Here we investigated the electrochemical properties and dopamine (DA) detection capability of SU-8 photoresist based pyrolytic carbon (PyC) as well as its biocompatibility with neural cells.
In
the current study, platinum—present as a negligible component
(below 1 ppb, the detection limit of the HR-ICP-MS at the dilutions
used) in real industrial hydrometallurgical process solutions—was
recovered by an electrodeposition–redox replacement (EDRR)
method on pyrolyzed carbon (PyC) electrode, a method not earlier applied
to metal recovery. The recovery parameters of the EDRR process were
initially investigated using a synthetic nickel electrolyte solution
([Ni] = 60 g/L, [Ag] = 10 ppm, [Pt] = 20 ppm, [H2SO4] = 10 g/L), and the results demonstrated an extraordinary
increase of 3 × 105 in the [Pt]/[Ni] on the electrode
surface cf. synthetic solution. EDRR recovery of platinum on PyC was
also tested with two real industrial process solutions that contained
a complex multimetal solution matrix: Ni as the major component (>140
g/L) and very low contents of Pt, Pd, and Ag (i.e., <1 ppb, 117
and 4 ppb, respectively). The selectivity of Pt recovery by EDRR on
the PyC electrode was found to be significant—nanoparticles
deposited on the electrode surface comprised on average of 90 wt %
platinum and a [Pt]/[Ni] enrichment ratio of 1011 compared
to the industrial hydrometallurgical solution. Furthermore, other
precious metallic elements like Pd and Ag could also be enriched on
the PyC electrode surface using the same methodology. This paper demonstrates
a remarkable advancement in the recovery of trace amounts of platinum
from real industrial solutions that are not currently considered as
a source of Pt metal.
Kainate type of glutamate receptors (KARs) are highly expressed during early brain development and may influence refinement of the circuitry, via modulating synaptic transmission and plasticity. KARs are also localized to axons, however, their exact roles in regulating presynaptic processes remain controversial. Here, we have used a microfluidic chamber system allowing specific manipulation of KARs in presynaptic neurons to study their functions in synaptic development and function in vitro. Silencing expression of endogenous KARs resulted in lower density of synaptophysin immunopositive puncta in microfluidically isolated axons. Various recombinant KAR subunits and pharmacological compounds were used to dissect the mechanisms behind this effect. The calcium permeable (Q) variants of the low-affinity (GluK1–3) subunits robustly increased synaptophysin puncta in axons in a manner that was dependent on receptor activity and PKA and PKC dependent signaling. Further, an associated increase in the mean active zone length was observed in electron micrographs. Selective presynaptic expression of these subunits resulted in higher success rate of evoked EPSCs consistent with higher probability of glutamate release. In contrast, the calcium-impermeable (R) variant of GluK1 or the high-affinity subunits (GluK4,5) had no effect on synaptic density or transmission efficacy. These data suggest that calcium permeable axonal KARs promote efferent connectivity by increasing the density of functional presynaptic release sites.
Biofouling imposes a significant threat for sensing probes used in vivo. Antifouling strategies commonly utilize a protective layer on top the electrode but this may compromise performance of the electrode....
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