A new strategy to achieve easily scalable triple stimuli-responsive elastomeric opal films for applications as stretch-tunable photonic band gap materials is reported. Novel monodisperse highly functional core-interlayer-shell beads are obtained by semicontinuous emulsion polymerization featuring a temperature-sensitive fluorescent rhodamine dye either locally restricted in the core or the shell of prepared beads. After extrusion and compression molding, homogeneous elastomeric opal films with fascinating stretch-tunable and temperature-dependent fluorescent properties can be obtained. Applying strains of only a few percent lead to significant blue shift of the reflected colors making these films excellent candidates for applications as deformation sensors. Higher strains up to 90% lead to a tremendous Bragg reflection color change caused by transition from the (111) to the (200) lattice plane. The well-ordered opaline structure with its stop band at the emission frequency of the incorporated fluorescent dye shows remarkable angle-dependent fluorescence suppression. Herein described elastomeric opal films can be valuable in a wide range of applications such as rewritable 3D optical data storage, tunable laser action, and sensing materials.
Electro-optical scanning (>1,000 frames/s) with pixel dwell times on the order of the lifetime of the fluorescent molecular state renders stimulated emission depletion (STED) nanoscopy temporally stochastic. Photon detection from a molecule occurs stochastically in one of several scanning frames, and the spatial origin of the photon is known with subdiffraction precision. Images are built up by binning consecutive frames, making the time resolution freely adjustable. We demonstrated nanoscopy of vesicle motions in living Drosophila larvae and the cellular uptake of viral particles with 5- to 10-ms temporal resolution.
Cellular ageing can lead to altered cell mechanical properties and is known to affect many fundamental physiological cell functions. To reveal age-dependent changes in cell mechanical properties and in active mechanoresponses, the stiffness of human fibroblasts from differently aged donors was determined, as well as the cell's reaction to periodic mechanical deformation of the culture substrate, and the two parameters were correlated. A comparison of the average Young's moduli revealed that cells from young donors (<25 years) are considerably stiffer than cells from older donors (>30 years). The reduced stiffness of cells from the older donor group corresponds to the measured decrease of actin in these cells. Remarkably, cells from the older donor group show a significantly faster reorganization response to periodic uniaxial tensile strain than cells from the young donor group. The impact of a reduced amount of actin on cell stiffness and cell reorganization kinetics is further confirmed by experiments where the amount of cellular actin in cells from the young donor group was decreased by transient siRNA knockdown of the actin gene. These cells show a reduced stiffness and enhanced reorganization speed, and in this way mimic the properties and behavior of cells from the older donor group. These results demonstrate that mechanical properties of human fibroblasts depend on the donor's age, which in turn may affect the cells' active responses to mechanical stimulations.
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.
hi@scite.ai
334 Leonard St
Brooklyn, NY 11211
Copyright © 2024 scite LLC. All rights reserved.
Made with 💙 for researchers
Part of the Research Solutions Family.