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Sequencing-based analysis of clonal evolution of 25 mantle cell lymphoma patients at diagnosis and after failure of standard immunochemotherapy

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Karolová, JanaORCiD Profile - 0000-0003-3828-6000WoS Profile - I-4041-2017
Kazantsev, DmitryORCiD Profile - 0000-0001-5660-8080WoS Profile - GQO-7481-2022Scopus Profile - 57220036875
Svatoň, MichaelORCiD Profile - 0000-0003-2966-3687WoS Profile - AAB-3869-2019Scopus Profile - 56440286100
Tušková, LilianaScopus Profile - 57964653500
Forsterová, KristinaORCiD Profile - 0000-0002-9119-081XWoS Profile - H-3858-2018Scopus Profile - 6504000225
Maláriková, DianaORCiD Profile - 0000-0002-3493-7833WoS Profile - N-3400-2017
Benešová, Kateřina
Heizer, TomášORCiD Profile - 0000-0002-6294-2939WoS Profile - F-7138-2017Scopus Profile - 55736697200
Dolníková, AlexandraORCiD Profile - 0000-0002-5982-6523WoS Profile - HZI-2078-2023
Klánová, MagdalenaORCiD Profile - 0000-0003-3526-8114WoS Profile - K-5756-2017Scopus Profile - 55547800300
Winkowska, LucieScopus Profile - 57209969024
Svobodová, Karla
Hojný, JanORCiD Profile - 0000-0002-3563-2484WoS Profile - H-2842-2017Scopus Profile - 55625337400
Krkavcová, Eva
Froňková, EvaORCiD Profile - 0000-0002-6900-8145Scopus Profile - 8905682100
Zemanová, ZuzanaORCiD Profile - 0000-0002-7538-6601WoS Profile - D-8041-2017
Trněný, MarekORCiD Profile - 0000-0002-6952-6073Scopus Profile - 6701742782
Klener, PavelORCiD Profile - 0000-0001-7786-9378WoS Profile - F-7185-2017Scopus Profile - 57193880269

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Publication date
2023
Published in
American Journal of Hematology
Volume / Issue
98 (10)
ISBN / ISSN
ISSN: 0361-8609
ISBN / ISSN
eISSN: 1096-8652
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  • 1. Faculty of Medicine
  • 2. Faculty of Medicine

This publication has a published version with DOI 10.1002/ajh.27044

Abstract
Our knowledge of genetic aberrations, that is, variants and copy number variations (CNVs), associated with mantle cell lymphoma (MCL) relapse remains limited. A cohort of 25 patients with MCL at diagnosis and the first relapse after the failure of standard immunochemotherapy was analyzed using whole-exome sequencing. The most frequent variants at diagnosis and at relapse comprised six genes: TP53, ATM, KMT2D, CCND1, SP140, and LRP1B. The most frequent CNVs at diagnosis and at relapse included TP53 and CDKN2A/B deletions, and PIK3CA amplifications. The mean count of mutations per patient significantly increased at relapse (n = 34) compared to diagnosis (n = 27). The most frequent newly detected variants at relapse, LRP1B gene mutations, correlated with a higher mutational burden. Variant allele frequencies of TP53 variants increased from 0.35 to 0.76 at relapse. The frequency and length of predicted CNVs significantly increased at relapse with CDKN2A/B deletions being the most frequent. Our data suggest, that the resistant MCL clones detected at relapse were already present at diagnosis and were selected by therapy. We observed enrichment of genetic aberrations of DNA damage response pathway (TP53 and CDKN2A/B), and a significant increase in MCL heterogeneity. We identified LRP1B inactivation as a new potential driver of MCL relapse.
Keywords
sequencing-based analysis, clonal evolution, mantle cell lymphoma, failure of standard immunochemotherapy
Permanent link
https://hdl.handle.net/20.500.14178/2001
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WOS:001052377200001
SCOPUS:2-s2.0-85168604207
PUBMED:37605345
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