ABSTRACT
Pulsed laser ablation in liquid, used for nanoparticle synthesis from solid bulk metal targets (a top-down approach), has been a hot topic of research in the past few decades. It is a highly efficient and 'green' fabrication method for producing pure, stable, non-toxic (ligand-free), colloidal nanoparticles, which is often challenging using traditional chemical methods. Due to the short time scale interaction between the laser pulses and the target, it is difficult to achieve complete control on the physical characteristics of metallic nanoparticles. Laser process parameters, liquid environment, and external fields vastly effect the shape and structure of nanoparticles for targeted applications. Past reviews on pulsed laser ablation have focused extensively on synthesising different materials using this technique but little attention has been given to explaining the dependency aspect of the process parameters in fine-tuning the nanoparticle characteristics. In this study, we reviewed the state of the art literature available on this technique, which can help the scientific community develop a comprehensive understanding with special insights into the laser ablation mechanism. We further examined the importance of these process parameters in improving the ablation rate and productivity and analysed the morphology, size distribution, and structure of the obtained nanoparticles. Finally, the challenges faced in nanoparticle research and prospects are presented.
ABSTRACT
Aptamers are single-stranded nucleic acids or peptides identified from a randomized combinatorial library through specific interaction with the target of interest. Targets can be of any size, from small molecules to whole cells, attesting to the versatility of aptamers for binding a wide range of targets. Aptamers show drug properties that are analogous to antibodies, with high specificity and affinity to their target molecules. Aptamers can penetrate disease-causing microbial and mammalian cells. Generated aptamers that target surface biomarkers act as cell-targeting agents and intracellular delivery vehicles. Within this context, the "cell-internalizing aptamers" are widely investigated via the process of cell uptake with selective binding during in vivo systematic evolution of ligands by exponential enrichment (SELEX) or by cell-internalization SELEX, which targets cell surface antigens to be receptors. These internalizing aptamers are highly preferable for the localization and functional analyses of multiple targets. In this overview, we discuss the ways by which internalizing aptamers are generated and their successful applications. Furthermore, theranostic approaches featuring cell-internalized aptamers are discussed with the purpose of analyzing and diagnosing disease-causing pathogens.
