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首页> 外文期刊>Brazilian Journal of Medical and Biological Research >p19Arf sensitizes B16 melanoma cells to interferon-β delivered via mesenchymal stem cells in vitro
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p19Arf sensitizes B16 melanoma cells to interferon-β delivered via mesenchymal stem cells in vitro

机译:P19ARF在体外将B16黑色素瘤细胞感染到通过间充质干细胞递送的干扰素-β

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摘要

The immune stimulatory and anti-neoplastic functions of type I interferon have long been applied for the treatment of melanoma. However, the systemic application of high levels of this recombinant protein is often met with toxicity. An approach that provides localized, yet transient, production of type I interferon may overcome this limitation. We propose that the use of mesenchymal stem cells (MSCs) as delivery vehicles for the production of interferon-β (IFNβ) may be beneficial when applied together with our cancer gene therapy approach. In our previous studies, we have shown that adenovirus-mediated gene therapy with IFNβ was especially effective in combination with p19Arf gene transfer, resulting in immunogenic cell death. Here we showed that MSCs derived from mouse adipose tissue were susceptible to transduction with adenovirus, expressed the transgene reliably, and yet were not especially sensitive to IFNβ production. MSCs used to produce IFNβ inhibited B16 mouse melanoma cells in a co-culture assay. Moreover, the presence of p19Arf in the B16 cells sensitizes them to the IFNβ produced by the MSCs. These data represent a critical demonstration of the use of MSCs as carriers of adenovirus encoding IFNβ and applied as an anti-cancer strategy in combination with p19Arf gene therapy.
机译:I型干扰素的免疫刺激和抗肿瘤功能长期以来一直应用于黑色素瘤的治疗方法。然而,通常会满足毒性高水平的该重组蛋白的全身应用。提供局部化但暂时的I型干扰素的方法可能会克服这种限制。我们提出使用间充质干细胞(MSCs)作为用于生产干扰素-β(IFNβ)的递送载体可能是有益的,当与我们的癌症基因治疗方法一起应用。在我们以前的研究中,我们表明,腺病毒介导的具有IFNβ的基因治疗与P19ARF基因转移结合特别有效,导致免疫原性细胞死亡。在这里,我们展示衍生自小鼠脂肪组织的MSCs易于与腺病毒进行转导,可靠地表达转基因,但对IFNβ产生没有特别敏感。用于生产IFNβ的MSCs在共培养测定中抑制B16小鼠黑素瘤细胞。此外,B16细胞中P19ARF的存在使它们敏感到MSCs产生的IFNβ中。这些数据表示MSCs作为编码IFNβ的腺病毒的载体的使用,并用作P19ARF基因治疗的抗癌策略。

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