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细胞表面分子和自体腹水在决定腺病毒转导卵巢癌细胞效率中的作用。

Role of cell surface molecules and autologous ascitic fluid in determining efficiency of adenoviral transduction of ovarian cancer cells.

机构信息

Department of Oncology, Cancer Research UK Clinical Centre in Leeds, St James's University Hospital, Leeds, UK.

出版信息

Cancer Gene Ther. 2010 Oct;17(10):684-93. doi: 10.1038/cgt.2010.24. Epub 2010 Jun 11.

Abstract

Adenovirus is the most frequently used virus in gene therapy clinical trials. There have been conflicting reports on the ability of adenovirus to transduce primary ovarian cancer samples and the expression of relevant cell surface molecules. These factors were examined using primary ovarian cancer cells cultured from ascites and solid tumor to gain insights into the clinical use of adenovirus in ovarian cancer. The level of transduction of primary cultures was much higher than uncultured cells and established cell lines, and correlated with higher levels of coxsackie-adenovirus receptor (CAR) and integrin expression. Growth of primary cultures in autologous ascitic fluid prevented an increase in CAR expression and inhibited transduction compared with cells treated in supplemented RPMI. Cells at the periphery of solid tumor samples were transduced using a replication-incompetent virus and correlated with CAR expression. However, transduction was abolished by autologous ascitic fluid, despite the expression of CAR. We conclude that the use of adenoviruses for ovarian cancer gene therapy will require testing in the presence of inhibitory factors in ascitic fluid. The clinical use of adenoviral vectors may require circumvention of such inhibitory factors and the use of replication competent adenovirus to enable efficient viral penetration of the cancer.

摘要

腺病毒是基因治疗临床试验中最常使用的病毒。关于腺病毒转导原发性卵巢癌细胞样本和相关细胞表面分子表达的能力,已有相互矛盾的报告。本研究使用从腹水和实体瘤中培养的原发性卵巢癌细胞来检测这些因素,以深入了解腺病毒在卵巢癌中的临床应用。与未培养的细胞和已建立的细胞系相比,原代培养物的转导水平要高得多,并且与 Coxsackie-adenovirus 受体(CAR)和整合素表达水平更高相关。与用补充的 RPMI 处理的细胞相比,在自体腹水培养原代培养物可防止 CAR 表达增加并抑制转导。使用复制缺陷型病毒对实体瘤样本周边的细胞进行转导,与 CAR 表达相关。然而,尽管表达了 CAR,但自体腹水还是会抑制转导。我们的结论是,腺病毒在卵巢癌基因治疗中的应用需要在腹水存在抑制因子的情况下进行测试。腺病毒载体的临床应用可能需要规避这种抑制因子,并使用复制型腺病毒,以实现病毒对癌症的有效穿透。

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