Literature DB >> 26783563

Systemic and tumor-targeted delivery of siRNA by cyclic NGR and isoDGR motif-containing peptides.

Yuanyu Huang1, Qiang Cheng1, Xingyu Jin2, Jia-Li Ji2, Shutao Guo3, Shuquan Zheng1, Xiaoxia Wang1, Huiqing Cao1, Shan Gao2, Xing-Jie Liang3, Quan Du1, Zicai Liang4.   

Abstract

The drug development of siRNA has been seriously hindered by the lack of an effective, safe and clinically applicable delivery system. The cyclic NGR motif and its isomerization product isoDGR recruit CD13 and integrin as their specific receptors, both of which are overexpressed by tumor and neovascular cells. In this study, a bi-functional peptide, named NGR-10R, was designed and tested for siRNA delivery in vitro and in vivo. Through the formation of peptide/siRNA nanoparticles, RNase resistance was greatly enhanced for the siRNAs. Both FACS and confocal assays revealed that the peptide/siRNA complexes were effectively internalized by MDA-MB-231 cells. Gene silencing assays indicated that anti-Lamin A/C siRNA delivered by NGR-10R robustly repressed gene expression in MDA-MB-231 and HUVEC (a CD13(+)/αvβ3(+) cell). Importantly, the siRNAs were efficiently delivered into tumor tissues and localized around the nuclei, as revealed by in vivo imaging and cryosection examination. In summary, NGR-10R not only efficiently delivered siRNAs into MDA-MB-231 cells in vitro but also delivered siRNAs into tumor cells in vivo, taking advantage of its specific binding to CD13 (neovascular) or αvβ3 (MDA-MB-231). Therefore, the NGR-10R peptide provides a promising siRNA delivery reagent that could be used for drug development, particularly for anti-tumor therapeutics.

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Year:  2016        PMID: 26783563     DOI: 10.1039/c5bm00429b

Source DB:  PubMed          Journal:  Biomater Sci        ISSN: 2047-4830            Impact factor:   6.843


  9 in total

1.  siRNA Design and GalNAc-Empowered Hepatic Targeted Delivery.

Authors:  Mei Lu; Mengjie Zhang; Bo Hu; Yuanyu Huang
Journal:  Methods Mol Biol       Date:  2021

2.  NGR-peptide-drug conjugates with dual targeting properties.

Authors:  Kata Nóra Enyedi; Szilárd Tóth; Gergely Szakács; Gábor Mező
Journal:  PLoS One       Date:  2017-06-02       Impact factor: 3.240

3.  Succinimide Formation from an NGR-Containing Cyclic Peptide: Computational Evidence for Catalytic Roles of Phosphate Buffer and the Arginine Side Chain.

Authors:  Ryota Kirikoshi; Noriyoshi Manabe; Ohgi Takahashi
Journal:  Int J Mol Sci       Date:  2017-02-16       Impact factor: 5.923

Review 4.  Therapeutic siRNA: state of the art.

Authors:  Bo Hu; Liping Zhong; Yuanyu Huang; Yuhua Weng; Ling Peng; Yongxiang Zhao; Xing-Jie Liang
Journal:  Signal Transduct Target Ther       Date:  2020-06-19

Review 5.  Nanocomposites as biomolecules delivery agents in nanomedicine.

Authors:  Magdalena Bamburowicz-Klimkowska; Magdalena Poplawska; Ireneusz P Grudzinski
Journal:  J Nanobiotechnology       Date:  2019-04-03       Impact factor: 9.429

6.  Pharmacokinetic Behaviors of Intravenously Administered siRNA in Glandular Tissues.

Authors:  Yuanyu Huang; Qiang Cheng; Jia-Li Ji; Shuquan Zheng; Lili Du; Lingwei Meng; Yidi Wu; Deyao Zhao; Xiaoxia Wang; Li Lai; Huiqing Cao; Kai Xiao; Shan Gao; Zicai Liang
Journal:  Theranostics       Date:  2016-06-18       Impact factor: 11.556

Review 7.  Molecular Imaging of Aminopeptidase N in Cancer and Angiogenesis.

Authors:  Cynthia L Schreiber; Bradley D Smith
Journal:  Contrast Media Mol Imaging       Date:  2018-06-25       Impact factor: 3.161

8.  Phosphate-Catalyzed Succinimide Formation from an NGR-Containing Cyclic Peptide: A Novel Mechanism for Deammoniation of the Tetrahedral Intermediate.

Authors:  Ryota Kirikoshi; Noriyoshi Manabe; Ohgi Takahashi
Journal:  Molecules       Date:  2018-08-31       Impact factor: 4.411

9.  Delivery of antisense oligonucleotide using polyethylenimine-based lipid nanoparticle modified with cell penetrating peptide.

Authors:  Shuang Yang; Dandan Wang; Yaojun Sun; Bin Zheng
Journal:  Drug Deliv       Date:  2019-12       Impact factor: 6.419

  9 in total

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