呼肠孤病毒在癌症治疗中的进化

B. Jayaprakash, Sivapriya Veeraiyan, S. Gunaseelan, Y. Purushothaman
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摘要

过度活跃的Ras信号最终会导致癌症。人类的3种Ras基因(HRas、KRas和NRas)是人类癌症中最常见的致癌基因。在所有人类肿瘤中,20%至25%的肿瘤中发现了永久性激活Ras的突变,在某些类型的癌症(例如胰腺癌)中发现了高达90%的突变。因此,Ras抑制剂正被研究用于治疗癌症和其他Ras过表达疾病。当研究表明呼肠孤病毒在某些癌细胞系中繁殖良好时,它被认为是一种潜在的癌症治疗药物。它在具有激活的Ras通路(一种参与细胞生长和分化的细胞信号通路)的细胞中特异性复制。呼肠孤病毒在ras激活的肿瘤细胞内复制并最终杀死肿瘤细胞,当细胞死亡时,其子代病毒颗粒可以自由地感染周围的癌细胞。这种感染、复制和细胞死亡的循环被认为是重复的,直到所有携带激活Ras通路的肿瘤细胞被破坏。呼肠孤病毒是一种双链核糖核酸病毒和良性人类病原体,以其未经修饰的形式优先感染和杀死癌细胞,是目前国际上正在进行临床试验的主要溶瘤病毒之一。重要的是,呼肠孤病毒已被证明是有效的单一疗法,以及与其他抗癌选择,包括放疗和化疗药物,如吉西他滨,多西紫杉醇,紫杉醇和卡铂联合使用。
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Evolution of Reovirus in Cancer Therapy
The overactive Ras signaling can ultimately lead to cancer. The 3 Ras genes in humans (HRas, KRas, and NRas) are the most common oncogenes in human cancer.Mutations that permanently activate Ras are found in 20% to 25% of all human tumors and up to 90% in certain types of cancer (e.g., pancreatic cancer). For this reason, Ras inhibitors are being studied as a treatment for cancer and other diseases with Ras overexpression. Reovirus was noted to be a potential cancer therapeutic when studies suggested it reproduces well in certain cancer cell lines. It replicates specifically in cells that have an activated Ras pathway (a cellular signaling pathway that is involved in cell growth and differentiation).Reovirus replicates in and eventually kills Ras-activated tumour cells and as cell death occurs, progeny virus particles are free to infect surrounding cancer cells. This cycle of infection, replication and cell death is believed to be repeated until all tumour cells carrying an activated Ras pathway are destroyed.Reovirus, a double-stranded ribonucleic acid virus and benign human pathogen, preferentially infects and kills cancer cells in its unmodified form, and is one of the leading oncolytic viruses currently undergoing clinical trials internationally. Importantly, reovirus has been shown to be effective as a monotherapy, as well as in combination with other anticancer options, including radiation and chemotherapeutic agents, such as gemcitabine, docetaxel, paclitaxel, and carboplatin.
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