Improved cell-penetrating peptide–PNA conjugates for splicing redirection in HeLa cells and exon skipping in mdx mouse muscle
Gabriela D. Ivanova,Andrey A. Arzumanov,Rachida Abes,HaiFang Yin,Matthew J.A. Wood,Bernard Lebleu,Michael J. Gait +6 more
TL;DR: It is shown that Pip-PNA705 conjugates are internalized in HeLa cells by an energy-dependent mechanism and that the predominant pathway of cell uptake of biologically active conjugate seems to be via clathrin-dependent endocytosis.
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Abstract: Steric blocking peptide nucleic acid (PNA) oligonucleotides have been used increasingly for redirecting RNA splicing particularly in therapeutic applications such as Duchenne muscular dystrophy (DMD). Covalent attachment of a cell-penetrating peptide helps to improve cell delivery of PNA. We have used a HeLa pLuc705 cell splicing redirection assay to develop a series of PNA internalization peptides (Pip) conjugated to an 18-mer PNA705 model oligonucleotide with higher activity compared to a PNA705 conjugate with a leading cell-penetrating peptide being developed for therapeutic use, (R-Ahx-R)(4). We show that Pip-PNA705 conjugates are internalized in HeLa cells by an energy-dependent mechanism and that the predominant pathway of cell uptake of biologically active conjugate seems to be via clathrin-dependent endocytosis. In a mouse model of DMD, serum-stabilized Pip2a or Pip2b peptides conjugated to a 20-mer PNA (PNADMD) targeting the exon 23 mutation in the dystrophin gene showed strong exon-skipping activity in differentiated mdx mouse myotubes in culture in the absence of an added transfection agent at concentrations where naked PNADMD was inactive. Injection of Pip2a-PNADMD or Pip2b-PNADMD into the tibealis anterior muscles of mdx mice resulted in approximately 3-fold higher numbers of dystrophin-positive fibres compared to naked PNADMD or (R-Ahx-R)(4)-PNADMD.
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Citations
Cell-penetrating peptides : methods and protocols
Ülo Langel
- 01 Jan 2011
TL;DR: The present invention relates to the development of innovative cellpenetrating peptides (CPPs) to deliver cargos inside cells with very high efficiency and without noticeable toxicity.
Anchor peptide captures, targets, and loads exosomes of diverse origins for diagnostics and therapy
Xianjun Gao,Ning Ran,Xue Dong,Bingfeng Zuo,Rong Yang,Qibing Zhou,Hong M. Moulton,Yiqi Seow,HaiFang Yin +8 more
TL;DR: This study demonstrates that an exosomal anchor peptide enables direct, effective functionalization and capture of exosomes, thus providing a tool for exosome engineering, probing gene function in vivo, and targeted therapeutic drug delivery.
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Delivery of therapeutic oligonucleotides with cell penetrating peptides
Prisca Boisguerin,Sébastien Deshayes,Michael J. Gait,Liz O'Donovan,Caroline Godfrey,Corinne A. Betts,Matthew J.A. Wood,Bernard Lebleu +7 more
TL;DR: A comprehensive coverage of the enormous amount of published data was not possible, so emphasis has been put on strategies that have proven to be effective in animal models of important human diseases and on examples taken from the authors' own expertise.
253
Cell-penetrating Peptides as Versatile Vehicles for Oligonucleotide Delivery
TL;DR: The number of studies demonstrating very high therapeutic potential of noncovalent complexes of ONs with novel CPP-based delivery vehicles is explosively increasing and the recent developments in the application of C PP-mediated oligonucleotide delivery by noncavalent strategy will be discussed.
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Peptide nucleic acids (PNA) in chemical biology and drug discovery.
TL;DR: This review will focus on the general properties of PNA, the main applications as they appear today, and with emphasis on the most recent developments.
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Peptide Conjugates of Oligonucleotide Analogs and siRNA for Gene Expression Modulation
John Turner,Andrey Arzumanov,Gabriela Ivanova,Martin Fabani,Michael Gait +4 more
TL;DR: Researchers develop peptide conjugates of oligonucleotide analogs and siRNA to modulate gene expression, overcoming delivery challenges through chemical synthesis and conjugation with cell-penetrating peptides, enhancing therapeutic potential for various applications.
Sustained dystrophin expression induced by peptide-conjugated morpholino oligomers in the muscles of mdx mice.
Natee Jearawiriyapaisarn,Hong M. Moulton,Brian Buckley,Jennifer Roberts,Peter Sazani,Suthat Fucharoen,Suthat Fucharoen,Patrick L. Iversen,Ryszard Kole,Ryszard Kole +9 more
TL;DR: PPMO M23D-B, designed to force skipping of stop-codon containing dystrophin exon 23, is investigated in an mdx mouse model of Duchenne muscular dystrophy, the first report of oligonucleotide-mediated exon skipping and dystrophic protein induction in the heart of treated animals.
Modification of splicing in the dystrophin gene in cultured Mdx muscle cells by antisense oligoribonucleotides
TL;DR: A novel approach to correct dystrophin deficiency at the post-transcriptional level by transfection of muscle cells with antisense RNA, which may in the future offer a therapeutic approach for DMD, as well as for other inherited disorders.
Cell penetrating peptide conjugates of steric block oligonucleotides
Bernard Lebleu,Hong M. Moulton,Rachida Abes,Gabriela D. Ivanova,Saïd Abes,David A. Stein,Patrick L. Iversen,Andrey A. Arzumanov,Michael J. Gait +8 more
TL;DR: Two new families of arginine-rich CPPs named (R-Ahx-R)4 AhxB and R6Pen allow efficient nuclear delivery of splice correcting PNA and PMO at micromolar concentrations in the absence of endosomolytic agents.
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TL;DR: In this article, reliable protocols for disulfide conjugation that have been verified for both cationic and hydrophobic peptides as well as oligonucleotides containing deoxyribonucleosides and their analogs are presented.
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