Department of Experimental Pathology, Mayo Clinic College of Medicine, Rochester, Minnesota 55905, USA.
J Biol Chem. 2010 Apr 16;285(16):12011-27. doi: 10.1074/jbc.M109.097790. Epub 2010 Feb 12.
Lung cancer is the leading cause of cancer-related deaths worldwide. Here we show for the first time that HtrA3 is a mitochondrial stress-response factor that promotes cytotoxicity to etoposide and cisplatin in lung cancer cell lines. Exogenous expression of wild type HtrA3 domain variants significantly attenuated cell survival with etoposide and cisplatin treatment in lung cancer cell lines H157 and A549 compared with expression of protease inactive mutants (S305A) or vector control. Conversely, HtrA3 suppression promoted cell survival with etoposide and cisplatin treatment in lung cancer cell lines Hop62 and HCC827. Survival was attenuated by re-expression of wild type HtrA3 variants during treatment but not by protease inactive mutants or vector control. HtrA3 also co-fractionated and co-localized with mitochondrial markers with both endogenous and exogenous expression in normal lung and lung cancer cell lines but was translocated from mitochondria following etoposide treatment. Moreover, HtrA3 translocation from mitochondria correlated with an increase in cell death that was attenuated by either HtrA3 suppression or Bcl-2 overexpression. Taken together, these results suggest that HtrA3 may be a previously uncharacterized mitochondrial cell death effector whose serine protease function may be crucial to modulating etoposide- and cisplatin-induced cytotoxicity in lung cancer cell lines.
肺癌是全球癌症相关死亡的主要原因。在这里,我们首次表明 HtrA3 是一种线粒体应激反应因子,可促进肺癌细胞系对依托泊苷和顺铂的细胞毒性。与表达蛋白酶失活突变体(S305A)或载体对照相比,外源性表达野生型 HtrA3 结构域变体可显著降低肺癌细胞系 H157 和 A549 中依托泊苷和顺铂处理后的细胞存活率。相反,HtrA3 抑制可促进肺癌细胞系 Hop62 和 HCC827 中依托泊苷和顺铂处理后的细胞存活。在治疗过程中,通过重新表达野生型 HtrA3 变体可降低存活率,但蛋白酶失活突变体或载体对照则不能。HtrA3 还与内源性和外源性表达的线粒体标志物共分馏和共定位,但在用依托泊苷处理后从线粒体易位。此外,HtrA3 从线粒体易位与细胞死亡增加相关,该增加可通过 HtrA3 抑制或 Bcl-2 过表达来减弱。总之,这些结果表明 HtrA3 可能是一种以前未被表征的线粒体细胞死亡效应因子,其丝氨酸蛋白酶功能对于调节肺癌细胞系中依托泊苷和顺铂诱导的细胞毒性可能至关重要。
