Your search keyword '"Saaka Y"' showing total 10 results

1. Book Reviews : Steffen W. Schmidt, Laura Guasti, Carl H. Lande and James C. Scott, (eds.), Friends, Followers and Factions : A Reader in Political Glientelism. Berkeley. Los Angeles, London, University of California Press, 1977, pp. 549, $ 20.00

Author

Saaka, Y., primary

Published

1979

2. Metabolite profiling, antifungal, biofilm formation prevention and disruption of mature biofilm activities of Erythrina senegalensis stem bark extract against Candida albicans and Candida glabrata.

Author

Harley BK, Quagraine AM, Neglo D, Aggrey MO, Orman E, Mireku-Gyimah NA, Amengor CD, Jato J, Saaka Y, and Fleischer TC

Subjects

Candida albicans, Antifungal Agents pharmacology, Fluconazole, Nystatin pharmacology, Plant Bark, Biofilms, Candida, Plant Extracts pharmacology, Candida glabrata, Erythrina

Abstract

The antifungal activity of the 70% ethanol stem bark extract of Erythrina senegalensis (ESB) against different strains and drug resistant clinical isolates of Candida albicans and Candida glabrata were evaluated in the study. The effect of ESB on biofilms as well as its activity in combination with fluconazole, nystatin or caspofungin against the Candida strains were also evaluated. We then evaluated the antifungal activity of a microemulsion formulation of ESB against planktonic and biofilms of the Candida species. UPLC-QTOF-MS2 analysis was then undertaken to identify the phytoconstituents of the extract and UPLC fingerprints developed for the routine authentication as part of quality control measures. ESB exerted strong antifungal activities against C. albicans ATCC 10231 and SC5314 strains, and C. glabrata ATCC 2001 strain with minimum inhibitory concentration (MIC) values from 3.91 to 31.25 μg/mL and minimum fungicidal concentrations (MFCs) that ranged from 62.5 to 250 μg/mL. It also exhibited potent antifungal activities (MIC = 4-64 μg/mL) against a collection of C. albicans and C. glabrata clinical isolates that were resistant to either nystatin or azole antifungals. The formulated ESB demonstrated higher antifungal potency against the C. albicans and C. glabrata strains with MIC values of 3.91-31.25 μg/mL which was the same as the MFC values. The extract and its microemulsion formulation were active against biofilms of the strains of the Candida species inhibiting their biofilm formations (SMIC50 = 16-64 μg/mL) and their preformed biofilms (SMIC50 = 128 ->512 μg/mL). ESB also exhibited synergistic antifungal action with fluconazole and nystatin against C. albicans ATCC 10231 and C. glabrata ATCC 2001 strains in the checkerboard assay. Chemical characterization of the extract revealed the presence of phenolic compounds such as flavonoids and their prenylated derivatives, anthracene glycosides and alkaloids. UPLC Fingerprints of the extract was also developed and validated for routine identification and authentication of the stem bark of E. senegalensis. The study findings have demonstrated that the stem bark of E. senegalensis is as a potential source of bioactive compounds that could be developed as novel antifungal agents., Competing Interests: The authors have declared that no competing interests exist., (Copyright: © 2022 Harley et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.)

Published

2022

3. Assessment of the Availability and Accuracy of Dosing Devices Packaged with Oral Liquid Medications in the Ho Municipality of Ghana.

Author

Saaka Y, Nyamadi DM, Amekyeh H, and Mensah A

Abstract

Introduction: Administering the right dose of medications is essential in avoiding potentially life-threatening adverse drug reactions. Industry guidelines for manufacturers of oral, over-the-counter, and liquid medications recommend including dose-delivery devices with packaging to limit dosing inaccuracy. This study describes the prevalence and accuracy of dosing devices packaged with oral liquid medications in the Ho municipality of Ghana., Methods: Dosing device accuracy was determined after deviation of the measured volume from the expected volume was evaluated using the United States Pharmacopoeia criteria., Results: A total of 78.6% of the oral liquid medications were packaged with a dosing device. The most common dosing devices were cups (83.6%), followed by spoons (14.3%), droppers (1.4%), and syringes (0.7%). The volumes measured with cups (5.14 ± 0.52 mL, p = 0.006) and spoons (5.3 ± 0.67 mL, p < 0.001) were significantly different from the desired 5 mL volume; this was dissimilar to the volume measured using syringes (5.01 ± 0.02 mL, p > 0.999). Further, the measured volumes for 38.6% and 72.2% of the cups and spoons, respectively, deviated by more than 15% of 5 mL., Conclusion: Dosing cups and spoons are associated with significant inaccuracy. Yet, manufacturers continually favour them over syringes in packaging for oral liquid medications. This is unacceptable and of considerable concern due to the risk of variations in therapeutic outcomes. Therefore, strict regulatory directives on the inclusion of accurate dosing devices in the packaging of oral liquid medicines are needed to reduce the possibility of medication errors., Competing Interests: The authors declare that they have no conflicts of interest., (Copyright © 2022 Yussif Saaka et al.)

Published

2022

4. Structure of surfactant and phospholipid monolayers at the air/water interface modeled from neutron reflectivity data.

Author

Campbell RA, Saaka Y, Shao Y, Gerelli Y, Cubitt R, Nazaruk E, Matyszewska D, and Lawrence MJ

Subjects

Air analysis, Models, Chemical, Neutrons, Surface Properties, Thermodynamics, Water chemistry, Phospholipids chemistry, Surface-Active Agents chemistry

Abstract

Specular neutron reflectometry is a powerful technique to resolve interfacial compositions and structures in soft matter. Surprisingly however, even after several decades, a universal modeling approach for the treatment of data of surfactant and phospholipid monolayers at the air/water interface has not yet been established. To address this shortcoming, first a systematic evaluation of the suitability of different models is presented. The result is a comprehensive validation of an optimum model, which is evidently much needed in the field, and which we recommend as a starting point for future data treatment. While its limitations are openly discussed, consequences of failing to take into account various key aspects are critically examined and the systematic errors quantified. On the basis of this physical framework, we go on to show for the first time that neutron reflectometry can be used to quantify directly in situ at the air/water interface the extent of acyl chain compaction of phospholipid monolayers with respect to their phase. The achieved precision of this novel quantification is ∼10%. These advances together enhance significantly the potential for exploitation in future studies data from a broad range of systems including those involving synthetic polymers, proteins, DNA, nanoparticles and drugs., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

5. Towards optimised drug delivery: structure and composition of testosterone enanthate in sodium dodecyl sulfate monolayers.

Author

Saaka Y, Allen DT, Luangwitchajaroen Y, Shao Y, Campbell RA, Lorenz CD, and Lawrence MJ

Subjects

Adsorption, Hydrophobic and Hydrophilic Interactions, Molecular Conformation, Molecular Dynamics Simulation, Surface Tension, Surface-Active Agents chemistry, Testosterone chemistry, Drug Carriers chemistry, Sodium Dodecyl Sulfate chemistry, Testosterone analogs & derivatives

Abstract

Surface tension and specular neutron reflectivity measurements have been used, for the first time to systematically study both the interfacial structure and composition of monolayers of the soluble surfactant, sodium dodecyl sulfate containing a low-dose, poorly water soluble drug, testosterone enanthate. Modelling of the specular neutron reflectivity data suggests that the hydrophobic testosterone enanthate was adsorbed in the C12 hydrophobic tail region of the surfactant monolayer, regardless of the concentration of surfactant at the interface and whether or not additional drug was added to the interface. The location of the hydrophobic drug in the tail region of the surfactant monolayer is supported by the results of classical, large-scale molecular dynamics simulations. The thickness of the surfactant monolayer obtained, in the presence and absence of drug, using molecular dynamics simulations was in good agreement with the corresponding values obtained from the specular neutron reflectivity measurements. The stoichiometry of surfactant:drug at the air-water interface at sodium dodecyl sulfate concentrations above the critical micelle concentration was determined from specular neutron reflectivity measurements to be approximately 3 : 1, and remained constant after the spreading of further testosterone enanthate at the interface. Significantly, this stoichiometry was the same as that obtained in the micelles from bulk solubilisation studies. Important insights into the preferred location of drug in surfactant monolayers at the air-water interface as well as its effect on the structure of the monolayer have been obtained from our combined use of experimental and simulation techniques.

Published

2018

6. Interaction of testosterone-based compounds with dodecyl sulphate monolayers at the air-water interface.

Author

Allen DT, Damestani N, Saaka Y, Lawrence MJ, and Lorenz CD

Abstract

A series of atomistic molecular dynamics simulations were performed for investigating the interactions between three different testosterone-based compounds (testosterone (T), testosterone propionate (TP) and testosterone enanthate (TE)) and sodium dodecyl sulphate (SDS) and ammonium dodecyl sulphate (ADS) monolayers, which vary only in the sodium or ammonium counterions used to neutralise the sulphate headgroup. These simulations were used to investigate how the structural and interfacial properties of the monolayer were affected by changing the number of drug molecules present per monolayer, and the chemical nature of the surfactant counterions and the testosterone-based compounds. Our results show that the structure of the interfacial water layer is affected by the change of the counterion but not the chemistry of the drug molecules. As a result of the difference in their chemical structure, the T, TP and TE drug molecules prefer different locations and orientations within the monolayers. Finally, we observed that the hydration of the drug molecules encapsulated within the ADS monolayers is significantly less than when they are encapsulated within the SDS monolayers. Understanding the role that the counterion and the chemistry of the drug molecules play in these systems provides us with a detailed description of the interactions that cause ADS micelles to encapsulate significantly less drug molecules than SDS micelles, which we have recently observed experimentally.

Published

2018

7. Specific effects of monovalent counterions on the structural and interfacial properties of dodecyl sulfate monolayers.

Author

Allen DT, Saaka Y, Pardo LC, Lawrence MJ, and Lorenz CD

Abstract

A series of molecular dynamics simulations have been conducted in order to study the specific ion effects of Li + , Na + , Cs + and NH 4 + cations on dodecyl sulfate (DS - ) monolayers. Varying the counterion had no appreciable effect on the structure of the surfactant molecules within the different monolayers. However, the different counterions have a significant effect on the interfacial properties of the monolayer. In particular, we have investigated to what extent each of the counterions is dehydrated when interacting with the DS - headgroup, the specific interactions between the counterions and the headgroup and the salt bridging of the headgroups caused by each counterion. The NH 4 + ions are found to directly compete with water molecules to form hydrogen bonds with the DS - headgroup and as a result the ammonium dodecyl sulfate monolayer is the least hydrated of any of those studied. The Cs + ions are strongly bound to the headgroup and weakly hydrated, such that they would prefer to displace water in the DS - hydration shell to interact with the headgroups. In the case of the Li + ions, they interact almost as strongly with the DS - headgroups as the Na + ions, but are generally less hydrated than the Na + ions and consequently the lithium dodecyl sulfate monolayers are less hydrated than the sodium dodecyl sulfate monolayers. Therefore, by changing the counterion, one can modify the interfacial properties of the surfactant monolayer, and thus affect their ability to encapsulate poorly water soluble drug molecules, which we discuss further in the manuscript.

Published

2016

8. Interaction of the Antimicrobial Peptides Rhesus θ-Defensin and Porcine Protegrin-1 with Anionic Phospholipid Monolayers.

Author

Knyght I, Clifton L, Saaka Y, Lawrence MJ, and Barlow DJ

Subjects

Animals, Macaca mulatta, Swine, Antimicrobial Cationic Peptides chemistry, Membranes, Artificial, Models, Molecular, Phospholipids chemistry, alpha-Defensins chemistry

Abstract

A combination of Langmuir isotherm, Brewster angle microscopy (BAM), and neutron reflectivity studies have been performed to gain insight into the effects on model bacterial cell membranes of the antimicrobial peptides, Rhesus θ-defensin 1 (RTD-1), and porcine protegrin 1 (PG-1). The peptides were interacted with monolayers spread at the air-water interface and prepared from a 3:1 molar mixture of phosphatidylethanolamine and phosphatidylglycerol used to approximate the cell membranes of Gram positive bacteria. The Langmuir film balance measurements show that both peptides perturb the lipid monolayers causing an increase in surface pressure, and the BAM studies show that each results in the formation of small domains within the lipid films, around 5 μm diameter. The overall change in monolayer surface pressure caused by PG-1, however, is a little more pronounced than that due to RTD-1 (+8.5 mN·m(-1) vs +5.5 mN·m(-1)), and the rate of its initial interaction with the monolayer is a little more rapid than that for RTD-1. The neutron reflectivity studies also show differences for PG-1 and RTD-1, with the model fits to these data showing that the more amphiphilic PG-1 becomes fully embedded within the lipid film-causing an extension of the lipid acyl chains but leaving the thickness of the lipid headgroup layer unaffected-while RTD-1 is seen to insert less deeply-causing the same extension of the lipid acyl chains as PG-1 but also causing a significant increase in thickness of the lipid headgroup layer. The various differing effects of the two peptides on anionic lipid monolayers are discussed in the context of their differing hemolytic activities, and their proposed differing propensities to form transmembrane pores.

Published

2016

9. Atomistic description of the solubilisation of testosterone propionate in a sodium dodecyl sulfate micelle.

Author

Allen DT, Saaka Y, Lawrence MJ, and Lorenz CD

Subjects

Molecular Dynamics Simulation, Solubility, Surface Properties, Testosterone Propionate metabolism, Micelles, Sodium Dodecyl Sulfate chemistry, Testosterone Propionate chemistry

Abstract

Large-scale molecular dynamics simulations were used to study the structural and dynamic properties of the solubilization process of testosterone propionate (TSTP) within sodium dodecyl sulfate (SDS) micelles. We observed that the TSTP spontaneously adsorb onto the SDS micelles and preferentially reside among the polar head groups of the SDS molecules. We found that the SDS micelle is slightly aspherical in size and has a surface area of ∼170 Å(2)/molecule, while the SDS+TSTP micelle is more aspherical and has a surface area of ∼156 Å(2)/molecule. The structural properties of the interior of the SDS micelle and the hydration of the SDS headgroup are largely undisturbed by the presence of the TSTP. However, there seems to be a correlation between the location of the TSTP molecules and the location of Na(+) counterions on the surface of the SDS micelle. Additionally, we also observe that the TSTP molecules diffuse on the surface of the SDS micelle and try to organize themselves such that they are approximately equidistant from one another.

Published

2014

10. Exploiting thermoresponsive polymers to modulate lipophilicity: interactions with model membranes.

Author

Saaka Y, Deller RC, Rodger A, and Gibson MI

Subjects

Animals, Drug Carriers chemical synthesis, Drug Carriers toxicity, Erythrocytes drug effects, Hemolysis drug effects, Hydrophobic and Hydrophilic Interactions, Light, Membranes, Artificial, Methacrylates chemical synthesis, Methacrylates toxicity, Nanoparticles chemistry, Polyethylene Glycols chemical synthesis, Polyethylene Glycols toxicity, Polymerization, Polymethacrylic Acids, Scattering, Radiation, Sheep, Temperature, Transition Temperature, Drug Carriers chemistry, Methacrylates chemistry, Polyethylene Glycols chemistry

Abstract

Upon heating above their lower critical solution temperature (LCST) poly[oligo(ethyleneglycol)methacrylate]s (POEGMA) were shown to undergo a shift in their partition coefficient triggering aqueous to organic phase transfer, which indicated their potential to partition into cell membranes upon application of an external stimulus. Fluorescence-based assays indicated that the LCST transition did not induce lysis of model phospholipid vesicles but did promote fusion, as confirmed by dynamic light scattering. Membrane perturbation assays and linear dichroism spectroscopy investigations suggest that POEGMAs above their transition temperatures can interact with, or insert into, membranes. These findings will help develop the application of responsive polymers in drug delivery., (Copyright © 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2012