Transfection efficacy and drug release depends upon the <scp>PEG</scp> derivative in cationic lipoplexes: Evaluation in <scp>3D</scp> in vitro model and in vivo

Gileva, Anastasia; Koloskova, Olesya O.; Nosova, A S; Vishniakova, L.I.; Simonova, V. A.; Kurbanova, L. A.; Егоренков, Е. А.; Смирнов, В. В.; Буданова, У. А.; Sebyakin, Yu. L.; Suzina, N. E.; Khaitov, Musa; Марквичева, Елена

doi:10.1002/jbm.b.35259

Cited by 3 publications

(1 citation statement)

References 34 publications

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“…Our previous findings demonstrate that an increase in the proportion of DOPE in liposome formulations, based on 2X3, enhances the efficiency of mRNA delivery to eukaryotic cells [38]. The addition of 1,2-distearoyl-sn-glycero-3-phosphoethanolamine-N-[methoxy(polyethyleneglycol)-2000] (DSPE-PEG 2000 ) plays a significant role in achieving efficient nuclease protection of siRNA and prolonged drug release of the PEGylated lipoplexes [39]. The prepared cationic liposomes had a size of 59 ± 1 nm and ζ-potential of +50.9±1.3 mV, as characterized by DLS.…”

Section: Resultsmentioning

confidence: 99%

Cell-penetrating peptide and cationic liposomes mediated siRNA delivery to arrest growth of chronic myeloid leukemia cellsin vitro

Vysochinskaya,

Zabrodskaya,

Dovbysh

et al. 2023

Preprint

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Gene silencing through RNA interference (RNAi) is a promising therapeutic approach for a wide range of disorders, including cancer. Non-viral gene therapy, using specific siRNAs againstBCR-ABL, can be a supportive or alternative measure to traditional chronic myeloid leukemia (CML) tyrosine kinase inhibitor (TKIs) therapies, given the prevalence of clinical TKI resistance. The main challenge for such approaches remains the development of the effective delivery system for siRNA tailored to the specific disease model.The purpose of this study was to examine and compare the efficiency of endosomolytic cell penetrating peptide (CPP) EB1 and PEG2000-decorated cationic liposomes composed of polycationic lipid 1,26-bis(cholest-5-en-3-yloxycarbonylamino)-7,11,16,20-tetraazahexacosane tetrahydrochloride (2X3) and helper lipid 1,2-dioleoyl-sn-glycero-3-phosphoethanolamine (DOPE) for anti-bcr-abl siRNA delivery into the K562 human CML cell line. We show that both EB1 and 2X3-DOPE-DSPE-PEG2000(0.62% mol.) liposomes effectively deliver siRNA into K562 cells by endocytic mechanisms, and the use of liposomes leads to more effective inhibition of expression of the targeted gene (BCR-ABL) and cancer cell proliferation. Taken together, these findings suggest that PEG-decorated cationic liposomes mediated siRNA delivery allows an effective antisense suppression of certain oncogenes, and represents a promising new class of therapies for CML.

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Section: Resultsmentioning

confidence: 99%

Cell-penetrating peptide and cationic liposomes mediated siRNA delivery to arrest growth of chronic myeloid leukemia cellsin vitro

Vysochinskaya,

Zabrodskaya,

Dovbysh

et al. 2023

Preprint

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CMC/SWCNT biocomposites: A combined study on experiments, molecular simulations and continuum models

Mergen,

Gul,

Kacar

et al. 2024

Materials Today Communications

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Cationic and ionizable amphiphiles based on di-hexadecyl ester of <I>L</I>-glutamic acid for liposomal transport of RNA

Bukharin,

Budanova,

Denieva

et al. 2024

Biologičeskie membrany

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Various RNAs are among the most promising and actively developed therapeutic agents for the treatment of tumors, infectious diseases and a number of other pathologies associated with the dysfunction of specific genes. Some nanocarriers are used for the effective delivery of RNAs to target cells, including liposomes based on cationic and/or ionizable amphiphiles. Cationic amphiphiles contain a protonated amino group and exist as salts in an aqueous environment. Ionizable amphiphiles are a new generation of cationic lipids that exhibit reduced toxicity and immunogenicity and undergo ionization only in the acidic environment of the cell. In this work we developed a scheme for the preparation and carried out the synthesis of new cationic and ionizable amphiphiles based on natural amino acids (L-glutamic acid, glycine, beta-alanine, and gamma-aminobutyric acid). Cationic and ionizable liposomes were formed based on the obtained compounds, mixed with natural lipids (phosphatidylcholine and cholesterol), and their physicochemical characteristics (particle size, zeta potential, and storage stability) were determined. Average diameter of particles stable for 5–7 days did not exceed 100 nm. Zeta potential of cationic and ionizable liposomes was about 30 and 1 mV, respectively. The liposomal particles were used to form complexes with RNA molecules. Such RNA complexes were characterized by atomic force microscopy and their applicability for nucleic acid transport was determined.

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Transfection efficacy and drug release depends upon the PEG derivative in cationic lipoplexes: Evaluation in 3D in vitro model and in vivo

Cited by 3 publications

References 34 publications

Cell-penetrating peptide and cationic liposomes mediated siRNA delivery to arrest growth of chronic myeloid leukemia cellsin vitro

Cell-penetrating peptide and cationic liposomes mediated siRNA delivery to arrest growth of chronic myeloid leukemia cellsin vitro

CMC/SWCNT biocomposites: A combined study on experiments, molecular simulations and continuum models

Cationic and ionizable amphiphiles based on di-hexadecyl ester of <I>L</I>-glutamic acid for liposomal transport of RNA

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