pH-Sensitive N,N-Dimethylalkane-1-amine N-Oxides in DNA Delivery: From Structure to Transfection Efficiency

Liskayová, Gilda; Hubčík, Lukáš; Búcsi, Alexander; Fazekáš, Tomáš; Martínez, Juan Carlos; Devı́nsky, Ferdinand; Pisárčik, Martin; Hanulová, Mária; Ritz, Sandra; Uhrı́ková, Daniela

doi:10.1021/acs.langmuir.9b02353

Cited by 6 publications

(3 citation statements)

References 73 publications

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“…Interestingly, PxB molecules mediated “close mutual contact” of EPS bilayers even if they constitute ULV that are diluted enough to avoid any interaction between particles (1 wt % of the lipid). This finding correlates well with the concept that PxB mimics the properties of SP-B protein and the formation of stable vesicle–vesicle contacts allowing the exchange of phospholipids. , A similar “condensing” effect was recently reported for the interaction of cationic nanoparticles and polymers with PSUR, , cationic liposomes with polyelectrolytes of opposite charges, such as DNA, − or in the context of antimicrobial mechanisms of cationic peptides that interact with bacterial model membranes . However, it is worth stressing two points: (1) our experiments show that binding of PxB molecules onto EPS bilayers results in charge inversion of the membrane, as shown by the zeta potential and proved by SANS measurements.…”

Section: Resultssupporting

confidence: 90%

Polymyxin B-Enriched Exogenous Lung Surfactant: Thermodynamics and Structure

Královič-Kanjaková,

Asi Shirazi,

Hubčík

et al. 2024

Langmuir

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The use of an exogenous pulmonary surfactant (EPS) to deliver other relevant drugs to the lungs is a promising strategy for combined therapy. We evaluated the interaction of polymyxin B (PxB) with a clinically used EPS, the poractant alfa Curosurf (PSUR). The effect of PxB on the protein-free model system (MS) composed of four phospholipids (diC16:0PC/16:0–18:1PC/16:0–18:2PC/16:0–18:1PG) was examined in parallel to distinguish the specificity of the composition of PSUR. We used several experimental techniques (differential scanning calorimetry, small- and wide-angle X-ray scattering, small-angle neutron scattering, fluorescence spectroscopy, and electrophoretic light scattering) to characterize the binding of PxB to both EPS. Electrostatic interactions PxB–EPS are dominant. The results obtained support the concept of cationic PxB molecules lying on the surface of the PSUR bilayer, strengthening the multilamellar structure of PSUR as derived from SAXS and SANS. A protein-free MS mimics a natural EPS well but was found to be less resistant to penetration of PxB into the lipid bilayer. PxB does not affect the gel-to-fluid phase transition temperature, T m, of PSUR, while T m increased by ∼+ 2 °C in MS. The decrease of the thickness of the lipid bilayer (d L) of PSUR upon PxB binding is negligible. The hydrophobic tail of the PxB molecule does not penetrate the bilayer as derived from SANS data analysis and changes in lateral pressure monitored by excimer fluorescence at two depths of the hydrophobic region of the bilayer. Changes in d L of protein-free MS show a biphasic dependence on the adsorbed amount of PxB with a minimum close to the point of electroneutrality of the mixture. Our results do not discourage the concept of a combined treatment with PxB-enriched Curosurf. However, the amount of PxB must be carefully assessed (less than 5 wt % relative to the mass of the surfactant) to avoid inversion of the surface charge of the membrane.

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Section: Resultssupporting

confidence: 90%

Polymyxin B-Enriched Exogenous Lung Surfactant: Thermodynamics and Structure

Královič-Kanjaková,

Asi Shirazi,

Hubčík

et al. 2024

Langmuir

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“…In addition to the promising utilization of cubic phases for encapsulation and delivery of short fragmented nucleic acids as mentioned above, also cubic and hexagonal structures with DNA strands containing thousands of base pairs have been reported recently (Dittrich et al 2018;Tassler et al 2019). The presence or formation of intracellular nonlamellar, namely cubic phases, on the DNA delivery path was revealed as an enhancing factor of transfection efficiency (Koynova et al 2006;Tenchov et al 2008;Safinya et al 2014;Liskayová et al 2019). The fusogenicity of lipoplexes plays a crucial role in transfection rate.…”

Section: Introductionmentioning

confidence: 95%

Calcium mediated DNA binding in non-lamellar structures formed by DOPG/glycerol monooleate

Kanjaková

Hubčík

Búcsi

et al. 2021

Chemistry and Physics of Lipids

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“…These smart drug carriers were stable at pH 7.4, whereas they showed size increase and 80% release of their cargo within 5 hours at pH 4.5 due to the cleavage of the cyclic acetal. Liskayová et al [137] investigated the relationship between the structure of N,Ndimethylalkane-1-amine N-oxides 62 (CnNO, n=1-18, Fig. 14) and in vitro TE of pH-sensitive DNA-CnNO/DOPE lipoplexes (cationic, non-viral lipid-DNA complexes) by delivering plasmid DNA (pEGFP-N1) into human bone OS epithelial cells (U2OS).…”

Section: Lps Functionalized With Unnatural Ph-sensitive Lipidsmentioning

confidence: 99%

Stimulus-responsive liposomes for biomedical applications

Antoniou

Giofrè

Seneci

et al. 2021

Drug Discovery Today

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Liposomes are amphipathic lipidic supramolecular aggregates able to encapsulate and carry molecules of both hydrophilic and hydrophobic nature. They have been widely used as in vivo drug delivery systems since long due to their favorable features, such as synthetic flexibility, biodegradability, biocompatibility, low immunogenicity, and negligible toxicity. In recent years, the possibility to introduce chemical modifications on liposomes has paved the way to smart liposome-based drug delivery systems characterized by even more tunable and disease-directed features. In this review, the different types of chemical modifications introduced so far have been highlighted, with a particular focus on internal stimuli-responsive liposomes and pro-drug activation.

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pH-Sensitive N,N-Dimethylalkane-1-amine N-Oxides in DNA Delivery: From Structure to Transfection Efficiency

Cited by 6 publications

References 73 publications

Polymyxin B-Enriched Exogenous Lung Surfactant: Thermodynamics and Structure

Polymyxin B-Enriched Exogenous Lung Surfactant: Thermodynamics and Structure

Calcium mediated DNA binding in non-lamellar structures formed by DOPG/glycerol monooleate

Stimulus-responsive liposomes for biomedical applications

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