Polymers for Improving the In Vivo Transduction Efficiency of AAV2 Vectors

Moulay, Gilles; Boutin, Sylvie; Masurier, Carole; Scherman, Daniel; Kichler, Antoine

doi:10.1371/journal.pone.0015576

Cited by 14 publications

(16 citation statements)

References 29 publications

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“…When s.c. xenograft models of LoVo or MDA-MB-231 cancers were established, BM-MSCs or iPSC-MSCs transduced with CMV-copGFP lentiviruses were injected via tail vein, and tumors were harvested 16 h later for section and qPCR assay of CMV promoter (50). For tumor initiating and growth assay, HCC1806 cancer cells were coinjected with BM-MSCs or iPSC-MSCs into the fourth mammary fat pad of NOD/SCID mice, and tumors were harvested 6 wk after inoculation.…”

mentioning

confidence: 99%

MSCs derived from iPSCs with a modified protocol are tumor-tropic but have much less potential to promote tumors than bone marrow MSCs

Zhao¹,

Gregory²,

Lee³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

141

139

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Mesenchymal stem or stromal cells (MSCs) have many potential therapeutic applications including therapies for cancers and tissue damages caused by cancers or radical cancer treatments. However, tissue-derived MSCs such as bone marrow MSCs (BM-MSCs) may promote cancer progression and have considerable donor variations and limited expandability. These issues hinder the potential applications of MSCs, especially those in cancer patients. To circumvent these issues, we derived MSCs from transgene-free human induced pluripotent stem cells (iPSCs) efficiently with a modified protocol that eliminated the need of flow cytometric sorting. Our iPSC-derived MSCs were readily expandable, but still underwent senescence after prolonged culture and did not form teratomas. These iPSC-derived MSCs homed to cancers with efficiencies similar to BM-MSCs but were much less prone than BM-MSCs to promote the epithelial-mesenchymal transition, invasion, stemness, and growth of cancer cells. The observations were probably explained by the much lower expression of receptors for interleukin-1 and TGFβ, downstream protumor factors, and hyaluronan and its cofactor TSG6, which all contribute to the protumor effects of BM-MSCs. The data suggest that iPSC-derived MSCs prepared with the modified protocol are a safer and better alternative to BM-MSCs for therapeutic applications in cancer patients. The protocol is scalable and can be used to prepare the large number of cells required for "off-the-shelf" therapies and bioengineering applications.

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mentioning

confidence: 99%

MSCs derived from iPSCs with a modified protocol are tumor-tropic but have much less potential to promote tumors than bone marrow MSCs

Zhao¹,

Gregory²,

Lee³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

141

139

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“…Cationic lipids and polymers have been shown to improve AAV2 transduction efficiency. 28,29 In one study, AAV-mediated insulin gene therapy was combined with preinjection of PEI in mice to achieve increased infection efficiency. 21 However, to our knowledge, we have used electrostatic surface coating of AAV2-VLPs for siRNA delivery for the first time.…”

Section: Discussionmentioning

confidence: 99%

“…Coating of virus-like particles with polymers could have other benefits, such as protection of virus-like particles from neutralization by the immune system and improved infection efficiency. [28][29][30] It is important to know the mechanism of cell penetration and the mechanism of siRNA protection by the novel PEI-AAV2-VLPs. Investigation of these mechanisms in future studies will definitely provide more understanding of this new formulation.…”

Section: Discussionmentioning

confidence: 99%

A novel polyethyleneimine-coated adeno-associated virus-like particle formulation for efficient siRNA delivery in breast cancer therapy: preparation and in vitro analysis

Shao

Paul²,

Abbasi³

et al. 2012

IJN

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Background: Systemic delivery of small interfering RNA (siRNA) is limited by its poor stability and limited cell-penetrating properties. To overcome these limitations, we designed an efficient siRNA delivery system using polyethyleneimine-coated virus-like particles derived from adeno-associated virus type 2 (PEI-AAV2-VLPs). Methods: AAV2-VLPs were produced in insect cells by infection with a baculovirus vector containing three AAV2 capsid genes. Using this method, we generated well dispersed AAV2-VLPs with an average diameter of 20 nm, similar to that of the wild-type AAV2 capsid. The nanoparticles were subsequently purified by chromatography and three viral capsid proteins were confirmed by Western blot. The negatively charged AAV2-VLPs were surface-coated with PEI to develop cationic nanoparticles, and the formulation was used for efficient siRNA delivery under optimized transfection conditions. Results: PEI-AAV2-VLPs were able to condense siRNA and to protect it from degradation by nucleases, as confirmed by gel electrophoresis. siRNA delivery mediated by PEI-AAV2-VLPs resulted in a high transfection rate in MCF-7 breast cancer cells with no significant cytotoxicity. A cell death assay also confirmed the efficacy and functionality of this novel siRNA formulation towards MCF-7 cancer cells, in which more than 60% of cell death was induced within 72 hours of transfection. Conclusion: The present study explores the potential of virus-like particles as a new approach for gene delivery and confirms its potential for breast cancer therapy.

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“…Also, there are relatively few reports of polypeptides being used as scavenger receptor inhibitors. One study showed that pre-injection of polylysine improves the gene transfer efficiency of adeno-associated virus 10-fold when compared to the widely used anionic inhibitor poly-I [84]. Another study showed that pre-injection of scavenger receptor ligand peptides results in a modest 4-fold increase in helper dependent adenovirus activity upon pre-administration [39].…”

Section: Discussionmentioning

confidence: 99%

“…In viral gene delivery, the most frequently used adjuvant is the polyinosinic acid (poly I). Preadministration of poly I, has been used to extend the half-life of adenovirus, adeno-10 associated virus and measles virus by reducing KC uptake [38,[80][81][82][83][84]. One limitation to the widespread use of poly I is toxicity resulting in mortality [38].…”

Section: Scavenger Receptor Blockade (Figure 1-3a)mentioning

confidence: 99%

Development of PEG-peptide scavenger receptor inhibitors for non-viral gene delivery

Allen¹

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The rapid capture and degradation of viral and non‐viral gene delivery nanoparticles by scavenger receptors (SR) on Kupffer cells and fenestrated endothelial cells in the liver results in a decreased half life of all nanoparticles in an in vivo system, as well as a lower percentage of the dose available for delivery to the target organ. Current attempts to achieve SR inhibition involves co‐administering high molecular weight, polyanionic inhibitors. Polyinosinic acid (Poly‐I), the most widely used and potent inhibitor, competes for SR binding and successfully inhibits the uptake and metabolism of viral gene delivery nanoparticles in the liver. However, Poly‐I also activates the immune system, resulting in toxicity in mice, making Poly‐I clinically unacceptable. We have discovered peptide based SR inhibitors that block SR uptake of DNA nanoparticles and improves their metabolic half‐life by forming protein nanoparticles in the blood. Radio‐iodinated PEG‐peptides were used to study the pharmacokinetics and biodistribution to understand the structural properties which influence transfection competency and potency. We hypothesized that the in vivo potency and activity is influenced by the stability of protein nanoparticles formed in the blood. Results show that peptides featuring both hydrophobic and positively charged residues are able to potently inhibit scavenger receptor uptake of non viral gene delivery systems. Support or Funding Information This work was supported by the Iowa Biosciences Academy and University of Iowa Pharmacological Sciences T32 training grant. The Iowa Biosciences Academy is supported by the National Institute Of General Medical Sciences of the National Institutes of Health under Award Number R25GM058939, the University of Iowa (UI) Office of the Vice President for Research and the UI Chief Diversity Office, the Pharmacological Sciences Training grant T32 GM067795 and NIH grant R01 GM087653. This abstract is from the Experimental Biology 2018 Meeting. There is no full text article associated with this abstract published in The FASEB Journal.

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Polymers for Improving the In Vivo Transduction Efficiency of AAV2 Vectors

Cited by 14 publications

References 29 publications

MSCs derived from iPSCs with a modified protocol are tumor-tropic but have much less potential to promote tumors than bone marrow MSCs

MSCs derived from iPSCs with a modified protocol are tumor-tropic but have much less potential to promote tumors than bone marrow MSCs

A novel polyethyleneimine-coated adeno-associated virus-like particle formulation for efficient siRNA delivery in breast cancer therapy: preparation and in vitro analysis

Development of PEG-peptide scavenger receptor inhibitors for non-viral gene delivery

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