Heme oxygenase-1 protects tumor cells against photodynamic therapy-mediated cytotoxicity

被引:166
作者
Nowis, D.
Legat, M.
Grzela, T.
Niderla, J.
Wilczek, E.
Wilczynski, G. M.
Glodkowska, E.
Mrowka, P.
Issat, T.
Dulak, J.
Jozkowicz, A.
Was, H.
Adamek, M.
Wrzosek, A.
Nazarewski, S.
Makowski, M.
Stoklosa, T.
Jakobisiak, M.
Golab, J.
机构
[1] Warsaw Univ, Ctr Biostruct Res, Dept Immunol, PL-02097 Warsaw, Poland
[2] Warsaw Univ, Ctr Biostruct Res, Dept Histol & Embryol, PL-02097 Warsaw, Poland
[3] Warsaw Univ, Ctr Biostruct Res, Dept Pathol, PL-02097 Warsaw, Poland
[4] Warsaw Univ, Dept Gen & Vasc Surg & Transplantat, PL-02097 Warsaw, Poland
[5] Jagiellonian Univ, Fac Biotechnol, Dept Med Biotechnol, Krakow, Poland
[6] Silesian Univ, Ctr Laser Diagnost & Therapy, Chair & Clin Internal Dis & Phys Med, Bytom, Poland
[7] M Nencki Inst Expt Biol, Dept Muscle Biochem, PL-02093 Warsaw, Poland
关键词
photodynamic therapy; Photofrin; heme oxygenase; cancer;
D O I
10.1038/sj.onc.1209378
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Photodynamic therapy is a promising antitumor treatment modality approved for the management of both early and advanced tumors. The mechanisms of its antitumor action include generation of singlet oxygen and reactive oxygen species that directly damage tumor cells and tumor vasculature. A number of mechanisms seem to be involved in the protective responses to PDT that include activation of transcription factors, heat shock proteins, antioxidant enzymes and antiapoptotic pathways. Elucidation of these mechanisms might result in the design of more effective combination strategies to improve the antitumor efficacy of PDT. Using DNA microarray analysis to identify stress-related genes induced by Photofrin-mediated PDT in colon adenocarcinoma C-26 cells, we observed a marked induction of heme oxygenase-1 (HO-1). Induction of HO-1 with hemin or stable transfection of C-26 with a plasmid vector encoding HO-1 increased resistance of tumor cells to PDT-mediated cytotoxicity. On the other hand, zinc (II) protoporphyrin IX, an HO-1 inhibitor, markedly augmented PDT-mediated cytotoxicity towards C-26 and human ovarian carcinoma MDAH2774 cells. Neither bilirubin, biliverdin nor carbon monoxide, direct products of HO-1 catalysed heme degradation, was responsible for cytoprotection. Importantly, desferrioxamine, a potent iron chelator significantly potentiated cytotoxic effects of PDT. Altogether our results indicate that HO-1 is involved in an important protective mechanism against PDT-mediated phototoxicity and administration of HO-1 inhibitors might be an effective way to potentiate antitumor effectiveness of PDT.
引用
收藏
页码:3365 / 3374
页数:10
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