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Platelet activating factor receptor antagonists improve the efficacy of experimental chemo- and radiotherapy

机译:血小板活化因子受体拮抗剂可提高实验性化学疗法和放射疗法的功效

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摘要

Platelet activating factor is a lipid mediator of inflammation, and in recent decades, it has emerged as an important factor in tumor outcomes. Platelet activating factor acts by specific binding to its receptor, which is present in both tumor cells and cells that infiltrate tumors. Pro-tumorigenic effects of platelet activating factor receptor in tumors includes promotion of tumor cell proliferation, production of survival signals, migration of vascular cells and formation of new vessels and stimulation of dendritic cells and macrophages suppressor phenotype. In experimental models, blocking of platelet activating factor receptor reduced tumor growth and increased animal survival. During chemotherapy and radiotherapy, tumor cells that survive treatment undergo accelerated proliferation, a phenomenon known as tumor cell repopulation. Work from our group and others showed that these treatments induce overproduction of platelet activating factor-like molecules and increase expression of its receptor in tumor cells. In this scenario, antagonists of platelet activating factor markedly reduced tumor repopulation. Here, we note that combining chemo- and radiotherapy with platelet activating factor antagonists could be a promising strategy for cancer treatment.
机译:血小板活化因子是炎症的脂质介质,在最近的几十年中,它已成为影响肿瘤预后的重要因素。血小板活化因子通过与其受体的特异性结合而起作用,该受体存在于肿瘤细胞和浸润肿瘤的细胞中。血小板活化因子受体在肿瘤中的促肿瘤作用包括促进肿瘤细胞增殖,产生存活信号,血管细胞迁移和新血管形成以及刺激树突状细胞和巨噬细胞抑制剂表型。在实验模型中,血小板活化因子受体的阻断降低了肿瘤的生长并增加了动物的存活率。在化学疗法和放射疗法期间,幸存下来的肿瘤细胞会加速增殖,这种现象被称为肿瘤细胞重新聚集。我们小组和其他小组的工作表明,这些治疗方法会诱导血小板活化因子样分子的过度生产,并增加其在肿瘤细胞中的受体表达。在这种情况下,血小板活化因子的拮抗剂显着减少了肿瘤的重新聚集。在这里,我们注意到将化学疗法和放射疗法与血小板活化因子拮抗剂结合起来可能是一种有前途的癌症治疗策略。

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