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Dive into the research topics where Elzbieta Pedziwiatr-Werbicka is active.

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Featured researches published by Elzbieta Pedziwiatr-Werbicka.


Colloids and Surfaces B: Biointerfaces | 2011

Characterization of complexes formed by polypropylene imine dendrimers and anti-HIV oligonucleotides

Elzbieta Pedziwiatr-Werbicka; Małgorzata Ferenc; Marian Zaborski; Barbara Gabara; Barbara Klajnert; Maria Bryszewska

Current anti-HIV therapies are capable of controlling viral infection but do not represent a definitive cure. They rely on the administration of antiretroviral nucleoside analogues, either alone or in combination with vectors. Dendrimers are branched, synthetic polymers with layered architectures, promising non-viral vectors in gene therapy. The aim of the paper was to study the interactions between three anti-HIV antisense oligonucleotides (ODNs): SREV, ANTI TAR, GEM91 and different generation polypropylene imine dendrimers (PPI) by monitoring changes in the fluorescence polarization of fluorescein attached to the ends of the ODNs when increasing concentrations of dendrimers were added. Laser Doppler electrophoresis, dynamic light scattering (DLS) and transmission electron microscopy (TEM) were used to characterize, respectively, zeta potential, particle size and morphology of dendriplexes formed in different molar ratios. Antisense oligonucleotides interacted with polypropylene imine dendrimers in different molar ratios depending on generation. Zeta potential of dendriplexes varied from (-25 to -21) mV to -5 mV (for PPIG3 and PPIG4 complexes) and to zero (for PPIG2 complexes). The structures presented a polydisperse size from about 50 nm to even 700-800 nm by TEM and about 250 nm by DLS. It means that besides single dendriplexes, aggregates were also present.


Pharmaceutics | 2011

Fourth generation phosphorus-containing dendrimers: prospective drug and gene delivery carrier.

Dzmitry Shcharbin; Volha Dzmitruk; Antos Shakhbazau; Natalya Goncharova; Ihar Seviaryn; Svetlana Kosmacheva; Mihail Potapnev; Elzbieta Pedziwiatr-Werbicka; Maria Bryszewska; M. Talabaev; A. Chernov; Vladimir A. Kulchitsky; Anne-Marie Caminade; Jean-Pierre Majoral

Research concerning new targeting delivery systems for pharmacologically active molecules and genetic material is of great importance. The aim of the present study was to investigate the potential of fourth generation (P4) cationic phosphorus-containing dendrimers to bind fluorescent probe 8-anilino-1-naphthalenesulfonate (ANS), anti-neoplastic drug cisplatin, anti-HIV siRNA siP24 and its capability to deliver green fluorescent protein gene (pGFP) into cells. The interaction between P4 and ANS (as the model drug) was investigated. The binding constant and the number of binding centers per one molecule of P4 were determined. In addition, the dendriplex between P4 and anti-HIV siRNA siP24 was characterized using circular dichroism, fluorescence polarization and zeta-potential methods; the average hydrodynamic diameter of the dendriplex was calculated using zeta-size measurements. The efficiency of transfection of pGFP using P4 was determined in HEK293 cells and human mesenchymal stem cells, and the cytotoxicity of the P4-pGFP dendriplex was studied. Furthermore, enhancement of the toxic action of the anti-neoplastic drug cisplatin by P4 dendrimers was estimated. Based on the results, the fourth generation cationic phosphorus-containing dendrimers seem to be a good drug and gene delivery carrier candidate.


Biochimica et Biophysica Acta | 2012

siRNA carriers based on carbosilane dendrimers affect zeta potential and size of phospholipid vesicles.

Maksim Ionov; Zuzana Garaiova; Iveta Waczulíková; Dominika Wrobel; Elzbieta Pedziwiatr-Werbicka; Rafael Gomez-Ramirez; Francisco Javier de la Mata; Barbara Klajnert; Tibor Hianik; Maria Bryszewska

One of the major limitations in gene therapy is an inability of naked siRNA to passively diffuse through negatively charged cell membranes. Therefore, the siRNA transport into a cell requires efficient carriers. In this work we analyzed the charge-dependent interaction of the complexes of cationic carbosilane dendrimers (CBD) and anti-HIV siRNA (dendriplexes) with the model membranes - large unilamellar vesicles (LUV). We used the second generation of branched with CBD carbon-silicon bonds (CBD-CS) which are water-stable and that of oxygen-silicon bonds (CBD-OS) which are slowly hydrolyzed in aqueous solutions. The LUVs were composed of zwitterionic dimyristoylphosphatidylcholine (DMPC), negatively charged dipalmitoylphosphatidylglycerol (DPPG) and their mixture (DMPC/DPPG, molar ratio 7:3). The interaction of dendriplexes with LUVs affected both zeta potential and size of the vesicles. The changes of these values were larger for the negatively charged LUV. CBD-CS resulted in the decrease of zeta potential values to more negative ones, whereas an opposite effect took place for CBD-OS suggesting a different kind of interaction between LUVs and the dendriplexes. The results indicate that both CBD-CS and CBD-OS can be used for transport of siRNA into the cells. However, CBD-CS are preferred due to a better stability in water and improved bioavailability of siRNA on their surface.


Molecules | 2013

Phosphorus Dendrimers as Carriers of siRNA—Characterisation of Dendriplexes

Małgorzata Ferenc; Elzbieta Pedziwiatr-Werbicka; Katarzyna E. Nowak; Barbara Klajnert; Jean-Pierre Majoral; Maria Bryszewska

There are many types of dendrimers used as nanomolecules for gene delivery but there is still an ongoing search for ones that are able to effectively deliver drugs to cells. The possibility of gene silencing using siRNA gives hope for effective treatment of numerous diseases. The aim of this work was to investigate in vitro biophysical properties of dendriplexes formed by siRNA and cationic phosphorus dendrimers of 3rd and 4th generation. First, using the ethidium bromide intercalation method, it was examined whether dendrimers have an ability to form complexes with siRNA. Next, the characterisation of dendriplexes formed at different molar ratios was carried out using biophysical methods. The effects of zeta potential, size and changes of siRNA conformation on the complexation with dendrimers were examined. It was found that both phosphorus dendrimers interacted with siRNA. The zeta potential values of dendriplexes ranged from negative to positive and the hydrodynamic diameter depended on the number of dendrimer molecules in the complex. Furthermore, using circular dichroism spectroscopy it was found that cationic phosphorus dendrimers changed only slightly the shape of siRNA CD spectra, thus they did not induce significant changes in the nucleic acid secondary structure during complex formation.


Current Medicinal Chemistry | 2012

Highly Organized Self-Assembled Dendriplexes Based on Poly(propylene imine) Glycodendrimer and Anti-HIV Oligodeoxynucleotides

Jan Maly; Elzbieta Pedziwiatr-Werbicka; Marek Maly; Alena Semeradtova; Dietmar Appelhans; Andrea Danani; Marian Zaborski; Barbara Klajnert; Maria Bryszewska

Dendrimers are artificial polymeric macromolecules which are widely considered to be a promising tool for future gene therapy applications. They have been used as efficient delivery vehicles for antisense oligonucleotides targeting the interior of cells. We demonstrate that dendriplexes formed from anti-HIV oligodeoxynucleotides ANTI-TAR, GEM91, and SREV in complex with generation 4 maltose (PPI-Mal G4) and maltotriose (PPI-Mal-III G4) modified poly(propylene imine) dendrimers are able to self-assemble into highly organized 1D and 3D nanostructures. The resulting nanostructures were characterized by fluorescence methods, laser Doppler electrophoresis, dynamic light scattering (DLS), atomic force microscopy (AFM) and molecular modeling. The results show that ANTI-TAR and GEM 91 dendriplexes self-assemble into fibrils with length scales up to several hundreds of nm. SREV, on the contrary, forms quadrilateral- like 3D nanostructures. A good correlation between the various experimental methods and molecular modeling indicates the formation of those nanostructures in solution. Space symmetry of the oligonucleotides and the resulting dendriplex monomeric units are probably the most important factors which influence the way of self-assembling.


International Journal of Pharmaceutics | 2017

Antibacterial and antifungal properties of dendronized silver and gold nanoparticles with cationic carbosilane dendrons

Cornelia E. Peña-González; Elzbieta Pedziwiatr-Werbicka; Tania Martín-Pérez; Eligia M. Szewczyk; José L. Copa-Patiño; Juan Soliveri; J. Pérez-Serrano; Rafael Gómez; Maria Bryszewska; Javier Sánchez-Nieves; F. Javier de la Mata

Water soluble silver nanoparticles (AgNPs) capped with cationic carbosilane dendrons have been synthesized by direct reaction in water of dendrons, silver precursor and a reducing agent. These nanoparticles have been characterized by nuclear magnetic resonance (NMR), transmission electron microscopy (TEM), dynamic light scattering (DLS), thermogravimetric analysis (TGA), ultraviolet spectroscopy (UV), elemental analysis, and zeta potential (ZP). The antibacterial and antifungal properties of the cationic dendrons and dendronized AgNPs and AuNPs with these dendrons have been evaluated against Gram-negative and Gram-positive bacterial -including resistant strains- and yeast strains, respectively. The results stand out for the activity of AgNPs covered with first generation dendron compared with this free dendron and corresponding dendronized AuNPs.


Colloids and Surfaces B: Biointerfaces | 2017

Dendrimer-protein interactions versus dendrimer-based nanomedicine

Dzmitry Shcharbin; Natallia Shcharbina; Volha Dzmitruk; Elzbieta Pedziwiatr-Werbicka; Maksim Ionov; Serge Mignani; F. Javier de la Mata; Rafael Gómez; María Ángeles Muñoz-Fernández; Jean-Pierre Majoral; Maria Bryszewska

Dendrimers are hyperbranched polymers belonging to the huge class of nanomedical devices. Their wide application in biology and medicine requires understanding of the fundamental mechanisms of their interactions with biological systems. Summarizing, electrostatic force plays the predominant role in dendrimer-protein interactions, especially with charged dendrimers. Other kinds of interactions have been proven, such as H-bonding, van der Waals forces, and even hydrophobic interactions. These interactions depend on the characteristics of both participants: flexibility and surface charge of a dendrimer, rigidity of protein structure and the localization of charged amino acids at its surface. pH and ionic strength of solutions can significantly modulate interactions. Ligands and cofactors attached to a protein can also change dendrimer-protein interactions. Binding of dendrimers to a protein can change its secondary structure, conformation, intramolecular mobility and functional activity. However, this strongly depends on rigidity versus flexibility of a proteins structure. In addition, the potential applications of dendrimers to nanomedicine are reviwed related to dendrimer-protein interactions.


RSC Advances | 2015

Synthesis, characterization and biological properties of new hybrid carbosilane–viologen–phosphorus dendrimers

Silvia Moreno; Aleksandra Szwed; Nabil El Brahmi; Katarzyna Milowska; Joanna Kurowska; Elena Fuentes-Paniagua; Elzbieta Pedziwiatr-Werbicka; Teresa Gabryelak; Nadia Katir; F. Javier de la Mata; Ma Ángeles Muñoz-Fernández; Rafael Gomez-Ramirez; Anne-Marie Caminade; Jean-Pierre Majoral; Maria Bryszewska

A series of hybrid carbosilane–viologen–phosphorus dendrimers was prepared, as a new example of the synthetic “onion peel” approach. This is based on a convergent strategy by combination of double alkylation of 4,4-bipyridine units with two different halogenated reagents, one of them as a carbosilane dendron, and their subsequent ligation to a hexafunctionalized phosphorus core through amine–aldehyde condensation reactions. In these systems two kinds of cationic groups were included: those located at the branches due to viologen quaternized units and those related to the ammonium groups at the surface of carbosilane wedges. This feature constitutes a novel situation to be explored in the search for new physical–chemical and biological properties, respecting traditional dendritic architectures. The biological properties of two of these hybrid molecules have been studied, focusing the investigation on their interactions with plasma proteins like human serum albumin (HSA), cytotoxicity and hemotoxicity experiments. Although the observed biological behaviors were mainly related to the presence of outer positive charges, in some cases the inner positive charges acted as fine tuning factors.


Biochimica et Biophysica Acta | 2014

Interaction of cationic carbosilane dendrimers and their complexes with siRNA with erythrocytes and red blood cell ghosts.

Dominika Wrobel; Katarzyna Kolanowska; Arkadiusz Gajek; Rafael Gomez-Ramirez; Javier de la Mata; Elzbieta Pedziwiatr-Werbicka; Barbara Klajnert; Iveta Waczulíková; Maria Bryszewska

Abstract We have investigated the interactions between cationic NN16 and BDBR0011 carbosilane dendrimers with red blood cells or their cell membranes. The carbosilane dendrimers used possess 16 cationic functional groups. Both the dendrimers are made of water-stable carbon–silicon bonds, but NN16 possesses some oxygen–silicon bonds that are unstable in water. The nucleic acid used in the experiments was targeted against GAG-1 gene from the human immunodeficiency virus, HIV-1. By binding to the outer leaflet of the membrane, carbosilane dendrimers decreased the fluidity of the hydrophilic part of the membrane but increased the fluidity of the hydrophobic interior. They induced hemolysis, but did not change the morphology of the cells. Increasing concentrations of dendrimers induced erythrocyte aggregation. Binding of short interfering ribonucleic acid (siRNA) to a dendrimer molecule decreased the availability of cationic groups and diminished their cytotoxicity. siRNA–dendrimer complexes changed neither the fluidity of biological membranes nor caused cell hemolysis. Addition of dendriplexes to red blood cell suspension induced echinocyte formation.


Chemistry: A European Journal | 2014

Oleochemical‐Tethered SBA‐15‐Type Silicates with Tunable Nanoscopic Order, Carboxylic Surface, and Hydrophobic Framework: Cellular Toxicity, Hemolysis, and Antibacterial Activity

Elzbieta Pedziwiatr-Werbicka; Katarzyna Milowska; Marta Podlas; Monika Marcinkowska; Małgorzata Ferenc; Younes Brahmi; Nadia Katir; Jean-Pierre Majoral; Aleksandra Felczak; Aleksandra Boruszewska; Katarzyna Lisowska; Maria Bryszewska; Abdelkrim El Kadib

Novel silicates were prepared by using silylated natural fatty acids (derived from triglyceride renewable oils) as co-condensing reagents in presence of tetraethyl orthosilicate (TEOS) and the triblock copolymer, pluronic P123, as a structure directing agent. A series of carboxylic acid functionalized SBA-15-type mesoporous silicates were obtained with tunable nanoscopic order and reactive functional groups that allow the conjugation of amino probes by peptide coupling. Photophysical studies of the covalently linked aminopyrene substantiated that the internal framework of these materials have pronounced hydrophobicity. Moreover, phase separation that can emanate from the bulkiness of the starting fatty silanes has been ruled out owing to the absence of excimers after aminopyrene grafting. The hemotoxicity, cytotoxicity, and antimicrobial activity of these novel silicates were then evaluated. Without discrimination, the functionalized silicates show a significant decrease of red blood cell hemolysis as compared to bare SBA-15-silica material. Within the modified silicate series, germanium-free mesoporous silicates induce only a slight decrease in cell viability and, more interestingly, they exhibit negligible hemolytic effect. Moreover, increasing their concentration in the medium reduces the concentration of released hemoglobin as a result of Hb adsorption. Promising antimicrobial properties were also observed for these silicates with a slight dependency on whether phenylgermanium fragments were present within the silicate framework.

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Jean-Pierre Majoral

Centre national de la recherche scientifique

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