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短暂的抗血管生成治疗可改善肺癌中细胞毒性化合物的递送和治疗效果。

Transient antiangiogenic treatment improves delivery of cytotoxic compounds and therapeutic outcome in lung cancer.

机构信息

Authors' Affiliations: Clinic I of Internal Medicine and Center for Integrated Oncology, University Hospital Cologne; Max Planck Institute for Neurological Research; Center for Molecular Medicine; Max Planck Institute for Biology of Aging; and Institute of Pathology, University Hospital Medical School, Cologne, GermanyAuthors' Affiliations: Clinic I of Internal Medicine and Center for Integrated Oncology, University Hospital Cologne; Max Planck Institute for Neurological Research; Center for Molecular Medicine; Max Planck Institute for Biology of Aging; and Institute of Pathology, University Hospital Medical School, Cologne, GermanyAuthors' Affiliations: Clinic I of Internal Medicine and Center for Integrated Oncology, University Hospital Cologne; Max Planck Institute for Neurological Research; Center for Molecular Medicine; Max Planck Institute for Biology of Aging; and Institute of Pathology, University Hospital Medical School, Cologne, Germany.

Authors' Affiliations: Clinic I of Internal Medicine and Center for Integrated Oncology, University Hospital Cologne; Max Planck Institute for Neurological Research; Center for Molecular Medicine; Max Planck Institute for Biology of Aging; and Institute of Pathology, University Hospital Medical School, Cologne, Germany.

出版信息

Cancer Res. 2014 May 15;74(10):2816-24. doi: 10.1158/0008-5472.CAN-13-2986. Epub 2014 Mar 27.

Abstract

Extensive oncologic experience argues that the most efficacious applications of antiangiogenic agents rely upon a combination with cytotoxic drugs. Yet there remains a lack of clarity about how to optimize scheduling for such drug combinations. Prudent antiangiogenic therapy might transiently normalize blood vessels to improve tumor oxygenation and drug exposure. Using [(15)O]H2O positron emission tomography imaging in a preclinical mouse model of non-small cell lung cancer, we observed that short-term treatment with the vascular endothelial growth factor receptor/platelet-derived growth factor receptor inhibitor PTK787 licensed a transient window of improved tumor blood flow. The improvement observed was associated with a reduced leakiness from tumor vessels, consistent with induction of a vascular normalization process. Initiation of a cytotoxic treatment in this window of tumor vessel normalization resulted in increased efficacy, as illustrated by improved outcomes of erlotinib administration after initial PTK787 treatment. Notably, intermittent PTK787 treatment also facilitated long-term tumor regression. In summary, our findings offer strong evidence that short-term antiangiogenic therapy can promote a transient vessel normalization process that improves the delivery and efficacy of a targeted cytotoxic drug.

摘要

大量肿瘤学经验表明,抗血管生成药物最有效的应用依赖于与细胞毒性药物的联合使用。然而,对于如何优化此类药物组合的方案安排,仍存在着不明确性。审慎的抗血管生成治疗可能会使血管短暂地正常化,从而改善肿瘤的氧合和药物暴露。在非小细胞肺癌的临床前小鼠模型中,我们使用 [(15)O]H2O 正电子发射断层扫描成像技术观察到,短期使用血管内皮生长因子受体/血小板衍生生长因子受体抑制剂 PTK787 可以为改善肿瘤血流提供一个短暂的窗口期。观察到的改善与肿瘤血管渗漏减少有关,这与诱导血管正常化过程一致。在这个肿瘤血管正常化的窗口期开始细胞毒性治疗,会增加疗效,如初始 PTK787 治疗后厄洛替尼给药的结果所示。值得注意的是,间歇性 PTK787 治疗也促进了长期肿瘤消退。总之,我们的研究结果提供了有力的证据表明,短期抗血管生成治疗可以促进短暂的血管正常化过程,从而提高靶向细胞毒性药物的递送和疗效。

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