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首页> 外文期刊>Cancer Cell International >The impact of γ-irradiation on the induction of bystander killing by genetically engineered ovarian tumor cells: implications for clinical use
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The impact of γ-irradiation on the induction of bystander killing by genetically engineered ovarian tumor cells: implications for clinical use

机译:γ射线辐射对转基因卵巢肿瘤细胞诱导旁观者杀伤的影响:对临床的意义

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Cellular based therapeutic approaches for cancer rely on careful consideration of finding the optimal cell to execute the cellular goal of cancer treatment. Cell lines and primary cell cultures have been used in some studies to compare the in vitro and in vivo efficacy of autologous vs allogeneic tumour cell vaccines. This study examines the effect of γ-irradiation on a range of tumor cell lines in conjunction with suicide gene therapy of cancer. To determine the efficacy of this modality, a series of in vitro and in vivo experiments were conducted using genetically modified and unmodified tumor cell lines. Following co-culture of HSV-TK modified tumor cells and unmodified tumor cells both in vitro and in vivo we observed that the PA-STK ovarian tumor cells were sensitive to γ-irradiation, completely abolishing their ability to induce bystander killing of unmodified tumor cells. In contrast, TK-modified human and mouse mesothelioma cells were found to retain their in vitro and in vivo bystander killing effect after γ-irradiation. Morphological evidence was consistent with the death of PA-STK cells being by pyknosis after γ-irradiation. These results suggest that PA-STK cells are not suitable for clinical application of suicide gene therapy of cancer, as lethal γ-irradiation (100?Gy) interferes with their bystander killing activity. However, the human mesothelioma cell line CRL-5830-TK retained its bystander killing potential after exposure to similarly lethal γ-irradiation (100?Gy). CRL-5830 may therefore be a suitable vehicle for HSV-TK suicide gene therapy. This study highlights the diversity among tumor cell lines and the careful considerations needed to find the optimal tumor cell line for this type of suicide gene therapy of cancer.
机译:基于细胞的癌症治疗方法依赖于仔细考虑寻找最佳细胞以执行癌症治疗的细胞目标。细胞系和原代细胞培养已用于一些研究中,以比较自体和异源肿瘤细胞疫苗的体外和体内功效。这项研究结合癌症的自杀基因疗法,研究了γ射线对一系列肿瘤细胞系的影响。为了确定这种方式的功效,使用基因修饰和未修饰的肿瘤细胞系进行了一系列的体外和体内实验。在体外和体内共培养HSV-TK修饰的肿瘤细胞和未修饰的肿瘤细胞后,我们观察到PA-STK卵巢肿瘤细胞对γ辐射敏感,从而完全消除了它们诱导旁观者杀死未修饰的肿瘤细胞的能力。 。相比之下,发现经TK修饰的人和小鼠间皮瘤细胞在γ射线照射后保留了其体外和体内旁观者杀伤作用。形态学证据与γ-射线照射后经变导致的PA-STK细胞死亡一致。这些结果表明,PA-STK细胞不适合用于癌症自杀基因疗法的临床应用,因为致命的γ射线辐射(100?Gy)会干扰其旁观者的杀伤活性。然而,人类间皮瘤细胞系CRL-5830-TK在暴露于类似的致命γ辐射(100?Gy)后仍保留了其旁观者杀伤力。因此,CRL-5830可能是HSV-TK自杀基因治疗的合适载体。这项研究强调了肿瘤细胞系之间的多样性,以及为这种自杀基因疗法寻找最佳肿瘤细胞系所需的谨慎考虑。

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