Direct Monitoring of Thickness and Refractive Index of Optical Thin Film Deposited on Fiber End-face

We propose a system for depositing thin films on waveguides which enables low-temperature deposition and precise control of the refractive index and film thickness. It is composed of a conventional ion-beam sputtering (IBS) system and a new system for directly monitoring film characteristics during deposition. We controlled refractive indices over a wide range from 1.52 to 1.97 by moving the sputtering targets (SiO₂ and Si₃N₄) in the IBS system. The refractive index or film thickness was in-situ monitored by observing the optical power reflected from the end-face of a monitoring fiber set in the deposition chamber. Antireflection coating films were successfully deposited on a fiber end-face and a laser diode chip facet with low reflectivity from 0.05 to 0.07%. This deposition system is attractive for constructing highly functional optical devices for future photonic networks.     

Some physico-chemical characteristics of amino-acid derivatives containing rest of 1,2,4-triazole-3,4-di-substituted with potential antitumoral activity

Abstract

Dipeptide derivatives from p-aminobenzoyl-phenylglycine and p-aminobenzoyl-phenylalanine were grafted on 1,2,4-triazole heterocycle in order to get new substances with potential biological activity. The compounds synthetized and characterized in this paper have a structure that fits in the antimetabolites category, products used to treat malignant tumors. The presence of several bioactive groups in the same molecule permits us to study the chemical structure - biological activity correlation based on computational analyses using SPARTAN’14 software. Some correlations between the molecular parameters established with Spartan’14 software are evidenced in this paper.     

Multiplexed therapeutic drug monitoring of antipsychotics in dried plasma spots by LC‐MS/MS

In this work, a convenient method for the therapeutic monitoring of seven common antipsychotic drugs in “dried plasma spot” samples has been developed. It is based on the liquid chromatography tandem mass spectrometry technique, operating in multiple reaction monitoring mode, and a straightforward procedure for the simultaneous extraction of all antipsychotics in a single step, with high extraction yield. The method was fully validated with proper accuracy, precision, selectivity and sensitivity, for all the drugs. Limits of quantification were 0.12, 1.09, 1.46, 1.47, 5.70, 1.32, 1.33 µg/L for haloperidol, aripiprazole, olanzapine, quetiapine, clozapine, risperidone, and paliperidone, respectively. Accuracy, intra‐ and interday precision values were <10% for all drugs at all concentration levels examined. The method was tested in the analysis of 30 plasma samples from real patients for each drug. The proposed analytical approach, by combining practical and logistical advantages of microsampling with liquid chromatography tandem mass spectrometry analytical performance, could offer an ideal strategy for accurate and timely therapeutic drug monitoring of antipsychotic drugs in most clinical settings, even in remote centers and/or in out‐patient settings, bringing so many potential improvements in psychiatric patient care.     

Monitoring photopolymerization reactions through thermal imaging: A unique tool for the real‐time follow‐up of thick samples, 3D printing,and composites

The ever increasing applications of photopolymers from historical thin (<50 µm) coatings to very deep samples (>1 cm) require the development of robust 4D monitoring strategies able to assess photopolymerization efficiencies (first dimension) as a function of time (second dimension) and position (third and fourth dimensions). Therefore, here, we demonstrated that thermal imaging is a valuable photopolymerization monitoring device showing: (a) very high response times (<1 s); (b) high repeatability of the measurement; (c) strong adaptability of the setup to various conditions (e.g., onto irregular surfaces or inside a real time Fourier transformed infrared spectrometer (RT‐FTIR)); (d) extremely deep photopolymerization follow‐ups (and subsequent rationalization) with good resolution in time and in space (real‐time thermal imaging microscopy experiments); (e) adaptability to applied materials. This monitoring strategy was found particularly robust when taking into account all the heat generating phenomena (i.e., direct heating from the lamp vs. temperature raised due to monomer conversion). As a result, we propose thermal imaging as the next reference monitoring system for the new ranges of thick and/or filled samples (e.g., 3D objects, composites) and/or applied photopolymerizations (e.g., 3D printing) more and more present in the literature. © 2018 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2018 , 56, 889–899     

基于Bragg光纤光栅传感器的监测系统设计

设计了基于Bragg光纤光栅传感技术的监测系统,当光纤光栅所处环境的温度、应力、应变或其他物理量发生变化时,光栅的周期或纤芯折射率将发生变化,从而使反射光的波长发生变化,通过测量反射光中心波长的变化,就可以获得待测物理量的变化情况.该系统利用薄膜滤波器完成对外界的分布式测量,采用光强度检测,能够实现无缝监测.     

Structural analysis of a fractional matching problem

Mixed Software Programming refers to a novel software development paradigm resulting from efforts to combine two different programming approaches: Solo Programming and Pair Programming. Solo Programming refers to the traditional practice of assigning a single developer to develop a software module and Pair Programming refers to a relatively new approach where two developers work simultaneously on developing a module. In Mixed Programming, given a set of modules to be developed, a chosen subset of modules may be developed using Solo Programming and the remaining modules using Pair Programming.Motivated by applications in Mixed Software Programming, we consider the following generalization of classical fractional 1-matching problem: Given an undirected simple graph G=(V;E), and a positive number F, find values for x_e,e∈E, satisfying the following:

1.

.

2.

, where δ(i)={e∈E:e=(i,j)},i∈V.

3.

Maximize {2∑_e∈Ex_e−F|{i∈V:∑_e∈δ(i)x_e=1}|}.

We show that this problem is solvable in strongly polynomial time. Our primary focus in this paper is on obtaining the structure of the optimal solution for an arbitrary instance of the problem.     

Synthesis of α-fluoro-α,β-unsaturated esters monitored by 1D and 2D benchtop NMR spectroscopy

For optimization and control of pharmaceutically and industrially important reactions, chemical information is required in real time. Instrument size, handling, and operation costs are important criteria to be considered when choosing a suitable analytical method apart from sensitivity and resolution. This present study explores the use of a robust and compact nuclear magnetic resonance (NMR) spectrometer to monitor the stereo-selective formation of α-fluoro-α,β-unsaturated esters from α-fluoro-β-keto esters via deprotonation and deacylation in real time. These compounds are precursors of various pharmaceutically active substances. The real-time study revealed the deprotonation and deacylation steps of the reaction. The reaction was studied at temperatures ranging from 293 to 333 K by interleaved one-dimensional ¹H and ¹⁹F and two-dimensional ¹H–¹H COSY experiments. The kinetic rate constants were evaluated using a pseudo first-order kinetic model. The activation energies for the deprotonation and deacylation steps were determined to 28 ± 2 and 63.5 ± 8 kJ/mol, respectively. This showed that the deprotonation step is fast compared with the deacylation step and that the deacylation step determines the rate of the overall reaction. The reaction was repeated three times at 293 K to monitor the repeatability and stability of the system. The compact NMR spectrometer provided detailed information on the mechanism and kinetics of the reaction, which is essential for optimizing the synthetic routes for stepwise syntheses of pharmaceutically active substances.     

改进的数据流缺失数据处理算法

数据流预处理主要是在原始观测数据的基础上进行,包括对原始监测到的数据集中的缺失数据进行插补或剔除,是数据流预测过程中一个重要性环节,是数据流应用中必不可少的组成部分.数据流预处理技术可以改进监测数据流的质量,从而有助于提高其后的处理过程的精度和性能.     

An efficient solution for resolving iTRAQ and TMT channel cross‐talk

Isobaric tagging reagents such as isobaric tag for relative and absolute quantitation (iTRAQ) and tandem mass tag (TMT) typically have isotopic impurities that cause significant cross‐talk between channels. Here, we present an efficient solution to compensate for channel cross‐talk using linear algebra and find that it is between 20× and 120× faster than previous methods. We also find that the effects of channel cross‐talk are as important to manage as the effects of ratio compression because of precursor impurities, and we have released an open‐source tool to perform both types of calculations.     

Quantitative selenium speciation in human urine by using liquid chromatography–electrospray tandem mass spectrometry

A liquid chromatography–electrospray-tandem mass spectrometry (ES-MS/MS) method was developed for the speciation analysis of four organic selenium species of relevance to human urinary metabolism, namely trimethylselenomium ion (TMSe⁺), selenomethionine (SeMet) and the two selenosugars, methyl 2-acetamido-2-deoxy-1-seleno-β-d-galactos/-glucos-amine (SeGalNAc and SeGluNAc, respectively). Their chromatographic separation was achieved by using a cation exchange pre-column coupled in-series with a reversed-phase high-performance liquid chromatography column, along with an isocratic mobile phase. Online detection was performed using ES-MS/MS in selective reaction monitoring mode. SeGalNAc was detected as the major human urinary metabolite of selenium in the samples analysed, whereas TMSe⁺ was detected in the urine of one volunteer before and after receiving a selenium supplement. SeMet was not detected as a urine excretory metabolite in this study. Spiking experiments performed with the urine samples revealed significant signal suppression caused by coeluting matrix constituents. To overcome such interferences, isotopically labelled ¹³CD₃⁸²SeGalNAc was used as an internal standard, whereas in the absence of an isotopically labelled internal standard for TMSe⁺, the standard addition method was applied. Quality control for the accurate quantitation of TMSe⁺ and SeGalNAc was carried out by analysing spiked human urine samples with appropriate selenium standards over a concentration range of 10–50 μg Se L⁻¹. The method has achieved a limit of detection in the presence of urine matrix comparable to that of HPLC-inductively coupled plasma-mass spectrometry for the four selenium species: 1.0 μg Se L⁻¹ for TMSe⁺, 5.6 μg Se L⁻¹ for SeMet, and 0.1 μg Se L⁻¹ for both SeGalNAc and SeGluNAc.