EGR2 mutations define a new clinically aggressive subgroup of chronic lymphocytic leukemia

Young, Emma; Noerenberg, Daniel; Mansouri, Larry; Ljungström, Viktor; Frick, Mareike; Sutton, La.; Blakemore, Stuart; Galan-Sousa, Joel; Plevová, Karla; Baliakas, Panagiotis; Rossi, Davide; Clifford, Ruth; Roos‐Weil, Damien; Navrkalová, Veronika; Dörken, Bernd; Schmitt, Clemens A.; Smedby, Ke.; Juliusson, Gunnar; Giacopelli, Brian; Blachly, JS; Belessi, Chrysoula; Panagiotidis, Panagiotis; Chiorazzi, Nicholas; Davi, Frédéric; Langerak, A. W.; Oscier, David; Schuh, Anna; Gaïdano, Gianluca; Ghia, Paolo; Xu, Wei; Fan, Lei; Bernard, Olivier A.; Nguyen‐Khac, Florence; Rassenti, Laura Z.; Li, J; Tj, Kipps; Stamatopoulos, Kostas; Pospı́šilová, Šárka; Zenz, Thorsten; Cc, Oakes; Strefford, Jonathan C.; Rosenquist, Richard; Damm, Frédérik

doi:10.1038/leu.2016.359

Cited by 49 publications

(46 citation statements)

References 57 publications

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“…CLL4 represents an ideal candidate for such an analysis, with expansive clinical and biological description [8, 12, 13, 17, 21, 24, 26, 29, 31-33, 40, 41] and protracted clinical follow-up. Our study confirms previous studies incorporating samples from this patient cohort showing the impact of TP53ab on PFS and OS in MVA, SF3B1, EGR2 [25,26], RPS15 [1,24] and NFKBIE [25,28,42] mutations on OS in univariate analysis, with SF3B1 and EGR2 mutations retained as independent markers of OS in MVA.…”

Section: Discussionsupporting

confidence: 90%

“…The trial demonstrated superior response rates and progression-free survival (PFS) for FC-treated patients compared with those patients treated with FDR or CHL. Previous genomic analysis of this trial has shown TP53 [8], SF3B1 [17], NOTCH1 (coding [17] and non-coding [21]), ATM plus del(11q) [12] and EGR2 [26] lesions to have prognostic significance in multivariate analysis (MVA) and of RPS15 [24] in univariate analysis. The importance of data from CLL4 may be questioned given the studies showing the superior efficacy of FC plus an anti-CD20 antibody (FCR) compared with chemotherapy alone, with the exception of patients with a NOTCH1 mutation [20], and emerging data suggesting the superiority of novel agents compared with chemotherapy-based regimens.…”

Section: Introductionmentioning

confidence: 78%

“…In particular, next generation sequencing of large patient cohorts has led to the discovery of These authors contributed equally: Anna Schuh, Jonathan C. Strefford recurring genomic mutations that cluster into distinct biological signalling pathways. Mutations of specific genes including TP53 [4][5][6][7][8][9][10], ATM [9,[11][12][13][14], BIRC3 [9,15,16], SF3B1 [9,[17][18][19][20], NOTCH1 [1,9,15,17,[20][21][22][23], RPS15 [2,24], EGR2 [25,26] and KRAS [27,28] are associated with poorer outcome, especially shorter time to first treatment or overall survival (OS). However, numerous factors influence the clinical significance of a driver mutation in an individual patient.…”

Section: Introductionmentioning

confidence: 99%

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Clinical significance of TP53, BIRC3, ATM and MAPK-ERK genes in chronic lymphocytic leukaemia: data from the randomised UK LRF CLL4 trial

et al. 2020

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Despite advances in chronic lymphocytic leukaemia (CLL) treatment, globally chemotherapy remains a central treatment modality, with chemotherapy trials representing an invaluable resource to explore disease-related/genetic features contributing to long-term outcomes. In 499 LRF CLL4 cases, a trial with >12 years follow-up, we employed targeted resequencing of 22 genes, identifying 623 mutations. After background mutation rate correction, 11/22 genes were recurrently mutated at frequencies between 3.6% (NFKBIE) and 24% (SF3B1). Mutations beyond Sanger resolution (<12% VAF) were observed in all genes, with KRAS mutations principally composed of these low VAF variants. Firstly, employing orthogonal approaches to confirm <12% VAF TP53 mutations, we assessed the clinical impact of TP53 clonal architecture. Whilst ≥ 12% VAF TP53mut cases were associated with reduced PFS and OS, we could not demonstrate a difference between <12% VAF TP53 mutations and either wild type or ≥12% VAF TP53mut cases. Secondly, we identified biallelic BIRC3 lesions (mutation and deletion) as an independent marker of inferior PFS and OS. Finally, we observed that mutated MAPK-ERK genes were independent markers of poor OS in multivariate survival analysis. In conclusion, our study supports using targeted resequencing of expanded gene panels to elucidate the prognostic impact of gene mutations.

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Section: Discussionsupporting

confidence: 90%

Section: Introductionmentioning

confidence: 78%

Section: Introductionmentioning

confidence: 99%

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Clinical significance of TP53, BIRC3, ATM and MAPK-ERK genes in chronic lymphocytic leukaemia: data from the randomised UK LRF CLL4 trial

et al. 2020

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“…This division between groups was used to perform the inter-group comparisons and the classification for the predictive analysis. The separation for the predictive analysis was made based on the assumption that, for the RNAseq analysis, patients with mutated EGR2 gene have a good prognosis [26] and, for the WES analysis, the patients with unmutated the IGVH gene are characterized as stable [27].…”

Section: Figure 1 Integrated Profile Creation Processmentioning

confidence: 99%

Developing an Integrated Genomic Profile for Cancer Patients with the Use of NGS Data

2019

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Next Generation Sequencing (NGS) technologies has revolutionized genomics data research by facilitating high-throughput sequencing of genetic material that comes from different sources, such as Whole Exome Sequencing (WES) and RNA Sequencing (RNAseq). The exploitation and integration of this wealth of heterogeneous sequencing data remains a major challenge. There is a clear need for approaches that attempt to process and combine the aforementioned sources in order to create an integrated profile of a patient that will allow us to build the complete picture of a disease. This work introduces such an integrated profile using Chronic Lymphocytic Leukemia (CLL) as the exemplary cancer type. The approach described in this paper links the various NGS sources with the patients’ clinical data. The resulting profile efficiently summarizes the large-scale datasets, links the results with the clinical profile of the patient and correlates indicators arising from different data types. With the use of state-of-the-art machine learning techniques and the association of the clinical information with these indicators, which served as the feature pool for the classification, it has been possible to build efficient predictive models. To ensure reproducibility of the results, open data were exclusively used in the classification assessment. The final goal is to design a complete genomic profile of a cancer patient. The profile includes summarization and visualization of the results of WES and RNAseq analysis (specific variants and significantly expressed genes, respectively) and the clinical profile, integration/comparison of these results and a prediction regarding the disease trajectory. Concluding, this work has managed to produce a comprehensive clinico-genetic profile of a patient by successfully integrating heterogeneous data sources. The proposed profile can contribute to the medical research providing new possibilities in personalized medicine and prognostic views.

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“…Several molecular studies have identified a set of genes, including NOTCH1, SF3B1 BIRC3, RSP15, and EGR2, as novel molecular biomarkers that account, at least in part, for chemorefractoriness in addition to TP53 disruption. These genetic aberrations appear to be mutually exclusive with disruption of TP53, at least in most cases, indicating that multiple alternative pathways can lead to CIT failure [11,[20][21][22][23]. In particular, in the case of FCR, mutations of BIRC3 (Baculoviral IAP Repeat Containing 3) stand out as a novel predictor of treatment failure.…”

Section: Molecular Abnormalities Of Patients Failing Citmentioning

confidence: 99%

An update on: molecular genetics of high-risk chronic lymphocytic leukemia

Moia

Patriarca

Deambrogi

et al. 2019

Expert Review of Hematology

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Introduction: During the past few years, new genomic approaches have elucidated the molecular genetics of chronic lymphocytic leukemia (CLL) to a large extent. As a consequence, specific high-risk genetic features of the disease, e.g. TP53 disruption, have become the backbone of the treatment algorithm for CLL and serve as robust biomarkers for a precision medicine approach to this leukemia. Areas covered: This review covers the genetics of CLL and highlights the translational implications of molecular biomarkers that characterize patients with a high risk of disease progression. Knowledge of the genetic landscape of CLL has allowed the identification of the main molecular features associated with chemo-refractoriness, as well as resistance to BCR inhibitors and BCL2 inhibitors. The molecular basis of Richter transformation has also been characterized. Expert opinion: The term 'high risk CLL' has been changing over time, and might be subject to further changes in the future. With the advent of new therapeutic strategies targeting pathogenetic pathways of the disease, the definition is shifting from the historical view of refractoriness to chemoimmunotherapy, to refractoriness to BCR inhibitors and/or to BCL2 inhibitors. Patients failing these novel medicines are those for whom new therapeutic approaches are still highly needed.

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EGR2 mutations define a new clinically aggressive subgroup of chronic lymphocytic leukemia

Cited by 49 publications

References 57 publications

Clinical significance of TP53, BIRC3, ATM and MAPK-ERK genes in chronic lymphocytic leukaemia: data from the randomised UK LRF CLL4 trial

Clinical significance of TP53, BIRC3, ATM and MAPK-ERK genes in chronic lymphocytic leukaemia: data from the randomised UK LRF CLL4 trial

Developing an Integrated Genomic Profile for Cancer Patients with the Use of NGS Data

An update on: molecular genetics of high-risk chronic lymphocytic leukemia

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