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Dive into the research topics where Pawel Jerzy Wojcik is active.

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Featured researches published by Pawel Jerzy Wojcik.


Biosensors and Bioelectronics | 2013

Bio-microfluidic platform for gold nanoprobe based DNA detection--application to Mycobacterium tuberculosis.

Iwona Bernacka-Wojcik; Paulo Lopes; Ana Catarina Vaz; Bruno Veigas; Pawel Jerzy Wojcik; Pedro Simões; David Barata; Elvira Fortunato; Pedro V. Baptista; Hugo Águas; Rodrigo Martins

We have projected and fabricated a microfluidic platform for DNA sensing that makes use of an optical colorimetric detection method based on gold nanoparticles. The platform was fabricated using replica moulding technology in PDMS patterned by high-aspect-ratio SU-8 moulds. Biochips of various geometries were tested and evaluated in order to find out the most efficient architecture, and the rational for design, microfabrication and detection performance is presented. The best biochip configuration has been successfully applied to the DNA detection of Mycobacterium tuberculosis using only 3 µl on DNA solution (i.e. 90 ng of target DNA), therefore a 20-fold reduction of reagents volume is obtained when compared with the actual state of the art.


Biosensors and Bioelectronics | 2014

Ion sensing (EIS) real-time quantitative monitorization of isothermal DNA amplification.

Bruno Veigas; Rita Branquinho; J.V. Pinto; Pawel Jerzy Wojcik; Rodrigo Martins; Elvira Fortunato; Pedro V. Baptista

Field-effect-based devices are becoming a basic structural element in a new generation of microbiosensors. Reliable molecular characterization of DNA and/or RNA is of paramount importance for disease diagnostics and to follow up alterations in gene expression profiles. The use of such devices for point-of-need diagnostics has been hindered by the need of standard or real-time PCR amplification procedures. The present work focuses on the development of a tantalum pentoxide (Ta2O5) based sensor for the real-time label free detection of DNA amplification via loop mediated isothermal amplification (LAMP) allowing for quantitative analysis of the cMYC proto-oncogene. The strategy based on the field effect sensor was tested within a range of 1 × 10(8)-10(11) copies of target DNA, and a linear relationship between the log copy number of the initial template DNA and threshold time was observed allowing for a semi-quantitative analysis of DNA template. The concept offers many of the advantages of isothermal quantitative real-time DNA amplification in a label free approach and may pave the way to point-of-care quantitative molecular analysis focused on ease of use and low cost.


Biotechnology and Bioengineering | 2015

Single nucleotide polymorphism detection using gold nanoprobes and bio‐microfluidic platform with embedded microlenses

Iwona Bernacka-Wojcik; Hugo Águas; Fábio Ferreira Carlos; Paulo Lopes; Pawel Jerzy Wojcik; Mafalda Costa; Bruno Veigas; Rui Igreja; Elvira Fortunato; Pedro V. Baptista; Rodrigo Martins

The use of microfluidics platforms combined with the optimal optical properties of gold nanoparticles has found plenty of application in molecular biosensing. This paper describes a bio‐microfluidic platform coupled to a non‐cross‐linking colorimetric gold nanoprobe assay to detect a single nucleotide polymorphism associated with increased risk of obesity fat‐mass and obesity‐associated (FTO) rs9939609 (Carlos et al., 2014). The system enabled significant discrimination between positive and negative assays using a target DNA concentration of 5 ng/µL below the limit of detection of the conventionally used microplate reader (i.e., 15 ng/µL) with 10 times lower solution volume (i.e., 3 µL). A set of optimization of our previously reported bio‐microfluidic platform (Bernacka‐Wojcik et al., 2013) resulted in a 160% improvement of colorimetric analysis results. Incorporation of planar microlenses increased 6 times signal‐to‐loss ratio reaching the output optical fiber improving by 34% the colorimetric analysis of gold nanoparticles, while the implementation of an optoelectronic acquisition system yielded increased accuracy and reduced noise. The microfluidic chip was also integrated with a miniature fiber spectrometer to analyze the assays’ colorimetric changes and also the LEDs transmission spectra when illuminating through various solutions. Furthermore, by coupling an optical microscope to a digital camera with a long exposure time (30 s), we could visualise the different scatter intensities of gold nanoparticles within channels following salt addition. These intensities correlate well to the expected difference in aggregation between FTO positive (none to small aggregates) and negative samples (large aggregates). Biotechnol. Bioeng. 2015;112: 1210–1219.


ACS Combinatorial Science | 2014

Statistical Mixture Design and Multivariate Analysis of Inkjet Printed a-WO3/TiO2/WOX Electrochromic Films

Pawel Jerzy Wojcik; L. Pereira; Rodrigo Martins; Elvira Fortunato

An efficient mathematical strategy in the field of solution processed electrochromic (EC) films is outlined as a combination of an experimental work, modeling, and information extraction from massive computational data via statistical software. Design of Experiment (DOE) was used for statistical multivariate analysis and prediction of mixtures through a multiple regression model, as well as the optimization of a five-component sol-gel precursor subjected to complex constraints. This approach significantly reduces the number of experiments to be realized, from 162 in the full factorial (L=3) and 72 in the extreme vertices (D=2) approach down to only 30 runs, while still maintaining a high accuracy of the analysis. By carrying out a finite number of experiments, the empirical modeling in this study shows reasonably good prediction ability in terms of the overall EC performance. An optimized ink formulation was employed in a prototype of a passive EC matrix fabricated in order to test and trial this optically active material system together with a solid-state electrolyte for the prospective application in EC displays. Coupling of DOE with chromogenic material formulation shows the potential to maximize the capabilities of these systems and ensures increased productivity in many potential solution-processed electrochemical applications.


Biosensors and Bioelectronics | 2010

Inkjet printed and "doctor blade" TiO2 photodetectors for DNA biosensors.

Iwona Bernacka-Wojcik; Rohan Senadeera; Pawel Jerzy Wojcik; Leonardo Bione Silva; Gonçalo Doria; Pedro V. Baptista; Hugo Águas; Elvira Fortunato; Rodrigo Martins


Journal of Materials Chemistry | 2012

Microstructure control of dual-phase inkjet-printed a-WO3/TiO2/WOX films for high-performance electrochromic applications

Pawel Jerzy Wojcik; Ana Sofia Cruz; Lídia Santos; L. Pereira; Rodrigo Martins; Elvira Fortunato


Advanced electronic materials | 2015

Structure and Morphologic Influence of WO3 Nanoparticles on the Electrochromic Performance of Dual‐Phase a‐WO3/WO3 Inkjet Printed Films

Lídia Santos; Pawel Jerzy Wojcik; J.V. Pinto; E. Elangovan; Jaime Viegas; L. Pereira; Rodrigo Martins; Elvira Fortunato


Nanoscale | 2015

Tailoring nanoscale properties of tungsten oxide for inkjet printed electrochromic devices

Pawel Jerzy Wojcik; Lídia Santos; L. Pereira; Rodrigo Martins; Elvira Fortunato


Advanced electronic materials | 2015

Flexible and Transparent WO3 Transistor with Electrical and Optical Modulation

Pedro Barquinha; Sónia Pereira; L. Pereira; Pawel Jerzy Wojcik; Paul Grey; Rodrigo Martins; Elvira Fortunato


International Journal of Electrochemical Science | 2014

Contrast Enhancement in Polymeric Electrochromic Devices Encompassing Room Temperature Ionic Liquids

Simone Zanarini; Nadia Garino; Jijeesh Ravi Nair; Carlotta Francia; Pawel Jerzy Wojcik; L. Pereira; Elvira Fortunato; Rodrigo Martins; Silvia Bodoardo; Nerino Penazzi

Collaboration


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Elvira Fortunato

Universidade Nova de Lisboa

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Rodrigo Martins

Universidade Nova de Lisboa

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L. Pereira

Universidade Nova de Lisboa

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Hugo Águas

Universidade Nova de Lisboa

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Pedro V. Baptista

Universidade Nova de Lisboa

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Lídia Santos

Universidade Nova de Lisboa

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Bruno Veigas

Universidade Nova de Lisboa

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J.V. Pinto

Universidade Nova de Lisboa

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