Electrochemical detection of trace silver

Increasing utilization of silver and silver nanoparticles (AgNPs) in daily processes and products has led to a significant growth in scientific interest in methods for monitoring silver. In particular, the amount of silver ions (Ag+) released to the environment is known to have a detrimental effect on aquatic ecology, and thus some control actions have been implemented in recent years; for example, the manufacturing industry is now required to control and certify the quantity of AgNPs present in products. Electrochemical sensors are well suited to the task of silver monitoring due to several beneficial properties, including low costs, fast measurements, and facile adaptation to miniaturized, portable instrumentation. The predominant method for electrochemical silver determination involves potentiometric ion selective electrodes (ISEs) and voltammetric measurements. Reviewing the literature of the last ten years reveals significant improvements in the analytical performance of electrochemical sensors, mainly related to the development of new protocols, selective receptors, and electrode materials. Remarkably, ISEs with limits of detection (LOD) in the nanomolar range have been reported, employing careful control of ion fluxes across the membrane interfaces. What's more, sub-nanomolar LODs are attainable by stripping voltammetry using either ligand-based deposition strategies or thin layer membranes coupled to conducting polymers. Selectivity has also been optimized through the membrane composition of ISEs, with special focus on Ag+ ionophores. Furthermore, novel voltammetric methods allow for discrimination between Ag+ and AgNPs. However, there is still a dearth of studies applying such electrochemical sensors to on-site water analysis, and hence, further research is needed in order to translate these laboratory scale achievements to real-world contexts. Overall, this review describes the state-of-the-art in electrochemical silver detection, and provides a comprehensive description of those aspects contributing to the further development and improvement of analytical performance

Microneedle based electrochemical (bio)sensing: towards decentralized and continuous health status monitoring

Microneedle (MN) based electrochemical (bio)sensing has become a growing field within the discipline of analytical chemistry as a result of its unique capacity for continuous, decentralized health status monitoring. There are two significant advantages to this exclusive feature: i) the ability to directly analyze interstitial fluid (ISF), a body fluid with a similar enough composition to plasma (and blood) to be considered a plentiful source of information related to biologically relevant molecules and biomarkers; and ii) the capacity to overcome some of the major limitations of blood analysis including painful extraction, high interferant concentrations, and incompatibility with diagnosis of infants (and especially newborns). Recent publications have demonstrated important advancements in electrochemical MN sensor technology, among which are included new MN fabrication methods and various modification strategies, providing different architectures and allowing for the integration of electronics. This versatility highlights the undeniable need for interdisciplinary efforts towards tangible progress in the field. In a context evidently dominated by glucose sensing, which is slowly being expanded towards other analytes, the following crucial questions arise: to what extent are electrochemical MN (bio)sensors a reliable analytical tool for continuous ISF monitoring? Which is the best calibration protocol to be followed for in vivo assays? Which strategies can be employed to protect the sensing element during skin penetration? Is there an appropriate validation methodology to assess the accuracy of electrochemical MN (bio)sensors? How significant is the distinction between successful achievements in the laboratory and the real commercial feasibility of products? This paper aims to reflect on those previous questions while reviewing the progress of electrochemical MN (bio)sensors in the last decade with a focus on the analytical aspects. Overall, we describe the current state of electrochemical MN (bio)sensors, the benefits and challenges associated to ISF monitoring, as well as key features (and bottlenecks) regarding its implementation for in vivo assays

Toward in vivo transdermal pH sensing with a validated microneedle membrane electrode

We present herein the most complete characterization of microneedle (MN) potentiometric sensors for pH transdermal measurements for the time being. Initial in vitro assessment demonstrated suitable analytical performances (e.g., Nernstian slope, linear range of response from 8.5 to 5.0, and fast response time) in both buffer media and artificial interstitial fluid (ISF). Excellent repeatability and reproducibility together with adequate selectivity and resiliency facilitate the appropriateness of the new pH MN sensor for transdermal ISF analysis in healthcare. The ability to resist skin insertions was evaluated in several ex vivo setups using three different animal skins (i.e., chicken, pork, and rat). The developed pH MN sensor was able to withstand from 5 to 10 repetitive insertions in all the skins considered with a minimal change in the calibration graph (<3% variation in both slope and intercept after the insertions). Ex vivo pH measurements were validated by determining the pH with the MN sensor and a commercial pH electrode in chicken skin portions previously conditioned at several pH values, obtaining excellent results with an accuracy of <1% and a precision of <2% in all cases. Finally, pH MN sensors were applied for the very first time to transdermal measurements in rats together with two innovative validation procedures: (i) measuring subcutaneous pH directly with a commercial pH microelectrode and (ii) collecting ISF using hollow MNs and then the pH measurement of the sample with the pH microelectrode. The pH values obtained with pH MN sensors were statistically more similar to subcutaneous measurements, as inferred by a paired sample t-test at 95% of confidence level. Conveniently, the validation approaches could be translated to other analytes that are transdermally measured with MN sensors

Why not glycine electrochemical biosensors?

Glycine monitoring is gaining importance as a biomarker in clinical analysis due to its involvement in multiple physiological functions, which results in glycine being one of the most analyzed biomolecules for diagnostics. This growing demand requires faster and more reliable, while affordable, analytical methods that can replace the current gold standard for glycine detection, which is based on sample extraction with subsequent use of liquid chromatography or fluorometric kits for its quantification in centralized laboratories. This work discusses electrochemical sensors and biosensors as an alternative option, focusing on their potential application for glycine determination in blood, urine, and cerebrospinal fluid, the three most widely used matrices for glycine analysis with clinical meaning. For electrochemical sensors, voltammetry/amperometry is the preferred readout (10 of the 13 papers collected in this review) and metal-based redox mediator modification is the predominant approach for electrode fabrication (11 of the 13 papers). However, none of the reported electrochemical sensors fulfill the requirements for direct analysis of biological fluids, most of them lacking appropriate selectivity, linear range of response, and/or capability of measuring at physiological conditions. Enhanced selectivity has been recently reported using biosensors (with an enzyme element in the electrode design), although this is still a very incipient approach. Currently, despite the benefits of electrochemistry, only optical biosensors have been successfully reported for glycine detection and, from all the inspected works, it is clear that bioengineering efforts will play a key role in the embellishment of selectivity and storage stability of the sensing element in the sensor

Lactate biosensing for reliable on-body sweat analysis

Wearable lactate sensors for sweat analysis are highly appealing for both the sports and healthcare fields. Electrochemical biosensing is the approach most widely used for lactate determination, and this technology generally demonstrates a linear range of response far below the expected lactate levels in sweat together with a high influence of pH and temperature. In this work, we present a novel analytical strategy based on the restriction of the lactate flux that reaches the enzyme lactate oxidase, which is immobilized in the biosensor core. This is accomplished by means of an outer plasticized polymeric layer containing the quaternary salt tetradodecylammonium tetrakis(4-chlorophenyl) borate (traditionally known as ETH500). Also, this layer prevents the enzyme from being in direct contact with the sample, and hence, any influence with the pH and temperature is dramatically reduced. An expanded limit of detection in the millimolar range (from 1 to 50 mM) is demonstrated with this new biosensor, in addition to an acceptable response time; appropriate repeatability, reproducibility, and reversibility (variations lower than 5% for the sensitivity); good resiliency; excellent selectivity; low drift; negligible influence of the flow rate; and extraordinary correlation (Pearson coefficient of 0.97) with a standardized method for lactate detection such as ion chromatography (through analysis of 22 sweat samples collected from 6 different subjects performing cycling or running). The developed lactate biosensor is suitable for on-body sweat lactate monitoring via a microfluidic epidermal patch additionally containing pH and temperature sensors. This applicability was demonstrated in three different body locations (forehead, thigh, and back) in a total of five on-body tests while cycling, achieving appropriate performance and validation. Moreover, the epidermal patch for lactate sensing is convenient for the analysis of sweat stimulated by iontophoresis in the subjects' arm, which is of great potential toward healthcare applications

Investigation of a mass stranding of 68 short-beaked common dolphins in Golfo Nuevo, Península Valdés, Argentina

We report on the investigation of a mass stranding of 68 short-beaked common dolphins (Delphinus delphis) that occurred in Golfo Nuevo, Península Valdés, Argentina in March 2018. Twenty-one of the stranded dolphins were returned alive to the sea, while 47 animals died. Dead dolphins included all ages, with more males than females (29 males and 18 females). The cause of death investigation reported here is restricted to 15 adult individuals and one fetus on which a full set of diagnostics was prioritized due to limited funding. Our results demonstrate that the death of 16 dolphins assessed in this study was not due to obvious human effects (e.g. bycatch) or underlying pathologies, as all animals were in good body condition and had no external evidence of injuries. Infections by Morbillivirus, Influenza A virus, Sarcocystis spp., Toxoplasma gondii, or Neospora caninum, as well domoic acid (DA) toxicity were ruled out as ethiologies in this event. Notably, results on exposure to paralytic shelfish toxins (PSP) were the only investigated cause of death found positive. This is the first documentation of exposure to PSP toxins in short-beaked common dolphins from the Argentine Sea. At present our results are insufficient to assess whether PSP toxin exposure played a role in the death of the stranded dolphins. Notwithstanding, the full documentation and investigation of the most commonly reported pathogens and toxins involved in cetacean mass strandings allowed us to clear the most relevant health differentials and suggests areas for future study. Additional potential hypothesis related to factors known or speculated to cause cetacean mass strandings are currently being explored within the ecological context at the time of the event

Non-motor symptom burden in patients with Parkinson's disease with impulse control disorders and compulsive behaviours : results from the COPPADIS cohort

The study was aimed at analysing the frequency of impulse control disorders (ICDs) and compulsive behaviours (CBs) in patients with Parkinson's disease (PD) and in control subjects (CS) as well as the relationship between ICDs/CBs and motor, nonmotor features and dopaminergic treatment in PD patients. Data came from COPPADIS-2015, an observational, descriptive, nationwide (Spain) study. We used the validated Questionnaire for Impulsive-Compulsive Disorders in Parkinson's Disease-Rating Scale (QUIP-RS) for ICD/CB screening. The association between demographic data and ICDs/CBs was analyzed in both groups. In PD, this relationship was evaluated using clinical features and treatment-related data. As result, 613 PD patients (mean age 62.47 ± 9.09 years, 59.87% men) and 179 CS (mean age 60.84 ± 8.33 years, 47.48% men) were included. ICDs and CBs were more frequent in PD (ICDs 12.7% vs. 1.6%, p < 0.001; CBs 7.18% vs. 1.67%, p = 0.01). PD patients had more frequent previous ICDs history, premorbid impulsive personality and antidepressant treatment (p < 0.05) compared with CS. In PD, patients with ICDs/CBs presented younger age at disease onset, more frequent history of previous ICDs and premorbid personality (p < 0.05), as well as higher comorbidity with nonmotor symptoms, including depression and poor quality of life. Treatment with dopamine agonists increased the risk of ICDs/CBs, being dose dependent (p < 0.05). As conclusions, ICDs and CBs were more frequent in patients with PD than in CS. More nonmotor symptoms were present in patients with PD who had ICDs/CBs compared with those without. Dopamine agonists have a prominent effect on ICDs/CBs, which could be influenced by dose

Ferrocene self assembled monolayer as a redox mediator for triggering ion transfer across nanometer-sized membranes

Modulation of ion-transfer processes across nanometer-sized voltammetry membranes by ferrocene-based self-assembled monolayer on regular glassy carbon electrode is herein demonstrated. The composition of the membrane is advantageously tuned to promote either cation or anion transfer: the presence of an exchangeable cation results in cation transfer, whereas a lipophilic salt induces anion transfer through the fulfilment of the electroneutrality of the system. When an anodic scan oxidizes ferrocene moieties in the monolayer, these are stabilized by the pairing of lipophilic anions present in the membrane. As a result, either, hydrophilic cations present in the membrane are expelled into the solution or anions enter from the solution generating hence reversible and voltammetric waves for these transfers. The use of a redox active monolayer rather than a conducting polymer film or a redox active compound into the membrane overcomes a number of drawbacks previously manifested by these systems. The confinement of the redox process in a thin film at the immediate vicinity of the membrane allows to avoid the need of elevated number of redox moieties to be sued in the membrane, therefore suppressing its acute leaching and being compatible with the incorporation of both cation and anion ionophores for the first time. In this sense, assisted transfer of lithium and chloride are shown as proof-of-concept. Here, the peak potential of the associated voltammetric waves shifts according to the Nernst equation, in analogy to potentiometric sensors. Analytical detection of lithium and chloride ions in real samples is additionally presented

Rapport de mission au Guatemala et au Mexique du 25 septembre au 2 octobre 1990

Cette mission, qui avait pour principal objectif un appui en biométrie et informatique aux chercheurs de l'IRCC en poste dans les 2 pays, et un cours de biométrie aux cadres de l'ANACAFE, a permis également à l'auteur de visiter des parcelles de caféiers (et cacaoyers au Guatemala), de participer à des réunions de travail, et de prendre connaissance des programmes de recherche caféière au Guatemala (phytopathologie et nématologie) et au Mexique (recherche développement dans la région de Xalapa-Coatepec). L'analyse de régression est présentée en annex