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  4. Liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS) methods for the therapeutic drug monitoring of cytotoxic anticancer drugs: An update
 
research article

Liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS) methods for the therapeutic drug monitoring of cytotoxic anticancer drugs: An update

Briki, Myriam  
•
Murisier, A.
•
Guidi, M.
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April 1, 2024
Journal Of Chromatography B-Analytical Technologies In The Biomedical And Life Sciences

In the era of precision medicine, there is increasing evidence that conventional cytotoxic agents may be suitable candidates for therapeutic drug monitoring (TDM)- guided drug dosage adjustments and patient's tailored personalization of non-selective chemotherapies. To that end, many liquid chromatography coupled to tandem mass spectrometry (LC-MS/MS) assays have been developed for the quantification of conventional cytotoxic anticancer chemotherapies, that have been comprehensively and critically reviewed. The use of stable isotopically labelled internal standards (IS) of cytotoxic drugs was strikingly uncommon, accounting for only 48 % of the methods found, although their use could possible to suitably circumvent patients' samples matrix effects variability. Furthermore, this approach would increase the reliability of cytotoxic drug quantification in highly multi-mediated cancer patients with complex fluctuating pathophysiological and clinical conditions. LC-MS/ MS assays can accommodate multiplexed analyses of cytotoxic drugs with optimal selectivity and specificity as well as short analytical times and, when using stable-isotopically labelled IS for quantification, provide concentrations measurements with a high degree of certainty. However, there are still organisational, pharmacological, and medical constraints to tackle before TDM of cytotoxic drugs can be more largely adopted in the clinics for contributing to our ever-lasting quest to improve cancer treatment outcomes.

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Type
research article
DOI
10.1016/j.jchromb.2024.124039
Web of Science ID

WOS:001221125700001

Author(s)
Briki, Myriam  
•
Murisier, A.
•
Guidi, M.
•
Seydoux, C.
•
Buclin, T.
•
Marzolini, C.
•
Girardin, F. R.
•
Thoma, Y.
•
Carrara, S  
•
Choong, E.
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Date Issued

2024-04-01

Publisher

Elsevier

Published in
Journal Of Chromatography B-Analytical Technologies In The Biomedical And Life Sciences
Volume

1236

Article Number

124039

Subjects

Life Sciences & Biomedicine

•

Physical Sciences

•

Lc-Ms/Ms

•

Stable Isotopically Labelled Internal Standards

•

Cytotoxic Drugs

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Chemotherapy

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Cancer

•

Therapeutic Drug Monitoring

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
SCI-STI-SC  
FunderGrant Number

Swiss National Science Foundation (SNF)

200021_207900/1

Swiss National Science Foundation (SNF)

200021_207900

Available on Infoscience
June 5, 2024
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/208341
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