MiR-219a-5p Enriched Extracellular Vesicles Induce OPC Differentiation and EAE Improvement More Efficiently Than Liposomes and Polymeric Nanoparticles

Remyelination is a key aspect in multiple sclerosis pathology and a special effort is being made to promote it. However, there is still no available treatment to regenerate myelin and several strategies are being scrutinized. Myelination is naturally performed by oligodendrocytes and microRNAs have been postulated as a promising tool to induce oligodendrocyte precursor cell differentiation and therefore remyelination. Herein, DSPC liposomes and PLGA nanoparticles were studied for miR-219a-5p encapsulation, release and remyelination promotion. In parallel, they were compared with biologically engineered extracellular vesicles overexpressing miR-219a-5p. Interestingly, extracellular vesicles showed the highest oligodendrocyte precursor cell differentiation levels and were more effective than liposomes and polymeric nanoparticles crossing the blood–brain barrier. Finally, extracellular vesicles were able to improve EAE animal model clinical evolution. Our results indicate that the use of extracellular vesicles as miR-219a-5p delivery system can be a feasible and promising strategy to induce remyelination in multiple sclerosis patients.This work was supported by Carlos III Institute, (PI17/00189 and DTS15/00069), by Fondo Europeo de Desarrollo Regional—FEDER, by the Gipuzkoa Regional Council (DFG 15/006), by grant from the Basque Government (RIS3/DTS/2018222025), by the Department of Industry of the Basque Country (ELKARTEK 16/014), and the Spanish State Research Agency (SAF2017-87670-R) and Maria de Maeztu Units of Excellence Program Grant MDM-2017-0720). I.O.-Q., A.A. and L.I. were supported by the Department of Education of the Basque Government. IOQ and LAN were supported by EMBO short Term Fellowship Programme. LAN was supported by a Canadian graduate scholarship from the Canadian Institutes of Health Research (CGS-D CIHR).PRC was supported by Ikerbasque, the Basque Foundation for Science

High-throughput roll-to-roll production of polymer biochips for multiplexed DNA detection in point-of-care diagnostics

Roll-to-roll UV nanoimprint lithography has superior advantages for high-throughput manufacturing of micro- or nano-structures on flexible polymer foils with various geometries and configurations. Our pilot line provides large-scale structure imprinting for cost-effective polymer biochips (4500 biochips/hour), enabling rapid and multiplexed detections. A complete high-volume process chain of the technology for producing structures like μ-sized, triangular optical out-couplers or capillary channels (width: from 1 μm to 2 mm, height: from 200 nm up to 100 μm) to obtain biochips (width: 25 mm, length: 75 mm, height: 100 μm to 1.5 mm) was described. The imprinting process was performed with custom-developed resins on polymer foils with resin thicknesses ranging between 125–190 μm. The produced chips were tested in a commercial point-of-care diagnostic system for multiplexed DNA analysis of methicillin resistant Staphylococcus aureus (e.g., mecA, mecC gene detections). Specific target DNA capturing was based on hybridisation between surface bound DNA probes and biotinylated targets from the sample. The immobilised biotinylated targets subsequently bind streptavidin–horseradish peroxidase conjugates, which in turn generate light upon incubation with a chemiluminescent substrate. To enhance the light out-coupling thus to improve the system performance, optical structures were integrated into the design. The limits-of-detection of mecA (25 bp) for chips with and without structures were calculated as 0.06 and 0.07 μM, respectively. Further, foil-based chips with fluidic channels were DNA functionalised in our roll-to-roll micro-array spotter following the imprinting. This straightforward approach of sequential imprinting and multiplexed DNA functionalisation on a single foil was also realised for the first time. The corresponding foil-based chips were able to detect mecA gene DNA sequences down to a 0.25 μM concentration.This research was supported by R2R BIOFLUIDICS project (http://www.r2r-biofluidics.eu/) under Horizon 2020 European Union (EU) Research and Innovation Programme with grant agreement no 646260. The research was also partially supported by NextGenMicrofluidics project (https:// www. nextgenmicrofluidics.eu/) under HORIZON2020 with grant agreement no 862092. The authors cordially thank Gerburg Schider & Gerhard Mohr, Markus Postl, Paul Patter and Alexander Wheeldon (JOANNEUM RESEARCH – Materials, Weiz, Austria) for revising the manuscript, preparing all the chip and R2R pilot line illustrations, taking the photographs and providing technical support, respectively. The authors are also grateful to Christian Wolf and Johannes Götz (JOANNEUM RESEARCH – Materials, Weiz, Austria) for their supports in the fluidic design and R2R UV-NIL structuring, respectively. We further kindly thank Alba Simon Munoz and Robert Fay (SCIENION AG, Berlin, Germany) for providing the illustration of the R2R micro-spotting line. PT specially thanks Ege Ozgun (NANOTAM, Bilkent University, Ankara, Turkey) for critically reading the manuscript

Treating drop-foot in hemiplegics: the role of matrix electrode

International audienceWe present advantages of the “intelligent matrix electrode” for providing selective correction of drop-foot in hemiplegic individuals. The matrix electrode which integrates stimulating and sensing parts could allow the emulation of the appropriate electrode shape and size; thereby, provision of selective stimulation that leads to functional movement and online adaptation of the electrode during the application. The need for selective stimulation follows recent findings about therapeutic effects of electrical stimulation in neurorehabilita-tion. The matrix electrode comprises small fields that can be made conductive and a controller that allows computerized selection of the fields being conductive. Here we present results from a study in nine hemiplegics. The matrix electrode was positioned over the peroneal nerve and primary dorsiflexor muscles and we estimated the movement of the foot by measur-ing the ankle joint angle. We found that the branched tree type shape and size of the electrode vary substantially when stimulating over the dorsiflexor muscles individuals in the study. We confirmed very high sensitivity to the position of small electrode when stimulating over the nerve. This indicates that the use of “intelligent matrix electrode” is favorable compared with conventional electrodes since it can adapt to individual and secure selective stimulation

Adsorption characteristics of stoichiometric and nonstoichiometric molecular polyelectrolyte complexes on silicon oxynitride surfaces

Adsorption properties of stoichiometric and nonstoichiometric polyelectrolyte complexes (PECs) have been investigated by means of dual polarization interferometry (DPI) and X-ray photoelectron spectroscopy (XPS). Poly(sodium styrenesulfonate) (NaPSS) of molecular weight 4300 g/mol was used as polyanion, and two bottle-brush copolymers possessing different molar ratios of the cationic segment methacryloxyethyltrimethylammonium chloride (METAC) and the nonionic segment poly(ethylene oxide) methyl ether methacrylate (PEO45MEMA) were used as polycations. They are referred to as PEO45MEMA:METAC-25 and PEO45MEMA:METAC-50, where the last digits denote the mol%of charged main-chain segments. The time evolution of the adsorbed amount, thickness, and refractive index of the PEC layers were determined in aqueous solution using DPI. We demonstrate that cationic, uncharged, and negatively charged complexes adsorb to negatively charged silicon oxynitride and that maximum adsorption is achieved when small amounts of PSS are present in the complexes. The surface composition of the adsorbed PEC layers was estimated from XPS measurements that demonstrated very low content of NaPSS. On the basis of these data, the PEC adsorption mechanism is discussed and the competition between PSS and negative surface sites for association with the cationic polyelectrolyte is identified as a key issue