On the utility of ultrafast MS1-only proteomics in drug target discovery studies based on thermal proteome profiling method
Ivan I Fedorov
1, 2
,
Julia A Bubis
1
,
Anna A Lobas
1
,
Mark V Ivanov
1
,
Daria D Emekeeva
1
,
Irina A Tarasova
1
,
Alexey A. Nazarov
3, 4
,
Publication type: Journal Article
Publication date: 2024-05-15
scimago Q2
wos Q1
SJR: 0.716
CiteScore: 7.9
Impact factor: 3.8
ISSN: 16182642, 16182650
PubMed ID:
38744720
Abstract
Advances in high-throughput high-resolution mass spectrometry and the development of thermal proteome profiling approach (TPP) have made it possible to accelerate a drug target search. Since its introduction in 2014, TPP quickly became a method of choice in chemical proteomics for identifying drug-to-protein interactions on a proteome-wide scale and mapping the pathways of these interactions, thus further elucidating the unknown mechanisms of action of a drug under study. However, the current TPP implementations based on tandem mass spectrometry (MS/MS), associated with employing lengthy peptide separation protocols and expensive labeling techniques for sample multiplexing, limit the scaling of this approach for the ever growing variety of drug-to-proteomes. A variety of ultrafast proteomics methods have been developed in the last couple of years. Among them, DirectMS1 provides MS/MS-free quantitative proteome-wide analysis in 5-min time scale, thus opening the way for sample-hungry applications, such as TPP. In this work, we demonstrate the first implementation of the TPP approach using the ultrafast proteome-wide analysis based on DirectMS1. Using a drug topotecan, which is a known topoisomerase I (TOP1) inhibitor, the feasibility of the method for identifying drug targets at the whole proteome level was demonstrated for an ovarian cancer cell line.
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Total citations:
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Citations from 2024:
4
(100%)
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Fedorov I. I. et al. On the utility of ultrafast MS1-only proteomics in drug target discovery studies based on thermal proteome profiling method // Analytical and Bioanalytical Chemistry. 2024. Vol. 416. No. 18. pp. 4083-4089.
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Fedorov I. I., Bubis J. A., Kazakova E. M., Lobas A. A., Ivanov M. V., Emekeeva D. D., Tarasova I. A., Nazarov A. A., Gorshkov M. V. On the utility of ultrafast MS1-only proteomics in drug target discovery studies based on thermal proteome profiling method // Analytical and Bioanalytical Chemistry. 2024. Vol. 416. No. 18. pp. 4083-4089.
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TY - JOUR
DO - 10.1007/s00216-024-05330-9
UR - https://link.springer.com/10.1007/s00216-024-05330-9
TI - On the utility of ultrafast MS1-only proteomics in drug target discovery studies based on thermal proteome profiling method
T2 - Analytical and Bioanalytical Chemistry
AU - Fedorov, Ivan I
AU - Bubis, Julia A
AU - Kazakova, Elizaveta M
AU - Lobas, Anna A
AU - Ivanov, Mark V
AU - Emekeeva, Daria D
AU - Tarasova, Irina A
AU - Nazarov, Alexey A.
AU - Gorshkov, Mikhail V.
PY - 2024
DA - 2024/05/15
PB - Springer Nature
SP - 4083-4089
IS - 18
VL - 416
PMID - 38744720
SN - 1618-2642
SN - 1618-2650
ER -
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BibTex (up to 50 authors)
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@article{2024_Fedorov,
author = {Ivan I Fedorov and Julia A Bubis and Elizaveta M Kazakova and Anna A Lobas and Mark V Ivanov and Daria D Emekeeva and Irina A Tarasova and Alexey A. Nazarov and Mikhail V. Gorshkov},
title = {On the utility of ultrafast MS1-only proteomics in drug target discovery studies based on thermal proteome profiling method},
journal = {Analytical and Bioanalytical Chemistry},
year = {2024},
volume = {416},
publisher = {Springer Nature},
month = {may},
url = {https://link.springer.com/10.1007/s00216-024-05330-9},
number = {18},
pages = {4083--4089},
doi = {10.1007/s00216-024-05330-9}
}
Cite this
MLA
Copy
Fedorov, Ivan I., et al. “On the utility of ultrafast MS1-only proteomics in drug target discovery studies based on thermal proteome profiling method.” Analytical and Bioanalytical Chemistry, vol. 416, no. 18, May. 2024, pp. 4083-4089. https://link.springer.com/10.1007/s00216-024-05330-9.