The 18kDa Translocator Protein (TSPO) is the most commonly used tissue-specific marker of inflammation in positron emission tomography (PET) studies. It is expressed in myeloid cells such as microglia and macrophages, and in rodent myeloid cells expression increases with cellular activation. We assessed the effect of myeloid cell activation on TSPO gene expression in both primary human and rodent microglia and macrophages in vitro, and also measured TSPO radioligand binding with 3H-PBR28 in primary human macrophages. As observed previously, we found that TSPO expression increases (∼9-fold) in rodent-derived macrophages and microglia upon pro-inflammatory stimulation. However, TSPO expression does not increase with classical pro-inflammatory activation in primary human microglia (fold change 0.85 [95% CI 0.58–1.12], p = 0.47). In contrast, pro-inflammatory activation of human monocyte-derived macrophages is associated with a reduction of both TSPO gene expression (fold change 0.60 [95% CI 0.45–0.74], p = 0.02) and TSPO binding site abundance (fold change 0.61 [95% CI 0.49–0.73], p < 0.0001). These findings have important implications for understanding the biology of TSPO in activated macrophages and microglia in humans. They are also clinically relevant for the interpretation of PET studies using TSPO targeting radioligands, as they suggest changes in TSPO expression may reflect microglial and macrophage density rather than activation phenotype.
The reaction of gold substrates with p-nitrobenzene diazonium tetrafluoroborate (NBD) in 0.1 M H(2)SO(4) at open-circuit potential (OCP) is demonstrated to proceed by electron transfer from gold to the NBD cation. Electrochemical, atomic force microscopy, and X-ray photoelectron spectroscopy analyses reveal the formation of multilayer films with the same composition as electrografted films. The film growth characteristics (surface concentration and film thickness vs time) also follow those observed during electrografting, consistent with electron transfer from the substrate to the diazonium cation. The OCP of the gold substrate increases during the period of film growth ( approximately 60 min) and then decreases to close to its initial value. The increase corresponds to accumulation of positive charge as electrons are transferred to NBD; the discharge process is tentatively attributed to slow oxidation of adventitious impurities in the reaction solution. Films formed at OCP or by electrografting from aqueous acid solution are markedly less stable to sonication in acetonitrile than are those electrografted from acetonitrile. Increased amounts of physisorbed material in films prepared in aqueous media or bonding of aryl groups to different gold sites in the two media are tentatively proposed to account for the different stabilities.
The covalent grafting of nitrophenyl functionalities to planar carbon substrates by reaction with 4-nitrobenezene diazonium salt at open circuit potential has been studied in aqueous acid and acetonitrile solutions. Atomic force microscopy and electrochemical measurements reveal that the reaction proceeds through two distinct mechanisms. Rapid film growth occurs via reduction of the 4-nitrobenezene diazonium cation by the substrate, giving an aryl radical that couples to the surface. Film growth by this mechanism ceases once the film has reached a thickness at which electron transfer through the passivating film is no longer possible. Slow film growth via a secondary, potential-independent mechanism continues even after the substrate-dependent reaction has ceased. We tentatively propose that slow film growth involves grafting of an aryl cation originating from thermal heterolytic decomposition of the diazonium cation.
An electrode surface confined redox group contributes to a substantial potential-dependent interfacial charging that can be sensitively probed and frequency-resolved by impedance-derived capacitance spectroscopy. In utilizing the sensitivity of this charging fingerprint to redox group environment, one can seek to generate derived sensory configurations. Exemplified here through the generation of mixed molecular films comprising ferrocene and antibody receptors to two clinically important targets, the label-free methodology is able to report on human prostatic acid phosphatase (PAP), a tumor marker, with a limit of detection of 11 pM and C-reactive protein with a limit of detection of 28 pM. Both assays exhibit linear ranges encompassing those of clinical value.
We have previously proposed, and experimentally resolved, an ionic charge relaxation model for redox inactive self-assembled monolayers (SAMs) on metallic electrodes in contact with a liquid electrolyte. Here we analyse, by capacitance spectroscopy, the resistance and capacitance terms presented by a range of thiolated molecular films. Molecular dynamics simulations support a SAM-specific energy barrier to solution-phase ions. Once surmounted, the entrapped ions support a film embedded ionic capacitance and non-faradaic relaxation, which can be assigned as a particular case of general electrochemical capacitance.
Surface modification through reduction of aryldiazonium salts to give covalently attached layers is a widely investigated procedure. However, realization of potential applications of the layers requires development of patterning methods. Here, we demonstrate that microcontact printing with poly(dimethylsiloxane) stamps inked with aqueous acid solutions of aryldiazonium salts gives stable organic layers on gold, copper, silicon, and graphitic carbon surfaces. Depending on the substrate-diazonium salt combination, the layers range from relatively irregular multilayers to smooth films with close to monolayer thickness. After printing, surface attached aminophenyl and carboxyphenyl groups retain their usual reactivity toward amide bond formation with solution species, and hence, the method is a simple route to patterned, covalently attached, reactive tether layers. Multicomponent patterned films can be prepared by printing a second modifier onto a film-coated surface. Microcontact printing using aryldiazonium salt inks is experimentally very simple and is applicable to the broad range of substrates capable of spontaneously reducing aryldiazonium salts.
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