22 research outputs found

    The effect of laser repetition rate on the LASiS synthesis of biocompatible silver nanoparticles in aqueous starch solution.

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    Laser ablation-based nanoparticle synthesis in solution is rapidly becoming popular, particularly for potential biomedical and life science applications. This method promises one pot synthesis and concomitant bio-functionalization, is devoid of toxic chemicals, does not require complicated apparatus, can be combined with natural stabilizers, is directly biocompatible, and has high particle size uniformity. Size control and reduction is generally determined by the laser settings; that the size and size distribution scales with laser fluence is well described. Conversely, the effect of the laser repetition rate on the final nanoparticle product in laser ablation is less well-documented, especially in the presence of stabilizers. Here, the influence of the laser repetition rate during laser ablation synthesis of silver nanoparticles in the presence of starch as a stabilizer was investigated. The increment of the repetition rate does not negatively influence the ablation efficiency, but rather shows increased productivity, causes a red-shift in the plasmon resonance peak of the silver-starch nanoparticles, an increase in mean particle size and size distribution, and a distinct lack of agglomerate formation. Optimal results were achieved at 10 Hz repetition rate, with a mean particle size of ~10 nm and a bandwidth of ~6 nm 'full width at half maximum' (FWHM). Stability measurements showed no significant changes in mean particle size or agglomeration or even flocculation. However, zeta potential measurements showed that optimal double layer charge is achieved at 30 Hz. Consequently, Ag-NP synthesis via the laser ablation synthesis in solution (LASiS) method in starch solution seems to be a trade-off between small size and narrow size distributions and inherent and long-term stability

    Advanced Fluorescence Microscopy Techniques-FRAP, FLIP, FLAP, FRET and FLIM

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    Fluorescence microscopy provides an efficient and unique approach to study fixed and living cells because of its versatility, specificity, and high sensitivity. Fluorescence microscopes can both detect the fluorescence emitted from labeled molecules in biological samples as images or photometric data from which intensities and emission spectra can be deduced. By exploiting the characteristics of fluorescence, various techniques have been developed that enable the visualization and analysis of complex dynamic events in cells, organelles, and sub-organelle components within the biological specimen. The techniques described here are fluorescence recovery after photobleaching (FRAP), the related fluorescence loss in photobleaching (FLIP), fluorescence localization after photobleaching (FLAP), Forster or fluorescence resonance energy transfer (FRET) and the different ways how to measure FRET, such as acceptor bleaching, sensitized emission, polarization anisotropy, and fluorescence lifetime imaging microscopy (FLIM). First, a brief introduction into the mechanisms underlying fluorescence as a physical phenomenon and fluorescence, confocal, and multiphoton microscopy is given. Subsequently, these advanced microscopy techniques are introduced in more detail, with a description of how these techniques are performed, what needs to be considered, and what practical advantages they can bring to cell biological research

    Focus on Extracellular Vesicles: Introducing the Next Small Big Thing

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    Intercellular communication was long thought to be regulated exclusively through direct contact between cells or via release of soluble molecules that transmit the signal by binding to a suitable receptor on the target cell, and/or via uptake into that cell. With the discovery of small secreted vesicular structures that contain complex cargo, both in their lumen and the lipid membrane that surrounds them, a new frontier of signal transduction was discovered. These “extracellular vesicles” (EV) were initially thought to be garbage bags through which the cell ejected its waste. Whilst this is a major function of one type of EV, i.e., apoptotic bodies, many EVs have intricate functions in intercellular communication and compound exchange; although their physiological roles are still ill-defined. Additionally, it is now becoming increasingly clear that EVs mediate disease progression and therefore studying EVs has ignited significant interests among researchers from various fields of life sciences. Consequently, the research effort into the pathogenic roles of EVs is significantly higher even though their protective roles are not well established. The “Focus on extracellular vesicles” series of reviews highlights the current state of the art regarding various topics in EV research, whilst this review serves as an introductory overview of EVs, their biogenesis and molecular composition

    Focus on Extracellular Vesicles: Development of Extracellular Vesicle-Based Therapeutic Systems

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    Many types of cells release phospholipid membrane vesicles thought to play key roles in cell-cell communication, antigen presentation, and the spread of infectious agents. Extracellular vesicles (EVs) carry various proteins, messenger RNAs (mRNAs), and microRNAs (miRNAs), like a “message in a bottle” to cells in remote locations. The encapsulated molecules are protected from multiple types of degradative enzymes in body fluids, making EVs ideal for delivering drugs. This review presents an overview of the potential roles of EVs as natural drugs and novel drug-delivery systems

    The Controversial Role of Retinoic Acid in Fibrotic Diseases: Analysis of Involved Signaling Pathways

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    Fibrotic diseases, such as liver, pulmonary and renal fibrosis, are common end-stage conditions and represent a major global health problem. Furthermore, effective therapeutic measures are presently unavailable. Extracellular matrix accumulation is the most prominent characteristic in the pathogenesis of fibrotic disease. Retinoic acid, including all-trans retinoic acid, 9-cis and 13-cis retinoic acid, play important roles in various physiological processes, such as in embryonic development, reproduction, vision, cell growth, differentiation, apoptosis and inflammation. Present studies report that retinoic acid treatment may affect various processes involved in the onset and progression of fibrotic disease. However, the therapeutic effects of retinoic acid in such diseases remain controversial. Several reports indicate that retinoic acid positively affects the progression of fibrosis and alleviates the accumulation of the extracellular matrix, whereas other studies report the opposite; that retinoic acid exacerbates fibrosis and induces extracellular matrix accumulation. Signaling pathways might be an important influencing factor and differences in signaling events might be responsible for the contradictory role of retinoic acid in fibrotic diseases. Since there was no review available that investigated the role of retinoic acid and the signaling pathways involved, we retrospectively studied the literature and provide a comprehensive analysis of retinoic acid’s role in fibrotic diseases, and provide an overview of the signal transduction pathways involved in its pathogenesis

    Laser-Ablation Synthesis and Evaluation of Thermal Non-Linear Optical Properties of Silver Nanoparticles in Monoolein

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    Silver nanoparticles were prepared in monoolein, a glycerol derivative of oleic acid, via pulsed laser ablation of a silver plate with a Q-Switched Nd:YAG laser (1064 nm). The average size of the nanoparticles was 8.8 +/- 0.5 nm, with a narrow size distribution of 4.6 nm FWHM. No significant agglomeration or flocculation was observed after one-month storage. The observed results indicated a nonlinear dependence of the refractive index n(2) on the particle volume fraction. Furthermore, the monoolein-silver nanoparticle solution showed self-defocusing behaviour, as deduced from the negative sign in n(2) and spatial self-phase modulation, which depended on the volume fraction. Non-linear absorption behaviour was not observed in any of the samples analyzed. The results in this work suggest that colloidal silver nanoparticle solutions in monoolein are interesting nonlinear materials to create and control different spatial effects and that such silver-monoolein colloids might be used in a multitude of optical applications, such as spatial soliton propagation, real time holography, and liquid crystal-based applications

    Hydrothermal synthesis of goethite (alpha-FeOOH) nanorods in the presence of ethylenediamine:thiourea

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    Goethite (alpha-FeOOH) nanorods were synthesized via the hydrothermal method with the assistance of coordinating ligands, i.e. ethylenediamine and thiourea. The homogeneity of the nanorod size distribution increased and the propensity to agglomerate decreased when ethylenediamine and thiourea were used in conjunction; contrary to goethite synthesis in the presence of a single ligand. The type and mode of structure-directing plays a critical role in the morphology of the final products. When using thiourea only or in combination with ethylenediamine, nanorods and nanoparticles of various morphologies were formed. Conversely, when exclusively using ethylenediamine, in addition to the nanorods, fine needles with a significantly smaller diameter were discernible. With all combinations, structurally uniform alpha-FeOOH nanorods were formed. This improved nanorod formation in the presence of both ligands might be attributed to a more ordered alignment and regular conformation of ethylenediamine molecules in the presence of thiourea and thus less susceptibility to thermal perturbations. Finally, higher concentrations of ligand influence the final product and increases particle aggregation
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