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蛋白激酶 C 激活和肌动蛋白丝解聚对碳酸磷灰石介导的淋巴细胞转染的协同作用。

Synergistic effect of PKC activation and actin filament disruption on carbonate apatite-facilitated lymphocyte transfection.

机构信息

Graduate School of Bioscience and Biotechnology, Tokyo Institute of Technology, Japan.

出版信息

Biochem Biophys Res Commun. 2012 Mar 16;419(3):482-4. doi: 10.1016/j.bbrc.2012.02.023. Epub 2012 Feb 16.

Abstract

Leukemia and lymphoma cells are potential targets for genetic manipulation in cancer therapy. On the other hand, genetically modified autologous lymphocytes expressing a chimeric antigen against a receptor overexpressed in tumor cells or tumor vasculature are promising cell-based therapeutics for cancer.However, the lack of a smart device for efficient transgene delivery to the lymphocytes poses the major obstacle to the successful clinical applications of these attractive approaches. Recently, we developed a carbonate apatite-based nanocarrier system for effective intracellular delivery and release of DNA molecules, achieving very high level of transgene expression in both primary and cancer cells. Although its efficacy in human T leukemia cells is relatively poor, immobilization of fibronectin and/or chimeric E-cadherin-Fc on particle surface could enhance transgene delivery in presence of an actin filament disrupter. Here, we report for the first time that simultaneous stimulation of human T leukemia cells by a protein kinase C (PKC) activator, a Ca(2+) ionophore and an actin filament disrupter dramatically accelerated carbonate apatite-mediated transgene delivery in the cells, resulting in over 100-fold more efficacy than commcercially available lipofectamine.

摘要

白血病和淋巴瘤细胞是癌症治疗中遗传操作的潜在靶标。另一方面,表达针对肿瘤细胞或肿瘤血管上过表达受体的嵌合抗原的基因修饰自体淋巴细胞是癌症的有前途的基于细胞的治疗方法。然而,缺乏将转基因有效递送至淋巴细胞的智能装置是这些有吸引力的方法成功临床应用的主要障碍。最近,我们开发了一种基于碳酸磷灰石的纳米载体系统,用于有效递送至细胞内和释放 DNA 分子,在原代细胞和癌细胞中均实现了非常高的转基因表达水平。尽管其在人 T 白血病细胞中的功效相对较差,但在肌动蛋白丝破坏剂存在下,将纤连蛋白和/或嵌合 E-钙粘蛋白-Fc 固定在颗粒表面上可以增强转基因的传递。在这里,我们首次报道,蛋白激酶 C(PKC)激活剂、钙离子载体和肌动蛋白丝破坏剂同时刺激人 T 白血病细胞,可显著加速细胞内碳酸磷灰石介导的转基因传递,其功效超过市售脂质体 100 多倍。

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