266 research outputs found
Celiac disease detection using a transglutaminase electrochemical immunosensor fabricated on nanohybrid screen-printed carbon electrodes
Celiac disease is a gluten-induced autoimmune enteropathy characterized by the presence of tissue tranglutaminase
(tTG) autoantibodies. A disposable electrochemical immunosensor (EI) for the detection
of IgA and IgG type anti-tTG autoantibodies in real patient’s samples is presented. Screen-printed carbon
electrodes (SPCE) nanostructurized with carbon nanotubes and gold nanoparticles were used as the
transducer surface. This transducer exhibits the excellent characteristics of carbon–metal nanoparticle
hybrid conjugation and led to the amplification of the immunological interaction. The immunosensing
strategy consisted of the immobilization of tTG on the nanostructured electrode surface followed by the
electrochemical detection of the autoantibodies present in the samples using an alkaline phosphatase
(AP) labelled anti-human IgA or IgG antibody. The analytical signal was based on the anodic redissolution
of enzymatically generated silver by cyclic voltammetry. The results obtained were corroborated with a
commercial ELISA kit indicating that the electrochemical immunosensor is a trustful analytical screening
tool
Voltammetric immunosensor for the simultaneous analysis of the breast cancer biomarkers CA 15-3 and HER2-ECD
Cancer Antigen 15-3 (CA 15-3) and the extracellular domain of the human epidermal growth factor receptor 2 (HER2-ECD) are independent breast cancer biomarkers. The combination of their profiles (presence and concentration) could provide an important contribution to diagnostics and patient follow-up. Therefore, a disposable electrochemical immunosensor for the simultaneous detection of CA 15-3 and HER2-ECD was developed in this work. The immunosensor was constructed on a customized dual screen-printed carbon electrode. The carbon working electrodes' surfaces were first modified with in situ electrodeposited gold nanoparticles and then individually coated with either a monoclonal anti-human CA 15-3 or a monoclonal anti-human HER2-ECD antibody. After incubation with the biomarkers and monoclonal biotin-labelled detection antibodies, the antigen-antibody interactions were detected by linear sweep voltammetric analysis of enzymatically (alkaline phosphatase) generated metallic silver. The immunosensor’s limits of detection for the selected biomarkers were 5.0 U mL−1 for CA 15-3 and 2.9 ng mL−1 for HER2-ECD. These values could allow the use of the sensor in the non-invasive control of these biomarkers in breast cancer patients.This work received financial support from the European Union (FEDER funds through COMPETE) and National Funds (FCT, Fundação para a Ciência e a Tecnologia) through projects PTDC/SAU-ENB/114786/2009 and UID/QUI/50006/2013. Estefanía Costa Rama thanks the Government of Principado de Asturias for the award of a Severo Ochoa predoctoral grant (BP11-097).info:eu-repo/semantics/publishedVersio
An electrochemical deamidated gliadin antibody immunosensor for celiac disease clinical diagnosis
The first electrochemical immunosensor (EI) for the detection of
antibodies against deamidated gliadin peptides (DGP) is described
here. A disposable nanohybrid screen-printed carbon electrode
modified with DGP was employed as the transducer's sensing
surface. Real serumsampleswere successfully assayed and the results
were corroborated with an ELISA kit. The presented EI is a promising
analytical tool for celiac disease diagnosis
Competitive electrochemical immunosensor for the detection of unfolded p53 protein in blood as biomarker for Alzheimer’s disease
Alzheimer's disease is one of the most common causes of dementia nowadays, and its prevalence increases over time. Because of this and the difficulty of its diagnosis, accurate methods for the analysis of specific biomarkers for an early diagnosis of this disease are much needed. Recently, the levels of unfolded isoform of the multifunctional protein p53 in plasma have been proved to increase selectively in Alzheimer's Disease patients in comparison with healthy subjects, thus entering the list of biomarkers that can be used for the diagnosis of this illness.
We present here the development of an electrochemical immunosensor based on nanostructured screen-printed carbon electrodes for the quantification of unfolded p53 in plasma samples. The sensor shows a suitable linear range (from 2 to 50 nM) for its application in real blood samples and a very low limit of detection (0.05 nM). The concentration of unfolded p53 has been accurately detected in plasma of elderly people in healthy conditions, subjects with mild cognitive impairment (MCI) and Alzheimer's Disease (AD) subjects, obtaining results with no significant differences to those provided by an ELISA assay. These results support the possibility of measuring unfolded p53 levels with a cheap, simple and miniaturized device with a promising future for point-of-care applications in the early diagnosis of Alzheimer's dementia.This work has been supported by the FC-15-GRUPIN14-021 project from the Asturias Regional Government and the CTQ2014-58826-R and MINECO-18-CTQ2017-86994-R projects from the Spanish Ministry of Economy and Competitiveness (MINECO). O. Amor-Gutiérrez thanks Vicerrectorado de Investigación from University of Oviedo for the award of a grant “Ayudas para la realización de tesis doctorales” (PAPI-18-PF-13) through Plan de Apoyo y Promoción de la Investigación.info:eu-repo/semantics/publishedVersio
Celiac disease diagnosis and gluten-free food analytical control
Celiac disease (CD) is an autoimmune enteropathy,
characterized by an inappropriate T-cell-mediated
immune response to the ingestion of certain dietary cereal
proteins in genetically susceptible individuals. This disorder
presents environmental, genetic, and immunological components.
CD presents a prevalence of up to 1% in
populations of European ancestry, yet a high percentage
of cases remain underdiagnosed. The diagnosis and
treatment should be made early since untreated disease
causes growth retardation and atypical symptoms, like
infertility or neurological disorders. The diagnostic criteria
for CD, which requires endoscopy with small bowel biopsy,
have been changing over the last few decades, especially
due to the advent of serological tests with higher sensitivity and specificity. The use of serological markers can be very
useful to rule out clinical suspicious cases and also to help
monitor the patients, after adherence to a gluten-free diet.
Since the current treatment consists of a life-long glutenfree
diet, which leads to significant clinical and histological
improvement, the standardization of an assay to assess in an
unequivocal way gluten in gluten-free foodstuff is of major
importance
Bioelectroanalysis in a Drop: Construction of a Glucose Biosensor
This lab experiment describes a complete method to fabricate an enzymatic glucose electroanalytical biosensor by students. Using miniaturized and disposable screen-printed electrodes (SPEs), students learn how to use them as transducers and understand the importance SPEs have acquired in sensor development during the last years. Students can also revise concepts related to enzymatic assays, with glucose oxidase and horseradish peroxidase involved in subsequent reactions. Moreover, they learn the trends that current analytical chemistry follows presently such as miniaturization, portability, and low cost. At the same time, this experiment serves to teach basic analytical concepts (accuracy, precision, sensitivity, and selectivity) in a practical way. The high clinical interest of glucose, due to a large number of diabetes patients around the world, and the application of the sensor to analysis of real food samples make this experiment very attractive to students. The questions set out along this experiment help students to acquire skills for solving analytical problems from the very beginning
Mercury determination in urine samples by gold nanostructured screen-printed carbon electrodes after vortex-assisted ionic liquid dispersive liquid–liquid microextraction
A novel approach is presented to determine mercury in urine samples, employing vortex-assisted ionic liquid dispersive liquid–liquid microextraction and microvolume back-extraction to prepare samples, and screen-printed electrodes modified with gold nanoparticles for voltammetric analysis. Mercury was extracted directly from non-digested urine samples in a water-immiscible ionic liquid, being back-extracted into an acidic aqueous solution. Subsequently, it was determined using gold nanoparticle-modified screen-printed electrodes. Under optimized microextraction conditions, standard addition calibration was applied to urine samples containing 5, 10 and 15 μg L−1 of mercury. Standard addition calibration curves using standards between 0 and 20 μg L−1 gave a high level of linearity with correlation coefficients ranging from 0.990 to 0.999 (N = 5). The limit of detection was empirical and statistically evaluated, obtaining values that ranged from 0.5 to 1.5 μg L−1, and from 1.1 to 1.3 μg L−1, respectively, which are significantly lower than the threshold level established by the World Health Organization for normal mercury content in urine (i.e., 10–20 μg L−1). A certified reference material (REC-8848/Level II) was analyzed to assess method accuracy finding 87% and 3 μg L−1 as the recovery (trueness) and standard deviation values, respectively. Finally, the method was used to analyze spiked urine samples, obtaining good agreement between spiked and found concentrations (recovery ranged from 97 to 100%).The authors would like to thank the Spanish Ministry of Science and Innovation (projects n. CTQ2011-23968 and CTQ2011-24560), Generalitat Valenciana (Spain) (projects n. ACOMP/2013/072, GVA/2014/096 and PROMETEO/2013/038) and University of Alicante (Spain) (project n. GRE12-45) for the financial support. E. Fernández also thanks Ministry of Education (FPU13/03125) for her FPU grant
High Performance Tunable Catalysts Prepared by Using 3D Printing
Honeycomb monoliths are the preferred supports in many industrial heterogeneous
catalysis reactions, but current extrusion synthesis only allows obtaining parallel channels. Here,
we demonstrate that 3D printing opens new design possibilities that outperform conventional
catalysts. High performance carbon integral monoliths have been prepared with a complex network
of interconnected channels and have been tested for carbon dioxide hydrogenation to methane after
loading a Ni/CeO2 active phase. CO2 methanation rate is enhanced by 25% at 300 ◦C because the
novel design forces turbulent flow into the channels network. The methodology and monoliths
developed can be applied to other heterogeneous catalysis reactions, and open new synthesis options
based on 3D printing to manufacture tailored heterogeneous catalysts
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