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肿瘤进展模型中增强的肿瘤细胞核靶向作用。

Enhanced tumour cell nuclear targeting in a tumour progression model.

作者信息

Nastasie Michael S, Thissen Helmut, Jans David A, Wagstaff Kylie M

机构信息

Nuclear Signalling Laboratory, Department Biochemistry and Molecular Biology, Monash University, Clayton, Victoria, 3800, Australia.

CSIRO Molecular and Health Technologies, Bayview Avenue, Clayton, Victoria, 3168, Australia.

出版信息

BMC Cancer. 2015 Feb 21;15:76. doi: 10.1186/s12885-015-1045-z.

Abstract

BACKGROUND

There is an urgent need for new approaches to deliver bioactive molecules to cancer cells efficiently and specifically.

METHODS

Here we fuse the cancer cell nuclear targeting module of the Chicken Anaemia Virus Apoptin protein to the core histones H2B and H3 and utilise them in transfection, protein transduction and DNA binding assays.

RESULTS

We found subsequent nuclear accumulation of these proteins to be 2-3 fold higher in tumour compared to normal cells in transfected isogenic human osteosarcoma and breast tumour progression models. This represents the first demonstration of enhanced nuclear targeting by Apoptin in a tumour progression model, and its functionality in a heterologous protein context. Excitingly, we found that the innate transduction ability of histones could be exploited in combination with the Apoptin nuclear targeting module to effect an overall 13-fold higher delivery of protein to osteosarcoma cancer cell nuclei compared to their isogenic normal counterparts.

CONCLUSIONS

This is the first report of cancer-cell specificity by a cell penetrating protein, with important implications for the use of protein transduction as a vehicle for gene/drug delivery in the future, and in particular in the development of highly specific and effective anti-cancer agents.

摘要

背景

迫切需要新的方法来高效且特异性地将生物活性分子递送至癌细胞。

方法

在此,我们将鸡贫血病毒凋亡素蛋白的癌细胞核靶向模块与核心组蛋白H2B和H3融合,并将它们用于转染、蛋白质转导和DNA结合测定。

结果

在转染的同基因人骨肉瘤和乳腺肿瘤进展模型中,我们发现与正常细胞相比,这些蛋白质在肿瘤中的后续核积累高2至3倍。这是凋亡素在肿瘤进展模型中增强核靶向及其在异源蛋白背景下功能的首次证明。令人兴奋的是,我们发现组蛋白的天然转导能力可与凋亡素核靶向模块结合利用,与同基因正常对应物相比,向骨肉瘤癌细胞核递送蛋白质的总量高出13倍。

结论

这是关于细胞穿透蛋白具有癌细胞特异性的首次报道,对未来将蛋白质转导用作基因/药物递送载体,尤其是在开发高度特异性和有效的抗癌药物方面具有重要意义。

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