Capsaicin-Loaded Chitosan Nanocapsules for wtCFTR-mRNA Delivery to a Cystic Fibrosis Cell Line

Kolonko, A Katharina; Efing, Janes; González-Espinosa, Yadira; Bangel-Ruland, Nadine; Driessche, Willy Van; Goycoolea, Francisco M.; Weber, Wolf-Michael

doi:10.3390/biomedicines8090364

Cited by 21 publications

(13 citation statements)

References 76 publications

(109 reference statements)

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“…In that study, the level of transfection was highly dependent on the excipient used for the preparation of the powders, being the MS prepared with HA the ones that gave the best results [ 80 ]—which could be expected taking into account the HA transfection enhancer effect. CS NCs have already been proposed for lung delivery of genes [ 37 ], but they had not been assessed in vivo. The main novelty of this work is that we devised the microencapsulation of the genetic material-loaded CS-based NCs in Ma MS to facilitate their pulmonary administration in dry powders form, leading to revealing results.…”

Section: Resultsmentioning

confidence: 99%

“…In addition, an interesting advantage of the CS-based NCs is that they can be used for a combined gene therapy, loading the genetic material on the coat and an adjuvant lipophilic molecule, in the core. This molecule can enhance the transfection, like capsaicin [ 37 ]—which decreases the thickness of the mucus layer [ 81 ] and opens the intercellular tight junctions in a reversible way [ 82 , 83 ]. The versatility of the simultaneous transport of HA and different active molecules in the same simple structure allows to carry out a synergistic transfection effect, being of enormous value for a more effective treatment of genetic lung diseases.…”

Section: Resultsmentioning

confidence: 99%

“…CS-based NCs were administered in vivo by the oral, nasal and ocular routes, but never before by the pulmonary route for gene therapy purposes [ 1 , 2 , 3 , 4 ], as in this study. In fact, they have recently been evaluated in vitro for gene therapy of CF—by administration of wtCFTR-mRNA in the CF cell line CFBE41o- [ 37 ]—confirming their interest in this field. However, their potential for lung gene therapy has not been investigated in vivo.…”

Section: Introductionmentioning

confidence: 96%

“…They have been assayed as carriers of lipophilic molecules—like anti-inflammatory, antibacterial, and antitumoral drugs (as docetaxel, for the treatment of breast, ovarian and non-small cells lung cancer)—and hydrosoluble AIs—such as peptides, proteins, vaccines (as tetanus toxoid), antigens (as of recombinant hepatitis B surface, influenza and IutA E. coli) and polynucleotides, among many others [ 30 , 31 , 36 ]. In this sense, CS-based NCs are very interesting in gene therapy because they allow the combined administration of genetic material (hydrophilic) on their surface, as well as an adjuvant molecule (lipophilic) in the oily nucleus [ 37 ]. CS-based NCs were administered in vivo by the oral, nasal and ocular routes, but never before by the pulmonary route for gene therapy purposes [ 1 , 2 , 3 , 4 ], as in this study.…”

Section: Introductionmentioning

confidence: 99%

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Microencapsulated Chitosan-Based Nanocapsules: A New Platform for Pulmonary Gene Delivery

et al. 2021

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In this work, we propose chitosan (CS)-based nanocapsules (NCs) for pulmonary gene delivery. Hyaluronic acid (HA) was incorporated in the NCs composition (HA/CS NCs) aiming to promote gene transfection in the lung epithelium. NCs were loaded with a model plasmid (pCMV-βGal) to easily evaluate their transfection capacity. The plasmid encapsulation efficiencies were of approx. 90%. To facilitate their administration to the lungs, the plasmid-loaded NCs were microencapsulated in mannitol (Ma) microspheres (MS) using a simple spray-drying technique, obtaining dry powders of adequate properties. In vivo, the MS reached the deep lung, where the plasmid-loaded CS-based NCs were released and transfected the alveolar cells more homogeneously than the control formulation of plasmid directly microencapsulated in Ma MS. The HA-containing formulation achieved the highest transfection efficiency, in a more extended area and more homogeneously distributed than the rest of tested formulations. The new micro-nanostructured platform proposed in this work represents an efficient strategy for the delivery of genetic material to the lung, with great potential for the treatment of genetic lung diseases.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

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Microencapsulated Chitosan-Based Nanocapsules: A New Platform for Pulmonary Gene Delivery

et al. 2021

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“…5). The two commercial chitosans have been used in biomedical research, especially for the transfection of human cells [54][55][56] . We therefore prepared polyplexes by mixing these chitosans with plasmid DNA encoding eGFP at different molar charge chitosan/DNA ratios.…”

Section: The Pa Influences the Biological Activity Of Chitosansmentioning

confidence: 99%

Biotechnology-Derived Chitosans with Non-Random Patterns of Acetylation Differ from Conventional Chitosans in Their Properties and Activities

Wattjes¹,

Sreekumar²,

Niehues³

et al. 2021

Preprint

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Chitosans are versatile biopolymers with multiple biological activities and potential applications. They are linear copolymers of glucosamine and N-acetylglucosamine defined by their degree of polymerization (DP), fraction of acetylation (FA), and pattern of acetylation (PA). Technical chitosans produced chemically from chitin possess defined DP and FA but random PA, while enzymatically produced natural chitosans are likely to have non-random PA. This natural process has not been replicated using biotechnology because chitin de-N-acetylases do not efficiently deacetylate crystalline chitin. Here, we show that such enzymes can partially N-acetylate polyglucosamine in the presence of excess acetate, yielding chitosans with FA up to 0.7 and an enzyme-dependent non-random PA. The biotech chitosans differ from technical chitosans both in terms of physicochemical and nanoscale solution properties and biological activities. As with synthetic block co-polymers, controlling the distribution of building blocks within the biopolymer chain will open a new dimension of chitosan research and exploitation.

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Nanoencapsulated Systems for Delivery of Phytopharmaceuticals

Renovato‐Núñez¹,

Cobos‐Puc²,

Viveros‐Valdez³

et al. 2023

Advances in Novel Formulations for Drug Delivery

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Capsaicin-Loaded Chitosan Nanocapsules for wtCFTR-mRNA Delivery to a Cystic Fibrosis Cell Line

Cited by 21 publications

References 76 publications

Microencapsulated Chitosan-Based Nanocapsules: A New Platform for Pulmonary Gene Delivery

Microencapsulated Chitosan-Based Nanocapsules: A New Platform for Pulmonary Gene Delivery

Biotechnology-Derived Chitosans with Non-Random Patterns of Acetylation Differ from Conventional Chitosans in Their Properties and Activities

Nanoencapsulated Systems for Delivery of Phytopharmaceuticals

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