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Electronic devicesforrecording neuralactivityinthe nervoussyste m needto bescalableacrosslargespatialandte mporalscales whilealso providing millisecondandsingle-cellspatiote mporalresolution. H o w e v e r, e xi s ti n g hi g h- r e s ol u ti o n n e u r al r e c o r di n g d e vi c e s c a n n o t achievesi multaneousscalability on bothspatialandte mporallevels due toatrade-offbetweensensordensityand mechanicalflexibility. Here weintroduceathree-di mensional(3D)stackingi mplantableelectronic platfor m,basedonperfluorinateddielectricelasto mersandtissue-levelsoft multilayerelectrodes,thatenablesspatiote mporallyscalablesingle-cell neuralelectrophysiologyinthenervoussyste m. Ourelasto mersexhibit stable dielectric perfor mancefor overayearin physiologicalsolutions andare10,000ti messofterthanconventional plastic dielectrics. By leveragingthese uniquecharacteristics we developthe packaging of lithographednano metre-thickelectrodearraysina3Dconfiguration with across-sectionaldensityof7.6electrodesper100μ m2.Theresulting3D integrated multilayersoftelectrodearrayretainstissue-levelflexibility, reducingchronici m muneresponsesin mouse neuraltissues,and de monstratestheabilitytoreliablytrackelectricalactivityinthe mouse brain orspinalcord over months without disruptingani mal behaviour. 

Abstract Accurately replicating and analyzing cellular responses to mechanical cues is vital for exploring metastatic disease progression. However, many of the existing in vitro platforms for applying mechanical stimulation seed cells on synthetic substrates. To better recapitulate physiological conditions, a novel actuating platform is developed with the ability to apply tensile strain on cells at various amplitudes and frequencies in a high‐throughput multi‐well culture plate using a physiologically relevant substrate. Suspending fibrillar fibronectin across the body of the magnetic actuator provides a matrix representative of early metastasis for 3D cell culture that is not reliant on a synthetic substrate. This platform enables the culturing and analysis of various cell types in an environment that mimics the dynamic stretching of lung tissue during normal respiration. Metabolic activity, YAP activation, and morphology of breast cancer cells are analyzed within one week of cyclic stretching or static culture. Further, matrix degradation is significantly reduced in breast cancer cell lines with metastatic potential after actuation. These new findings demonstrate a clear suppressive cellular response due to cyclic stretching that has implications for a mechanical role in the dormancy and reactivation of disseminated breast cancer cells to macrometastases.