Issue 12, 2018
From the journal:

Biomaterials Science

A Pt(iv)-mediated polymer architecture for facile and stimuli-responsive intracellular gene silencing with chemotherapy

Sungjin Jung,a   Jinhwan Kim,b   Swapan Pramanick,c   Hyeongmok Park,c   Hyori Lee,c   Junseok Leec  and  Won Jong Kim ORCID logo *abc  

* Corresponding authors

a School of Interdisciplinary Bioscience and Bioengineering, Pohang University of Science and Technology (POSTECH), Pohang 37673, Republic of Korea
E-mail: wjkim@postech.ac.kr
Fax: +82-54-279-3399
Tel: +82-54-279-2104

b Center for Self-assembly and Complexity, Institute of Basic Science (IBS), Pohang 37673, Republic of Korea

c Department of Chemistry, Pohang University of Science and Technology (POSTECH), Pohang 37673, Republic of Korea

Abstract

Conventional chemotherapy has been impeded by the inherent characteristics of cancer including fast mutagenesis and drug resistance; thus a combination therapy consisting of multiple therapeutic strategies has attracted much attention. However, the loading processes of multiple therapeutic molecules affect each other; thus the development of a nanocarrier that enables independent loading of the cargo molecules has been demanded. Herein, we report an ingeniously designed Pt(IV)-mediated polymeric architecture (Pt-PA) for combinatorial gene and chemotherapy to address the issue, prepared by crosslinking a cationic polymer (polyethylenimine, PEI) with a Pt(IV) prodrug. Therapeutic siRNA (anti-BCL2) was simply loaded by electrostatic interaction to form a stable nanocomplex. In the cellular study, the simultaneous release of both the active Pt(II) drug and siRNA was monitored under the intracellular reducing environment, driven by dissociation of the polymer architecture due to an inherent characteristic of the Pt(IV) crosslinker. Therefore, an enhanced gene silencing effect and an anticancer effect were observed. Furthermore, in the animal study, an improved therapeutic effect of the nanocomplex was observed, which can be explained by tumor targeting via the EPR effect, and enhanced drug and siRNA release at the intracellular environment simultaneously. Taken together, the overall results from in vitro and in vivo studies strongly suggest the therapeutic potential of our precisely designed Pt(IV)-mediated polymer architecture.

Graphical abstract: A Pt(iv)-mediated polymer architecture for facile and stimuli-responsive intracellular gene silencing with chemotherapy

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Article information

DOI
https://doi.org/10.1039/C8BM01019F
Article type
Paper
Submitted
23 Aug 2018
Accepted
05 Oct 2018
First published
08 Oct 2018

Biomater. Sci., 2018,6, 3345-3355

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A Pt(IV)-mediated polymer architecture for facile and stimuli-responsive intracellular gene silencing with chemotherapy

S. Jung, J. Kim, S. Pramanick, H. Park, H. Lee, J. Lee and W. J. Kim, Biomater. Sci., 2018, 6, 3345 DOI: 10.1039/C8BM01019F

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