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化疗免疫调节:抗肿瘤化学治疗药物的免疫调节作用。

ChemoImmunoModulation: immune regulation by the antineoplastic chemotherapeutic agents.

机构信息

Department of Pathology, University of Pittsburgh Medical Center, Pittsburgh, PA 15261, USA.

出版信息

Curr Med Chem. 2012;19(12):1792-803. doi: 10.2174/092986712800099785.

Abstract

Since 1948, when Farber et al. introduced aminopterin, the first chemotherapeutic agent, more than 100 such agents have come into use. Initially, antitumor chemotherapies were thought to produce only antiproliferative or cytotoxic effects on dividing tumor cells as it was often associated with the damage to healthy tissues and the development of resistant tumor clones. However, that view has been changing as a consequence of recent demonstrations that several antineoplastic drugs, even at low doses, have antiangiogenic and sometimes immunomodulating effects. In addition, new studies indicate that lowering the dose of conventional cytotoxic agents and combining chemotherapy with other modalities may not only decrease the toxicity of conventional chemotherapy, but also up-regulate the efficacy of different anticancer therapies. Giving chemotherapy in this manner has several potential advantages, including impediment of the onset of mutation-dependent mechanisms of acquired drug resistance and increase in the efficacy and durability of combinatorial therapeutic modalities. Certain "immunogenic" forms of cancer chemotherapy may cause indirect activation of immune cells due to the accessibility of tumor antigens and certain "danger" signals. Furthermore, new findings indicate that several chemotherapeutic agents can directly activate immune cells when used in ultra low noncytotoxic concentrations, the new phenomenon that was termed chemoimmunomodulation. The goal of this review is to analyze the immune modulating properties of antineoplastic chemotherapeutic agents and present new evidence of the immunostimulating potentials of several agents used in low and ultra low nontoxic doses. Therapeutic potentials of combined chemo-immunotherapeutic regimens have been extensively reviewed in a variety of recent publications and will not be discussed.

摘要

自 1948 年法伯等人引入第一个化疗药物氨蝶呤以来,已有 100 多种此类药物投入使用。最初,抗肿瘤化疗被认为仅对分裂的肿瘤细胞产生抗增殖或细胞毒性作用,因为它常常与对健康组织的损害和耐药肿瘤克隆的发展有关。然而,这种观点随着最近的一些研究结果而发生了变化,这些研究表明,即使是低剂量的几种抗肿瘤药物也具有抗血管生成作用,有时还具有免疫调节作用。此外,新的研究表明,降低常规细胞毒性药物的剂量并将化疗与其他方法相结合,不仅可以降低常规化疗的毒性,还可以提高不同抗癌疗法的疗效。以这种方式给予化疗有几个潜在的优点,包括阻止获得性耐药机制中突变的发生以及提高组合治疗方式的疗效和持久性。某些“免疫原性”形式的癌症化疗可能会由于肿瘤抗原的可及性和某些“危险”信号而间接激活免疫细胞。此外,新的发现表明,当以超低非细胞毒性浓度使用时,几种化疗药物可以直接激活免疫细胞,这一现象被称为化疗免疫调节。本综述的目的是分析抗肿瘤化疗药物的免疫调节特性,并提出新的证据,证明低剂量和超低剂量使用的几种药物具有免疫刺激潜力。联合化疗免疫治疗方案的治疗潜力已在各种最近的出版物中进行了广泛的综述,这里不再讨论。

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