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Multiplexed Relative Quantitation with Isobaric Tagging Mass Spectrometry Reveals Class I Major Histocompatibility Complex Ligand Dynamics in Response to Doxorubicin

Authors :
Murphy, J. Patrick
Yu, Qijia
Konda, Prathyusha
Paulo, Joao A.
Jedrychowski, Mark P.
Kowalewski, Daniel J.
Schuster, Heiko
Kim, Youra
Clements, Derek
Jain, Aditya
Stevanovic, Stefan
Gygi, Steven P.
Mancias, Joseph D.
Gujar, Shashi
Source :
Analytical Chemistry; April 2019, Vol. 91 Issue: 8 p5106-5115, 10p
Publication Year :
2019

Abstract

MHC-I peptides are intracellular-cleaved peptides, usually 8–11 amino acids in length, which are presented on the cell surface and facilitate CD8+T cell responses. Despite the appreciation of CD8+T-cell antitumor immune responses toward improvement in patient outcomes, the MHC-I peptide ligands that facilitate the response are poorly described. Along these same lines, although many therapies have been recognized for their ability to reinvigorate antitumor CD8+T-cell responses, whether these therapies alter the MHC-I peptide repertoire has not been fully assessed due to the lack of quantitative strategies. We develop a multiplexing platform for screening therapy-induced MHC-I ligands by employing tandem mass tags (TMTs). We applied this approach to measuring responses to doxorubicin, which is known to promote antitumor CD8+T-cell responses during its therapeutic administration in cancer patients. Using both in vitro and in vivo systems, we show successful relative quantitation of MHC-I ligands using TMT-based multiplexing and demonstrate that doxorubicin induces MHC-I peptide ligands that are largely derived from mitotic progression and cell-cycle proteins. This high-throughput MHC-I ligand discovery approach may enable further explorations to understand how small molecules and other therapies alter MHC-I ligand presentation that may be harnessed for CD8+T-cell-based immunotherapies.

Details

Language :
English
ISSN :
00032700 and 15206882
Volume :
91
Issue :
8
Database :
Supplemental Index
Journal :
Analytical Chemistry
Publication Type :
Periodical
Accession number :
ejs48574074
Full Text :
https://doi.org/10.1021/acs.analchem.8b05616