Arnaud Lubin

@jnj.com

Principal Biotransformation Scientist - Translational PKPD and Investigative Toxicology

Arnaud Lubin


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https://researchid.co/arnaudl

RESEARCH, TEACHING, or OTHER INTERESTS

Analytical Chemistry, Drug Discovery, Pharmaceutical Science, General Pharmacology, Toxicology and Pharmaceutics
8

Scopus Publications

Scopus Publications

  • Development of a Robust Platform for Infrared Ion Spectroscopy: A New Addition to the Analytical Toolkit for Enhanced Metabolite Structure Elucidation
    Teun van Wieringen, Arnaud Lubin, Rianne van Outersterp, Jonathan Martens, Eric van Beelen, et al.
    Analytical Chemistry, 2025
  • Identification of Drug Metabolites with Infrared Ion Spectroscopy – Application to Midazolam in vitro Metabolism**
    Rianne E. van Outersterp, Jonathan Martens, Giel Berden, Arnaud Lubin, Filip Cuyckens, et al.
    Chemistry Methods, 2023
    The identification of biotransformation products of drug compounds is a crucial step in drug development. Over the last decades, liquid chromatography‐mass spectrometry (LC‐MS) has become the method of choice for metabolite profiling because of its high sensitivity and selectivity. However, determining the full molecular structure of the detected metabolites, including the exact biotransformation site, remains challenging on the basis of MS alone. Here we explore infrared ion spectroscopy (IRIS) as a novel MS‐based method for the elucidation of metabolic pathways in drug metabolism research. Using the drug midazolam as an example, we identify several biotransformation products directly from an in vitro drug incubation sample. We show that IR spectra of the aglycone MS/MS fragment ions of glucuronide metabolites establish a direct link between detected phase I and phase II metabolites. Moreover, using quantum‐chemically computed IR spectra of candidate structures, we are able to assign the exact sites of biotransformation in absence of reference standards. Additionally, we demonstrate the utility of IRIS for structural elucidation by identifying several ring‐opened midazolam derivatives formed in an acidic environment.
  • Strategies and analytical workflows to extend the dynamic range in quantitative LC-MS/MS analysis
    Emmanuel Njumbe Ediage, Tania Aerts, Arnaud Lubin, Filip Cuyckens, Lieve Dillen, et al.
    Bioanalysis, 2019
    Aim: To evaluate alternative analytical strategies to extend the dynamic range in quantitative LC-MS/MS. Methodology & results: Two approaches based on prior or no prior knowledge of expected exposure levels were evaluated. These approaches make use of two analytical strategies, which include the use of more than one injection volume or dilution of sample extract with solvents or solvent mixtures. A total of 16 compounds with varying logP values were classified into polar and nonpolar groups and used in this evaluation. From the two analytical strategies, three workflows were derived. Conclusion: All three workflows were successfully evaluated and resulted in good accuracy (80-120%) for all the compound groups.
  • Flexible nano- and microliter injections on a single liquid chromatography–mass spectrometry system: Minimizing sample preparation and maximizing linear dynamic range
    Arnaud Lubin, Sheng Sheng, Deirdre Cabooter, Patrick Augustijns, Filip Cuyckens
    Journal of Chromatography A, 2017
  • An atmospheric pressure ionization source using a high voltage target compared to electrospray ionization for the LC/MS analysis of pharmaceutical compounds
    Arnaud Lubin, Ronald De Vries, Deirdre Cabooter, Patrick Augustijns, Filip Cuyckens
    Journal of Pharmaceutical and Biomedical Analysis, 2017
  • Atmospheric Pressure Ionization Using a High Voltage Target Compared to Electrospray Ionization
    Arnaud Lubin, Steve Bajic, Deirdre Cabooter, Patrick Augustijns, Filip Cuyckens
    Journal of the American Society for Mass Spectrometry, 2017
  • Enhanced performance for the analysis of prostaglandins and thromboxanes by liquid chromatography-tandem mass spectrometry using a new atmospheric pressure ionization source
    Arnaud Lubin, Suzy Geerinckx, Steve Bajic, Deirdre Cabooter, Patrick Augustijns, et al.
    Journal of Chromatography A, 2016
  • One drop chemical derivatization - DESI-MS analysis for metabolite structure identification
    Arnaud Lubin, Deirdre Cabooter, Patrick Augustijns, Filip Cuyckens
    Journal of Mass Spectrometry, 2015
    Structural elucidation of metabolites is an important part during the discovery and development process of new pharmaceutical drugs. Liquid Chromatography (LC) in combination with Mass Spectrometry (MS) is usually the technique of choice for structural identification but cannot always provide precise structural identification of the studied metabolite (e.g. site of hydroxylation and site of glucuronidation). In order to identify those metabolites, different approaches are used combined with MS data including nuclear magnetic resonance, hydrogen/deuterium exchange and chemical derivatization followed by LC‐MS. Those techniques are often time‐consuming and/or require extra sample pre‐treatment.In this paper, a fast and easy to set up tool using desorption electrospray ionization–MS for metabolite identification is presented. In the developed method, analytes in solution are simply dried on a glass plate with printed Teflon spots and then a single drop of derivatization mixture is added. Once the spot is dried, the derivatized compound is analyzed. Six classic chemical derivatizations were adjusted to work as a one drop reaction and applied on a list of compounds with relevant functional groups. Subsequently, two successive reactions on a single spot of amoxicillin were tested and the methodology described was successfully applied on an in vitro incubated alprazolam metabolite. All reactions and analyses were performed within an hour and gave useful structural information by derivatizing functional groups, making the method a time‐saving and efficient tool for metabolite identification if used in addition or in some cases as an alternative to common methods. Copyright © 2015 John Wiley & Sons, Ltd.