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血管靶向光动力疗法的全身抗肿瘤保护涉及细胞免疫和体液免疫。

Systemic antitumor protection by vascular-targeted photodynamic therapy involves cellular and humoral immunity.

作者信息

Preise Dina, Oren Roni, Glinert Itai, Kalchenko Vyacheslav, Jung Steffen, Scherz Avigdor, Salomon Yoram

机构信息

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

出版信息

Cancer Immunol Immunother. 2009 Jan;58(1):71-84. doi: 10.1007/s00262-008-0527-0. Epub 2008 May 17.

Abstract

Vascular-targeted photodynamic therapy (VTP) takes advantage of intravascular excitation of a photosensitizer (PS) to produce cytotoxic reactive oxygen species (ROS). These ROS are potent mediators of vascular damage inducing rapid local thrombus formation, vascular occlusion, and tissue hypoxia. This light-controlled process is used for the eradication of solid tumors with Pd-bacteriochlorophyll derivatives (Bchl) as PS. Unlike classical photodynamic therapy (PDT), cancer cells are not the primary target for VTP but instead are destroyed by treatment-induced oxygen deprivation. VTP initiates acute local inflammation inside the illuminated area accompanied by massive tumor tissue death. Consequently, in the present study, we addressed the possibility of immune response induction by the treatment that may be considered as an integral part of the mechanism of VTP-mediated tumor eradication. The effect of VTP on the host immune system was investigated using WST11, which is now in phase II clinical trials for age-related macular degeneration and intended to be evaluated for cancer therapy. We found that a functional immune system is essential for successful VTP. Long-lasting systemic antitumor immunity was induced by VTP involving both cellular and humoral components. The antitumor effect was cross-protective against mismatched tumors, suggesting VTP-mediated production of overlapping tumor antigens, possibly from endothelial origin. Based on our findings we suggest that local VTP might be utilized in combination with other anticancer therapies (e.g., immunotherapy) for the enhancement of host antitumor immunity in the treatment of both local and disseminated disease.

摘要

血管靶向光动力疗法(VTP)利用血管内光敏剂(PS)的激发来产生细胞毒性活性氧(ROS)。这些ROS是血管损伤的有效介质,可诱导局部快速血栓形成、血管闭塞和组织缺氧。这种光控过程用于使用钯细菌叶绿素衍生物(Bchl)作为PS来根除实体瘤。与经典光动力疗法(PDT)不同,癌细胞不是VTP的主要靶点,而是被治疗诱导的缺氧所破坏。VTP在光照区域内引发急性局部炎症,并伴有大量肿瘤组织死亡。因此,在本研究中,我们探讨了该治疗诱导免疫反应的可能性,这可能被视为VTP介导的肿瘤根除机制的一个组成部分。使用WST11研究了VTP对宿主免疫系统的影响,WST11目前正处于年龄相关性黄斑变性的II期临床试验中,并打算用于癌症治疗评估。我们发现功能性免疫系统对于成功的VTP至关重要。VTP诱导了持久的全身抗肿瘤免疫,涉及细胞和体液成分。抗肿瘤作用对不匹配的肿瘤具有交叉保护作用,表明VTP介导了重叠肿瘤抗原的产生,可能来源于内皮细胞。基于我们的研究结果,我们建议局部VTP可与其他抗癌疗法(如免疫疗法)联合使用,以增强宿主抗肿瘤免疫力,用于治疗局部和播散性疾病。

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