Novel insights into the pathogenesis of follicular lymphoma by molecular profiling of localized and systemic disease forms

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作者
Sabrina Kalmbach
Michael Grau
Myroslav Zapukhlyak
Ellen Leich
Vindi Jurinovic
Eva Hoster
Annette M. Staiger
Katrin S. Kurz
Oliver Weigert
Erik Gaitzsch
Verena Passerini
Marianne Engelhard
Klaus Herfarth
Klaus Beiske
Francesca Micci
Peter Möller
Heinz-Wolfram Bernd
Alfred C. Feller
Wolfram Klapper
Harald Stein
Martin-Leo Hansmann
Sylvia Hartmann
Martin Dreyling
Harald Holte
Georg Lenz
Andreas Rosenwald
German Ott
Heike Horn
机构
[1] Robert-Bosch Hospital,Department of Clinical Pathology
[2] Dr. Margarete Fischer-Bosch Institute of Clinical Pharmacology,Department of Medicine A, Department of Hematology, Oncology and Pneumology
[3] University of Tübingen,Institute of Pathology
[4] University Hospital Münster,Department of Medicine III
[5] University of Würzburg and Comprehensive Cancer Center Main,Department for Radiotherapy
[6] University Hospital,Department of Radiation Oncology
[7] LMU Munich,Department of Oncology
[8] University Hospital of Essen,Section for Cancer Cytogenetics
[9] University of Heidelberg,Institute of Pathology
[10] Oslo University Hospital,Institute of Pathology, Hematopathology Section and Lymph Node Registry
[11] KG Jebsen center for B cell malignancies,Institute of Pathology
[12] Oslo University Hospital,undefined
[13] University Hospital Ulm,undefined
[14] Hematopathology,undefined
[15] University Hospital Schleswig-Holstein,undefined
[16] Campus Kiel,undefined
[17] Pathodiagnostik Berlin,undefined
[18] University Hospital Frankfurt,undefined
来源
Leukemia | 2023年 / 37卷
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摘要
Knowledge on the pathogenesis of FL is mainly based on data derived from advanced/systemic stages of FL (sFL) and only small cohorts of localized FL (lFL) have been characterized intensively so far. Comprehensive analysis with profiling of somatic copy number alterations (SCNA) and whole exome sequencing (WES) was performed in 147 lFL and 122 sFL. Putative targets were analyzed for gene and protein expression. Overall, lFL and sFL, as well as BCL2 translocation-positive (BCL2+) and –negative (BCL2−) FL showed overlapping features in SCNA and mutational profiles. Significant differences between lFL and sFL, however, were detected for SCNA frequencies, e.g., in 18q-gains (14% lFL vs. 36% sFL; p = 0.0003). Although rare in lFL, gains in 18q21 were associated with inferior progression-free survival (PFS). The mutational landscape of lFL and sFL included typical genetic lesions. However, ARID1A mutations were significantly more often detected in sFL (29%) compared to lFL (6%, p = 0.0001). In BCL2 + FL mutations in KMT2D, BCL2, ABL2, IGLL5 and ARID1A were enriched, while STAT6 mutations more frequently occurred in BCL2- FL. Although the landscape of lFL and sFL showed overlapping features, molecular profiling revealed novel insights and identified gains in 18q21 as prognostic marker in lFL.
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页码:2058 / 2065
页数:7
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