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Dive into the research topics where Svitlana Silchenko is active.

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Featured researches published by Svitlana Silchenko.


CrystEngComm | 2013

Synthesis, spectroscopic and structural characterization of the first phenyl bis-cyanoximes: non-chelating extended ionisable building block ligands for new MOFs

Scott Curtis; Olesya T. Ilkun; Amy Brown; Svitlana Silchenko; Nikolay Gerasimchuk

Two new isomeric bis-cyanoximes were synthesized and characterized by a variety of spectroscopic methods including UV-visible, infrared, NMR, pKa measurements and X-ray analysis. These synthesized compounds represent the first non-chelating bis-cyanoximes that can function as building blocks for new MOF-like structures.


Journal of Pharmaceutical Sciences | 2013

Evaluation of a Nanoemulsion Formulation Strategy for Oral Bioavailability Enhancement of Danazol in Rats and Dogs

Harikrishna Devalapally; Svitlana Silchenko; Feng Zhou; Jessica McDade; Galina Goloverda; Albert Owen; Ismael J. Hidalgo

The objective of this study was to determine whether nanoemulsion formulations constitute a viable strategy to improve the oral bioavailability of danazol, a compound whose poor aqueous solubility limits its oral bioavailability. Danazol-containing oil-in-water nanoemulsions (NE) with and without cosurfactants stearylamine (SA) and deoxycholic acid (DCA) were prepared and characterized. Nanoemulsion droplets size ranging from 238 to 344 nm and with surface charges of -24.8 mV (NE), -26.5 mV (NE-DCA), and +27.8 mV (NE-SA) were reproducibly obtained. Oral bioavailability of danazol in nanoemulsions was compared with other vehicles such as PEG400, 1% methylcellulose (MC) in water (1% MC), Labrafil, and a Labrafil/Tween 80 (9:1) mixture, after intragastric administration to rats and after oral administration of NE-SA, a Labrafil solution, or a Danocrine® tablet to dogs. The absolute bioavailability of danazol was 0.6% (PEG400), 1.2% (1% MC), 6.0% (Labrafil), 7.5% (Labrafil/Tween80), 8.1% (NE-DCA), 14.8% (NE), and 17.4% (NE-SA) in rats, and 0.24% (Danocrine), 6.2% (Labrafil), and 58.7% (NE-SA) in dogs. Overall, danazol bioavailability in any nanoemulsion was higher than any other formulation. Danazol bioavailability from NE and NE-SA was 1.8- to 2.2-fold higher than NE-DCA nanoemulsion and could be due to significant difference in droplet size.


Drug Delivery | 2015

Optimization of PEGylated nanoemulsions for improved pharmacokinetics of BCS class II compounds.

Harikrishna Devalapally; Feng Zhou; Jessica McDade; Galina Goloverda; Albert Owen; Ismael J. Hidalgo; Svitlana Silchenko

Abstract The objective of the study was the optimization of nanoemulsion formulations to prevent their rapid systemic clearance after intravenous administration. An amphiphilic PEG derivative DSPE-PEG (1,2-distearoyl-sn-glycero-3-phosphoethanolamine-N-methoxy-poly(polyethylene glycol) with different chain lengths and concentration was used as a nanoemulsion droplet surface modifier. The danazol loading in all nanoemulsions was kept on the same level of ∼2 mg/mL. In the present investigation, PEGylated and non-PEGylated nanoemulsions were compared in vitro phagocytosis by incubating with lung macrophages and in vivo after intravenous administration in rats. Danazol-containing nanoemulsions (NE) modified with various PEG chain lengths (2000–10 000) and concentrations (3–12 mg/mL) were prepared and characterized. Nanoemulsion droplets were reproducibly obtained in the size range of 213–340 nm. The non-PEGylated NE had the surface charge of −25.4 mV. This absolute charge value decreased with increasing chain length and concentration. With increase in chain length and density the macrophage uptake decreased which could be due to decrease in surface charge and hydrophilicity of droplets. The greatest shielding of the NE droplets was reached with DSPE-PEG5000 at the concentration of 6 mg/mL where the surface charge changed to −1.27 mV. Following intravenous administration a maximum danazol exposure (401 ± 68.2 h ng/mL) was observed with the lowest clearance rate (5.06 ± 0.95 L/h/kg) from 6 mg/mL DSPE-PEG5000 nanoemulsion. PEG5000 and PEG10000 altered the pharmacokinetic of danazol by decreasing clearance and volume of distribution which is likely explained by the presence of hydrophilic shields around the droplets that prevent their rapid systemic clearance and tissue partitioning.


Dalton Transactions | 2013

The first bis-cyanoxime: synthesis and properties of a new versatile and accessible polydentate bifunctional building block for coordination and supramolecular chemistry

Carl Cheadle; Nikolay Gerasimchuk; Charles L. Barnes; Sergiy Tyukhtenko; Svitlana Silchenko

A new multidentate bifunctional organic ligand – di-N,N′-(2-cyano-2-oximinoacetyl)piperazine – was synthesized in high yield using a two-step procedure carried out under ambient conditions. At first, the reaction of piperazine and neat methylcyanoacetate led to the di-N,N′-(cyanoacetyl)piperazine (1), which then was converted into bis-cyanoxime, di-N,N′-(2-cyano-2-oximinoacetyl)piperazine (HL, 2) using a room temperature nitrosation reaction with gaseous methylnitrite. Synthesized bis-cyanoxime was characterized by 1H, 13C NMR, UV-visible, IR spectroscopy and the X-ray analysis. The ligand 2 exists as a mixture of three diastereomers arising from the syn- and anti-geometry of the cyanoxime group. The prolonged crystallization of 2 from an ethanol–water mixture leads to the formation of: (a) colorless crystals that according to the X-ray analysis contain a 51.2:48.8% co-crystallized mixture of both isomers that have the same H-bonding motif (minority), and (b) a white amorphous material that represents an almost pure anti-isomer (majority). The deprotonation of 2 leads to the formation of a yellow dianion that demonstrated pronounced solvatochromism of its n → π* transition in the nitroso-chromophore. The disodium salt Na2L·4H2O (3) was obtained from 2 using NaOC2H5 in ethanol. The new bis-cyanoxime 2 reacts with Tl2CO3 and AgNO3 in aqueous solutions with the formation of light-stable, sparingly soluble yellow precipitates of M′2L·xH2O composition (M′ = Tl, Ag; Tl = 4, x = 0; Ag = 5, x = 2). The reaction of 3 with Ni2+ or K2M′′Cl4 (M′′ = Pd, Pt) in aqueous solutions leads to NiL·4H2O (6), PdL·4H2O (7) and PtL·5H2O (8). The crystal structure of 4 was determined and revealed the formation of a 3D-coordination polymeric complex in which the bis-cyanoxime acts as a dianionic, bridging, formally decadentate ligand. Each Tl(I) center has two bonds (2.655, 2.769 Å), shorter than the sum of ionic radii Tl–O (oxime group), and three longer, >2.89 Å, mostly electrostatic Tl···O contacts, involving oxygen atoms of the amide-group and the oxime-group of neighboring units. Among several possible binding modes, the coordination of the bis-cyanoxime dianion of 2 adopted in complex 4 is unusual, and evidenced its great potential as a versatile building block for coordination and supramolecular chemistry.


Inorganic Chemistry | 2015

1D polymeric platinum cyanoximate: a strategy toward luminescence in the near-infrared region beyond 1000 nm.

Danielle R. Klaus; Matthew Keene; Svitlana Silchenko; Mikhail Y. Berezin; Nikolay Gerasimchuk


Inorganica Chimica Acta | 2008

Synthesis and characterization of disubstituted arylcyanoximes and their several metal complexes

Nikolay Gerasimchuk; Leon Goeden; Paul L. Durham; Charles L. Barnes; John F. Cannon; Svitlana Silchenko; Ismael J. Hidalgo


Crystal Growth & Design | 2012

Synthesis, Characterization, and Studies of Coordination-Polymeres With Isomeric Pyridylcyanoximes: Route to Metal Ribbons With Very Short Tl···Tl Separations

Daniela Marcano; Nikolay Gerasimchuk; Victor N. Nemykin; Svitlana Silchenko


Dalton Transactions | 2008

Benz(2-heteroaryl)cyanoximes and their Tl(I) complexes: new room temperature blue emitters

Olesya T. Ilkun; Stephen J. Archibald; Charles L. Barnes; Nikolay Gerasimchuk; Richard N. Biagioni; Svitlana Silchenko; Olga A. Gerasimchuk; Victor N. Nemykin


Inorganica Chimica Acta | 2014

Synthesis and characterization of two cyanoxime ligands, their precursors, and light insensitive antimicrobial silver(I) cyanoximates

Courtney N. Riddles; Mark Whited; Shalaka R. Lotlikar; Korey Still; Marianna A. Patrauchan; Svitlana Silchenko; Nikolay Gerasimchuk


Inorganica Chimica Acta | 2016

New non-aggregating bivalent cis -ML 2 (M=Pd, Pt; L=pivaloylcyanoxime)

Alexandra Mann; Nikolay Gerasimchuk; Svitlana Silchenko

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Olesya T. Ilkun

Missouri State University

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Alexandra Mann

Missouri State University

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Amy Brown

Missouri State University

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