Focal structural variants revealed by whole genome sequencing disrupt the histone demethylase KDM4C in B-cell lymphomas

被引：2

作者：

Lopez, Cristina ^{[1
,2
,3
]}

Schleussner, Nikolai ^{[4
,5
,6
]}

Bernhart, Stephan H. ^{[7
,8
,9
]}

Kleinheinz, Kortine ^{[10
]}

Sungalee, Stephanie ^{[11
]}

Sczakiel, Henrike L. ^{[4
,5
,6
]}

Kretzmer, Helene ^{[7
,8
,9
,12
]}

Toprak, Umut H. ^{[13
,14
,15
]}

Glaser, Selina ^{[1
,2
]}

Wagener, Rabea ^{[1
,2
,3
]}

Ammerpohl, Ole ^{[1
,2
,3
]}

Bens, Susanne ^{[1
,2
,3
]}

Giefing, Maciej ^{[3
,16
]}

Sanchez, Juan C. Gonzalez ^{[17
]}

Apic, Gordana ^{[17
]}

Huebschmann, Daniel ^{[18
,19
,20
]}

Janz, Martin ^{[4
,5
,6
]}

Kreuz, Markus ^{[21
]}

Mottok, Anja ^{[1
,2
]}

Mueller, Judith M. ^{[22
,23
]}

Seufert, Julian ^{[13
]}

Hoffmann, Steve ^{[7
,8
,9
,24
]}

Korbel, Jan O. ^{[11
]}

Russell, Robert B. ^{[17
]}

Schuele, Roland ^{[22
,23
,25
]}

Truemper, Lorenz ^{[26
]}

Klapper, Wolfram ^{[27
]}

Radlwimmer, Bernhard ^{[28
]}

Lichter, Peter ^{[28
]}

Kueppers, Ralf ^{[29
,30
]}

Schlesner, Matthias ^{[13
,31
]}

Mathas, Stephan ^{[4
,5
,6
]}

Siebert, Reiner ^{[1
,2
,3
]}

机构：

[1] Ulm Univ, Inst Human Genet, Ulm, Germany

[2] Ulm Univ, Med Ctr, Ulm, Germany

[3] Univ Kiel, Inst Human Genet, Kiel, Germany

[4] Max Delbruck Ctr Mol Med, Helmholtz Assoc MDC, Berlin, Germany

[5] Charite Univ Med Berlin, Hematol Oncol & Tumor Immunol, Berlin, Germany

[6] Expt & Clin Res Ctr, MDC & Charite, Berlin, Germany

[7] Univ Leipzig, Interdisciplinary Ctr Bioinformat, Leipzig, Germany

[8] Univ Leipzig, Dept Comp, Bioinformat Grp, Leipzig, Germany

[9] Univ Leipzig, LIFE Res Ctr Civilizat Dis, Transcriptome Bioinformat, Leipzig, Germany

[10] Heidelberg Univ, Inst Pharm & Mol Biotechnol & Bioquant, Dept Bioinformat & Funct Genom, Heidelberg, Germany

[11] EMBL Heidelberg, Genome Biol Unit, Heidelberg, Germany

[12] Max Planck Inst Mol Genet, Dept Genome Regulat, Berlin, Germany

[13] German Canc Res Ctr, Bioinformat & Omics Data Analyt B240, Heidelberg, Germany

[14] Heidelberg Univ, Fac Biosci, Heidelberg, Germany

[15] German Canc Res Ctr, Hopp Childrens Canc Ctr NCT Heidelberg KiTZ, Div Neuroblastoma Genom B087, Heidelberg, Germany

[16] Polish Acad Sci, Inst Human Genet, Poznan, Poland

[17] Heidelberg Univ, BioQuant & Biochem Zentrum Heidelberg BZH, Heidelberg, Germany

[18] German Canc Consortium DKTK, Heidelberg, Germany

[19] Heidelberg Inst Stem Cell Technol & Expt Med HIST, Heidelberg, Germany

[20] German Canc Res Ctr, Natl Ctr Tumor Dis NCT, Mol Precis Oncol Program, Computat Oncol, Heidelberg, Germany

[21] Inst Med Informat Stat & Epidemiol, Leipzig, Germany

[22] Albert Ludwigs Univ Freiburg, Klin Urol, Freiburg, Germany

[23] Albert Ludwigs Univ Freiburg, Zentrale Klin Forsch, Freiburg, Germany

[24] Leibniz Inst Ageing Fritz Lipmann Inst FLI, Computat Biol, Jena, Germany

[25] Albert Ludwigs Univ, BIOSS Ctr Biol Signalling Studies, Freiburg, Germany

[26] Georg August Univ Gottingen, Dept Hematol & Oncol, Gottingen, Germany

[27] Univ Kiel, Hematopathol Sect, Kiel, Germany

[28] German Canc Res Ctr, Div Mol Genet, Heidelberg, Germany

[29] Univ Duisburg Essen, Inst Cell Biol Canc Res, Essen, Germany

[30] German Canc Consortium DKTK, Essen, Germany

[31] Augsburg Univ, Biomed Informat Data Min & Data Analyt, Augsburg, Germany

来源：

HAEMATOLOGICA | 2023年 / 108卷 / 02期

关键词：

MUTATIONS; BURKITT; EXOME; PATHOGENESIS; LANDSCAPE; GENES;

D O I：

10.3324/haematol.2021.280005

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Histone methylation-modifiers, such as EZH2 and KMT2D, are recurrently altered in B-cell lymphomas. To comprehensively describe the landscape of alterations affecting genes encoding histone methylation-modifiers in lymphomagenesis we investigated whole genome and transcriptome data of 186 mature B-cell lymphomas sequenced in the ICGC MMML-Seq project. Besides confirming common alterations of KMT2D (47% of cases), EZH2 (17%), SETD1B (5%), PRDM9 (4%), KMT2C (4%), and SETD2 (4%), also identified by prior exome or RNA-sequencing studies, we here found recurrent alterations to KDM4C in chromosome 9p24, encoding a histone demethylase. Focal structural variation was the main mechanism of KDM4C alterations, and was independent from 9p24 amplification. We also identified KDM4C alterations in lymphoma cell lines including a focal homozygous deletion in a classical Hodgkin lymphoma cell line. By integrating RNA-sequencing and genome sequencing data we predict that KDM4C structural variants result in loss-of-function. By functional reconstitution studies in cell lines, we provide evidence that KDM4C can act as a tumor suppressor. Thus, we show that identification of structural variants in whole genome sequencing data adds to the comprehensive description of the mutational landscape of lymphomas and, moreover, establish KDM4C as a putative tumor suppressive gene recurrently altered in subsets of B-cell derived lymphomas.

引用

页码：543 / 554

页数：12

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