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Literature DB >> 23603860

Inhibition of lung metastasis by chemokine CCL17-mediated in vivo silencing of genes in CCR4+ Tregs.

Arya Biragyn¹, Monica Bodogai, Purevdorj B Olkhanud, Sinan R Denny-Brown, Nitin Puri, Koichi Ayukawa, Shiro Kanegasaki, Cory M Hogaboam, Katarzyna Wejksza, Catalina Lee-Chang.

Abstract

Despite significant attractiveness of antisense oligonucleotide/RNAi technology, its clinical application has been precluded by a lack of methods for targeted delivery and transduction of primary immune cells in vivo. Here, we devised a chemokine CCL17-based strategy (TARC-arp) that transiently silences expression of genes in immune cells by delivering inhibitory oligonucleotides through their chemokine receptors. In modeling studies using mice with established 4T1.2 breast cancer, we show that IL10 produced by CCR4 cells, in particular FoxP3 regulatory T cells (Tregs), plays an important role in lung metastasis. As such, TARC-arp-mediated silencing of IL10 or FoxP3 in CCR4 Tregs is sufficient to block lung metastasis. Thus, we provide a simple solution that circumvents the problems of RNAi use in vivo, indicating that a disease outcome can be successfully controlled by delivering inhibitory oligonucleotides with chemokines to inactivate a selective subset of immune cells.

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Year: 2013 PMID： 23603860 PMCID： PMC3707614 DOI： 10.1097/CJI.0b013e318294357c

Source DB: PubMed Journal: J Immunother ISSN： 1524-9557 Impact factor: 4.456

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