low-LET radiation. Although some clinical trials in head and neck cancer and in cervical cancer have yielded positive results in patients treated using hyperbaric oxygen, attempts have been made to devise other methods, such as those using perfluorochemicals with normobaric oxygen, because of the technical difficulty involved with the former method. A more promising and easier method is the combined use of electron-affinic chemicals, which like oxygen can sensitize the hypoxic cells. Misonidazole (alpha 2-nitroimidazole derivative) was found to be an excellent sensitizer of this kind in cultured mammalian cells and in some rodent tumors. Several randomized clinical trials to determine its efficacy have been carried out on a word-wide scale, but most of them failed to demonstrate any beneficial effect, mainly because of the drug's neurotoxicity which limits its dose. After misonidazole, many researchers have made every effort to develop more efficient hypoxic cell sensitizers. The present state and future prospects of study were reviewed with special reference to studies currently being undertaken in Japan.

摘要

放射化学和放射生物学的最新进展已促使在治疗抗辐射肿瘤时将放射增敏剂与辐射联合使用。尽管放射增敏剂被定义为可增加细胞放射敏感性但无直接抗癌作用的药物,但仍使用了包括抗癌药物在内的各种化学物质。至少四类药物,即嘧啶类似物、乏氧细胞增敏剂、PLDR抑制剂和巯基耗竭剂,可改变放射敏感性并具有差异增敏的潜力。嘧啶类似物在正在复制的肿瘤细胞中掺入DNA,并可使这些细胞对辐射的敏感性提高达3倍。动脉内输注BUdR的临床试验结果并不令人满意,尤其是在长期生存方面,这可能是因为肿瘤中存在非复制细胞。后两类仍处于研究的实验阶段。肿瘤中乏氧细胞的放射抗性被认为是放射局部控制癌症的限制因素之一。改善这种情况的尝试包括高传能线密度辐射以及将化学物质(如氧气、全氟化合物和电子亲和性化合物)与低传能线密度辐射联合使用。尽管一些针对头颈癌和宫颈癌的临床试验在使用高压氧治疗的患者中取得了阳性结果,但由于前一种方法存在技术困难,人们已尝试设计其他方法,如使用全氟化合物与常压氧联合的方法。一种更有前景且更简便的方法是联合使用电子亲和性化学物质,这类物质与氧气一样可使乏氧细胞增敏。米索硝唑(α2-硝基咪唑衍生物)在培养的哺乳动物细胞和一些啮齿动物肿瘤中被发现是这类出色的增敏剂。已在全球范围内进行了多项随机临床试验以确定其疗效,但大多数试验未能证明有任何有益效果,主要是因为该药物的神经毒性限制了其剂量。在米索硝唑之后,许多研究人员全力开发更有效的乏氧细胞增敏剂。特别参考了日本目前正在进行的研究,对研究的现状和未来前景进行了综述。

相似文献

1
[Radiation sensitizers: with special reference to hypoxic cell sensitizers].[辐射增敏剂:特别提及乏氧细胞增敏剂]
Gan To Kagaku Ryoho. 1986 Apr;13(4 Pt 1):894-903.
2
[Present status of radiation sensitizers--hypoxic cell radiosensitizer].辐射增敏剂的现状——乏氧细胞放射增敏剂
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3
Optimization of cancer radiotherapy with selective sensitizers.
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[Present status of hypoxic cell sensitizers and PLDR inhibitors].
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[Radiosensitization research in cancer therapy].[癌症治疗中的放射增敏研究]
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[Clinical trials of hypoxic cell sensitizer misonidazole].[乏氧细胞增敏剂米索硝唑的临床试验]
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Evaluation of hypoxic cell radio-sensitizers in terms of radio-sensitizing and repair-inhibiting potential. Dependency on p53 status of tumor cells and the effects on intratumor quiescent cells.从放射增敏和修复抑制潜力方面评估乏氧细胞放射增敏剂。取决于肿瘤细胞的p53状态以及对肿瘤内静止细胞的影响。
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Bull Cancer. 2008 Mar;95(3):282-91. doi: 10.1684/bdc.2008.0592.