Direct analysis in real time accurate mass spectrometry determination of bisphenol A in thermal printing paper
-
Add time:07/23/2019 Source:sciencedirect.com
Contact with thermal printing paper is a relevant source of dermal exposure to unbonded bisphenol A (BPA). In order to limit this exposure route, the European Union has introduced a drastic reduction in the maximum allowed concentration of BPA in thermal paper produced after beginning of year 2020. This study investigates the suitability of direct analysis in real time (DART), combined with accurate mass spectrometry, as a faster alternative to chromatography-based methods for the quantitative determination of BPA, and three analogues species, in receipts and tickets usually printed on thermal paper. The ionization efficiency of these compounds is evaluated under different conditions, and the effect of instrumental parameters of the DART source in the observed responses is discussed. The yield of the DART desorption-ionization process was greatly improved when compounds are previously converted into their acetyl derivatives; thereafter, the temperature of electronically excited helium atoms was the most relevant of the evaluated instrumental parameters. Under optimized conditions, the reported method provided recoveries in the range from 90 to 110%, a limit of quantification of 0.004% (w:w), well below the maximum concentration established after 2020 for BPA (0.02%, w:w), and permitted to perform duplicate determinations of each sample extract with a response time around 1 min. The accuracy of BPA levels found in non-spiked samples was confirmed using GC-EI-MS as reference technique. BPA was systematically noticed in the processed samples with concentrations ranging from 0.005% to more than 6%.
We also recommend Trading Suppliers and Manufacturers of BISPHENOL A DIACETATE (cas 10192-62-8). Pls Click Website Link as below: cas 10192-62-8 suppliers
Prev:Alkylaldehyde–bisulfite adducts as cleavable surfactants
Next:Embryonic stem cell- and transcriptomics-based in vitro analyses reveal that bisphenols A, F and S have similar and very complex potential developmental toxicities) - 【Back】【Close 】【Print】【Add to favorite 】
- Related Information
- Bisphenol-A induces neurodegeneration through disturbance of intracellular calcium homeostasis in human embryonic stem cells-derived cortical neurons08/01/2019
- DNA damaging and apoptotic potentials of Bisphenol A and Bisphenol S in human bronchial epithelial cells07/31/2019
- Effects of bisphenol A and its analogs bisphenol F and S on life parameters, antioxidant system, and response of defensome in the marine rotifer Brachionus koreanus07/30/2019
- Bisphenol A, bisphenol S, bisphenol F and bisphenol AF induce different oxidative stress and damage in human red blood cells (in vitro study)07/29/2019
- Immunotoxicity of bisphenol S and F are similar to that of bisphenol A during zebrafish early development07/28/2019
- Bisphenol A induced oxidative stress mediated genotoxicity in Drosophila melanogaster07/27/2019
- Carbon nanotubes affect the formation of trihalomethanes during chlorination of bisphenol A07/26/2019
- Toxic effects of bisphenol A diglycidyl ether and derivatives in human placental cells07/25/2019
- Embryonic stem cell- and transcriptomics-based in vitro analyses reveal that bisphenols A, F and S have similar and very complex potential developmental toxicities07/24/2019
