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通过抗血管生成疗法绕过肿瘤耐药性。

Bypass of tumor drug resistance by antivascular therapy.

作者信息

Preise Dina, Mazor Ohad, Koudinova Natalia, Liscovitch Mordechai, Scherz Avigdor, Salomon Yoram

机构信息

Department of Biological Regulation, The Weizmann Institute of Science, Rehovot, Israel.

出版信息

Neoplasia. 2003 Nov-Dec;5(6):475-80. doi: 10.1016/s1476-5586(03)80031-3.

Abstract

Multidrug resistance (MDR) presents a major obstacle for the successful chemotherapy of cancer. Its emergence during chemotherapy is attributed to a selective process, which gives a growth advantage to MDR cells within the genetically unstable neoplastic cell population. The pleiotropic nature of clinical MDR poses a great difficulty for the development of treatment strategies that aim at blocking MDR at the tumor cell level. Targeting treatment to the nonmalignant vascular network-the lifeline of the tumor-is a promising alternative for the treatment of drug-resistant tumors. The present study demonstrates that MDR in cancer can be successfully circumvented by photodynamic therapy (PDT) using an antivascular treatment protocol. We show that, although P-glycoprotein-expressing human HT29/MDR colon carcinoma cells in culture are resistant to PDT with Pd-bacteriopheophorbide (TOOKAD), the same treatment induces tumor necrosis with equal efficacy (88% vs 82%) in HT29/MDR-derived xenografts and their wild type counterparts, respectively. These results are ascribed to the rapid antivascular effects of the treatment, supporting the hypothesis that MDR tumors can be successfully eradicated by indirect approaches that bypass their inherent drug resistance. We suggest that with progress in ongoing clinical trials, TOOKAD-PDT may offer a novel option for local treatment of MDR tumors.

摘要

多药耐药(MDR)是癌症化疗成功的主要障碍。化疗期间MDR的出现归因于一个选择过程,该过程使基因不稳定的肿瘤细胞群体中的MDR细胞具有生长优势。临床MDR的多效性给旨在在肿瘤细胞水平阻断MDR的治疗策略的开发带来了很大困难。将治疗靶向非恶性血管网络——肿瘤的生命线——是治疗耐药肿瘤的一种有前景的替代方法。本研究表明,使用抗血管治疗方案的光动力疗法(PDT)可以成功规避癌症中的MDR。我们表明,尽管培养的表达P-糖蛋白的人HT29/MDR结肠癌细胞对用钯细菌叶绿素(TOOKAD)进行的PDT有抗性,但相同的治疗分别在HT29/MDR衍生的异种移植瘤及其野生型对应物中诱导肿瘤坏死,疗效相同(88%对82%)。这些结果归因于该治疗的快速抗血管作用,支持了通过绕过其固有耐药性的间接方法可以成功根除MDR肿瘤的假设。我们建议,随着正在进行的临床试验取得进展,TOOKAD-PDT可能为MDR肿瘤的局部治疗提供一种新选择。

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Bypass of tumor drug resistance by antivascular therapy.通过抗血管生成疗法绕过肿瘤耐药性。
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