缺氧诱导因子-1/spl α / (HIF-1/spl α /)和光动力治疗

The Second Asian and Pacific Rim Symposium on Biophotonics, 2004. APBP 2004. Pub Date : 2004-12-15 DOI:10.1109/APBP.2004.1412292

Lin-Hung Wei, C. Chou, J. Su

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引用次数: 0

摘要

只提供摘要形式。光动力疗法(PDT)是一种很有前途的治疗方式，正在临床试验中用于肿瘤治疗。PDT需要三个要素:光、光敏剂和氧气。pdt介导的氧化应激可直接引起暴露肿瘤内的肿瘤细胞损伤和微血管损伤。PDT后的微血管损伤导致血流明显减少以及肿瘤组织严重和持续的缺氧。随后，组织缺氧可以诱导大量的分子和生理反应，包括与基因激活相关的适应性反应。缺氧介导的基因激活的首要步骤是缺氧诱导因子(HIF-1)转录因子复合物的形成。缺氧诱导HIF-1/spl α /的稳定，这反过来又允许转录活性蛋白复合物的形成。迄今为止，能够调节PDT反应的hif -1应答基因尚未得到很好的鉴定。在本研究中，我们采用5-氨基乙酰丙酸作为光敏剂，采用工业技术研究院生产的630 nm波长发光二极管(LED)作为光源。实验结果表明，缺氧状态下癌细胞对PDT的抵抗力更强。PDT可转录诱导或增强HIF-1/spl α /在不同宫颈癌细胞系(SiHa、HeLa、Caski、C33A、HT-3)、不朽宫颈上皮细胞系183a和人脐静脉内皮细胞(HUVECs)中的表达。药理和遗传抑制实验显示，PI3K/Akt信号通路在SiHa细胞中参与PDT对HIF-1/spl α /的激活。当SiHa细胞被反义HIF-1/spl α / (20/spl μ /M)处理时，PDT激活的HIF-1/spl α /蛋白表达明显被抑制，随后SiHa细胞对PDT敏感。目前，制药公司积极开发针对HIF-1/spl α /的新型化合物，作为一种有前景的癌症治疗方法。因此，本研究结果将为提高PDT的治疗效果提供重要信息，具有很大的临床应用潜力。

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Hypoxia-inducible factor-1/spl alpha/ (HIF-1/spl alpha/) and photodynamic therapy

Summary form only given. Photodynamic therapy (PDT) is a promising treatment modality that is being tested in the clinic for use in oncology. PDT requires three elements: light, a photosensitizer and oxygen. PDT-mediated oxidative stress elicits direct tumor cell damage and microvascular injury within exposed tumor. Microvasculature damage following PDT leads to a significant decrease in blood flow as well as severe and persistent tumor tissue hypoxia. Subsequently, tissue hypoxia can induce a plethora of molecular and physiological responses, including an adaptive response associated with gene activation. A primary step in hypoxia-mediated gene activation is the formation of the hypoxia-inducible factor (HIF-1) transcription factor complex. Hypoxia induces the stabilization of the HIF-1/spl alpha/, which in turn allows for the formation of the transcriptionally active protein complex. Up to date, the HIF-1-responsive genes that can modulate the PDT response have not been well identified. In the current study, we employed 5-aminolevulinic acid as a photosensitizer, 630 nm wavelength light-emitting diode (LED) manufactured by the Industrial Technology Research Institute as a light source. The experimental results demonstrated that cancer cells are more resistant to PDT under hypoxic status. PDT can transcriptionally induce or enhance HIF-1/spl alpha/ expression in different cervical cancer cell lines (SiHa, HeLa, Caski, C33A, HT-3), immortalized cervical epithelium cell line 183 A, and human umbilical vein endothelial cells (HUVECs). Pharmacological and genetic inhibition assays revealed that PI3K/Akt signaling critically involves in the activation of HIF-1/spl alpha/ by PDT in SiHa cells. When SiHa cells was treated with antisense HIF-1/spl alpha/ (20/spl mu/M), PDT activated HIF-1/spl alpha/ protein expression was markedly inhibited, and subsequently sensitized SiHa cells to PDT. Currently, pharmaceutical companies actively develop novel compounds targeting HIF-1/spl alpha/ as a promising cancer therapy. The results of this study will, therefore, provide important information to improve the therapeutic efficacy of PDT and have great clinical applicable potential.

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The Second Asian and Pacific Rim Symposium on Biophotonics, 2004. APBP 2004.

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