Your search keyword '"Bernd Heinz"' showing total 35 results

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

Author

Kalmbach, Sabrina, Grau, Michael, Zapukhlyak, Myroslav, Leich, Ellen, Jurinovic, Vindi, Hoster, Eva, Staiger, Annette M., Kurz, Katrin S., Weigert, Oliver, Gaitzsch, Erik, Passerini, Verena, Engelhard, Marianne, Herfarth, Klaus, Beiske, Klaus, Micci, Francesca, Möller, Peter, Bernd, Heinz-Wolfram, Feller, Alfred C., Klapper, Wolfram, Stein, Harald, Hansmann, Martin-Leo, Hartmann, Sylvia, Dreyling, Martin, Holte, Harald, Lenz, Georg, Rosenwald, Andreas, Ott, German, and Horn, Heike

Abstract

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 BCL2translocation-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, ARID1Amutations were significantly more often detected in sFL (29%) compared to lFL (6%, p= 0.0001). In BCL2+ FL mutations in KMT2D, BCL2, ABL2, IGLL5and ARID1Awere enriched, while STAT6mutations 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.

Published

2023

2. Integrative genomic and transcriptomic analysis in plasmablastic lymphoma identifies disruption of key regulatory pathways

Author

Witte, Hanno M., Künstner, Axel, Hertel, Nadine, Bernd, Heinz-Wolfram, Bernard, Veronica, Stölting, Stephanie, Merz, Hartmut, von Bubnoff, Nikolas, Busch, Hauke, Feller, Alfred C., and Gebauer, Niklas

Abstract

Plasmablastic lymphoma (PBL) represents a clinically heterogeneous subtype of aggressive B-cell non-Hodgkin lymphoma. Targeted-sequencing studies and a single-center whole-exome sequencing (WES) study in HIV-positive patients recently revealed several genes associated with PBL pathogenesis; however, the global mutational landscape and transcriptional profile of PBL remain elusive. To inform on disease-associated mutational drivers, mutational patterns, and perturbed pathways in HIV-positive and HIV-negative PBL, we performed WES and transcriptome sequencing (RNA-sequencing) of 33 PBL tumors. Integrative analysis of somatic mutations and gene expression profiles was performed to acquire insights into the divergent genotype–phenotype correlation in Epstein-Barr virus–positive (EBV+) and EBV– PBL. We describe a significant accumulation of mutations in the JAK signal transducer and transcription activator (OSMR, STAT3, PIM1, and SOCS1), as well as receptor tyrosine-kinase RAS (ERBB3, NRAS, PDGFRB, and NTRK) pathways. We provide further evidence of frequent perturbances of NF-κB signaling (NFKB2 and BTK). Induced pathways, identified by RNA-sequencing, closely resemble the mutational profile regarding alterations accentuated in interleukin-6/JAK/STAT signaling, NF-κB activity, and MYC signaling. Moreover, class I major histocompatibility complex–mediated antigen processing and cell cycle regulation were significantly affected by EBV status. An almost exclusive upregulation of phosphatidylinositol 3-kinase/AKT/mTOR signaling in EBV+ PBL and a significantly induced expression of NTRK3 in concert with recurrent oncogenic mutations in EBV– PBL hint at a specific therapeutically targetable mechanism in PBL subgroups. Our characterization of a mutational and transcriptomic landscape in PBL, distinct from that of diffuse large B-cell lymphoma and multiple myeloma, substantiates the pathobiological independence of PBL in the spectrum of B-cell malignancies and thereby refines the taxonomy for aggressive lymphomas.

Published

2022

3. Integrative genomic and transcriptomic analysis in plasmablastic lymphoma identifies disruption of key regulatory pathways

Author

Witte, Hanno M., Künstner, Axel, Hertel, Nadine, Bernd, Heinz-Wolfram, Bernard, Veronica, Stölting, Stephanie, Merz, Hartmut, von Bubnoff, Nikolas, Busch, Hauke, Feller, Alfred C., and Gebauer, Niklas

Abstract

Plasmablastic lymphoma (PBL) represents a clinically heterogeneous subtype of aggressive B-cell non-Hodgkin lymphoma. Targeted-sequencing studies and a single-center whole-exome sequencing (WES) study in HIV-positive patients recently revealed several genes associated with PBL pathogenesis; however, the global mutational landscape and transcriptional profile of PBL remain elusive. To inform on disease-associated mutational drivers, mutational patterns, and perturbed pathways in HIV-positive and HIV-negative PBL, we performed WES and transcriptome sequencing (RNA-sequencing) of 33 PBL tumors. Integrative analysis of somatic mutations and gene expression profiles was performed to acquire insights into the divergent genotype–phenotype correlation in Epstein-Barr virus–positive (EBV+) and EBV–PBL. We describe a significant accumulation of mutations in the JAK signal transducer and transcription activator (OSMR, STAT3, PIM1,and SOCS1), as well as receptor tyrosine-kinase RAS (ERBB3, NRAS, PDGFRB,and NTRK) pathways. We provide further evidence of frequent perturbances of NF-κB signaling (NFKB2and BTK). Induced pathways, identified by RNA-sequencing, closely resemble the mutational profile regarding alterations accentuated in interleukin-6/JAK/STAT signaling, NF-κB activity, and MYC signaling. Moreover, class I major histocompatibility complex–mediated antigen processing and cell cycle regulation were significantly affected by EBV status. An almost exclusive upregulation of phosphatidylinositol 3-kinase/AKT/mTOR signaling in EBV+PBL and a significantly induced expression of NTRK3in concert with recurrent oncogenic mutations in EBV–PBL hint at a specific therapeutically targetable mechanism in PBL subgroups. Our characterization of a mutational and transcriptomic landscape in PBL, distinct from that of diffuse large B-cell lymphoma and multiple myeloma, substantiates the pathobiological independence of PBL in the spectrum of B-cell malignancies and thereby refines the taxonomy for aggressive lymphomas.

Published

2022

4. Localized- and advanced-stage follicular lymphomas differ in their gene expression profiles

Author

Staiger, Annette M., Hoster, Eva, Jurinovic, Vindi, Winter, Stefan, Leich, Ellen, Kalla, Claudia, Möller, Peter, Bernd, Heinz-Wolfram, Feller, Alfred C., Koch, Karoline, Klapper, Wolfram, Stein, Harald, Hansmann, Martin-Leo, Hartmann, Sylvia, Dreyling, Martin, Weigert, Oliver, Hiddemann, Wolfgang, Herfarth, Klaus, Rosenwald, Andreas, Engelhard, Marianne, Ott, German, and Horn, Heike

Abstract

The genetic background of follicular lymphomas (FLs) diagnosed in advanced clinical stages III/IV, and which are frequently characterized by t(14;18), has been substantially unraveled. Molecular features, as exemplified in the clinicogenetic risk model m7FLIPI, are important tools in risk stratification. In contrast, little information is available concerning localized-stage FL (clinical stages I/II), which accounts for ~20% of newly diagnosed FL in which the detection rate of t(14;18) is only ~50%. To investigate the genetic background of localized-stage FL, patient cohorts with advanced-stage FL or localized-stage FL, uniformly treated within phase 3 trials of the German Low-Grade Lymphoma Study Group, were comparatively analyzed. Targeted gene expression (GE) profiling of 184 genes using nCounter technology was performed in 110 localized-stage and 556 advanced-stage FL patients. By penalized Cox regression, a prognostic GE signature could not be identified in patients with advanced-stage FL, consistent with results from global tests and univariate regression. In contrast, it was possible to define robust GE signatures discriminating localized-stage and advanced-stage FL (area under the curve, 0.98) by penalized logistic regression. Of note, 3% of samples harboring an “advanced-stage signature” in the localized-stage cohort exhibited inferior failure-free survival (hazard ratio [HR], 7.1; P = .0003). Likewise, in the advanced-stage cohort, 7% of samples with a “localized-stage signature” had prolonged failure-free survival (HR, 2.3; P = .017) and overall survival (HR, 3.4; P = .072). These data support the concept of a biological difference between localized-stage and advanced-stage FL that might contribute to the superior outcome of localized FL.

Published

2020

5. Localized- and advanced-stage follicular lymphomas differ in their gene expression profiles

Author

Staiger, Annette M., Hoster, Eva, Jurinovic, Vindi, Winter, Stefan, Leich, Ellen, Kalla, Claudia, Möller, Peter, Bernd, Heinz-Wolfram, Feller, Alfred C., Koch, Karoline, Klapper, Wolfram, Stein, Harald, Hansmann, Martin-Leo, Hartmann, Sylvia, Dreyling, Martin, Weigert, Oliver, Hiddemann, Wolfgang, Herfarth, Klaus, Rosenwald, Andreas, Engelhard, Marianne, Ott, German, and Horn, Heike

Abstract

The genetic background of follicular lymphomas (FLs) diagnosed in advanced clinical stages III/IV, and which are frequently characterized by t(14;18), has been substantially unraveled. Molecular features, as exemplified in the clinicogenetic risk model m7FLIPI, are important tools in risk stratification. In contrast, little information is available concerning localized-stage FL (clinical stages I/II), which accounts for ∼20% of newly diagnosed FL in which the detection rate of t(14;18) is only ∼50%. To investigate the genetic background of localized-stage FL, patient cohorts with advanced-stage FL or localized-stage FL, uniformly treated within phase 3 trials of the German Low-Grade Lymphoma Study Group, were comparatively analyzed. Targeted gene expression (GE) profiling of 184 genes using nCounter technology was performed in 110 localized-stage and 556 advanced-stage FL patients. By penalized Cox regression, a prognostic GE signature could not be identified in patients with advanced-stage FL, consistent with results from global tests and univariate regression. In contrast, it was possible to define robust GE signatures discriminating localized-stage and advanced-stage FL (area under the curve, 0.98) by penalized logistic regression. Of note, 3% of samples harboring an “advanced-stage signature” in the localized-stage cohort exhibited inferior failure-free survival (hazard ratio [HR], 7.1; P= .0003). Likewise, in the advanced-stage cohort, 7% of samples with a “localized-stage signature” had prolonged failure-free survival (HR, 2.3; P= .017) and overall survival (HR, 3.4; P= .072). These data support the concept of a biological difference between localized-stage and advanced-stage FL that might contribute to the superior outcome of localized FL.

Published

2020

6. Clinical Impact of the Cell-of-Origin Classification and the MYC/ BCL2 Dual Expresser Status in Diffuse Large B-Cell Lymphoma Treated Within Prospective Clinical Trials of the German High-Grade Non-Hodgkin's Lymphoma Study Group.

Author

Staiger, Annette M., Ziepert, Marita, Horn, Heike, Scott, David W., Barth, Thomas F. E., Bernd, Heinz-Wolfram, Feller, Alfred C., Klapper, Wolfram, Szczepanowski, Monika, Hummel, Michael, Stein, Harald, Lenze, Dido, Hansmann, Martin-Leo, Hartmann, Sylvia, Möoller, Peter, Cogliatti, Sergio, Lenz, Georg, Trümper, Lorenz, Löffer, Markus, and Schmitz, Norbert

Published

2017

7. Prognostic Value of Ki-67 Index, Cytology, and Growth Pattern in Mantle-Cell Lymphoma: Results From Randomized Trials of the European Mantle Cell Lymphoma Network.

Author

Hoster, Eva, Rosenwald, Andreas, Berger, Françoise, Bernd, Heinz-Wolfram, Hartmann, Sylvia, Loddenkemper, Christoph, Barth, Thomas F. E., Brousse, Nicole, Pileri, Stefano, Rymkiewicz, Grzegorz, Kodet, Roman, Stilgenbauer, Stephan, Forstpointner, Roswitha, Thieblemont, Catherine, Hallek, Michael, Coiffier, Bertrand, Vehling-Kaiser, Ursula, Bouabdallah, Réda, Kanz, Lothar, and Pfreundschuh, Michael

Published

2016

8. The prognostic impact of variant histology in nodular lymphocyte-predominant Hodgkin lymphoma: a report from the German Hodgkin Study Group (GHSG)

Author

Hartmann, Sylvia, Eichenauer, Dennis A., Plütschow, Annette, Mottok, Anja, Bob, Roshanak, Koch, Karoline, Bernd, Heinz-Wolfram, Cogliatti, Sergio, Hummel, Michael, Feller, Alfred C., Ott, German, Möller, Peter, Rosenwald, Andreas, Stein, Harald, Hansmann, Martin-Leo, Engert, Andreas, and Klapper, Wolfram

Abstract

Nodular lymphocyte–predominant Hodgkin lymphoma (NLPHL) accounts for approximately 5% of all Hodgkin lymphoma cases. The aim of this study was to evaluate the prognostic implication of histopathologic NLPHL variants. Biopsies of 423 NLPHL patients treated within 9 prospective clinical trials performed by the German Hodgkin Study Group were classified as tumor cell–rich cases (n = 10), typical NLPHL (n = 308), or histopathologic variants (n = 105). Histopathologic variants were characterized by the presence of lymphoma cells outside the B-cell nodules or B-cell depletion of the microenvironment. Compared with typical NLPHL, histopathologic variants were associated with advanced disease (29.5% vs 14.6%, P = .0012) and a higher relapse rate (18.1% vs 6.5% at 5 years, P = .0009). Variant histology represented an independent prognostic factor (odds ratio = 2.955) in a multivariate model of progression/relapse. A prognostic score, including the risk factors variant histopathologic growth pattern, low serum albumin, and male gender, was derived from this model and allowed the definition of 3 distinct risk groups. NLPHL patients presenting with histopathologic variants have a poorer outcome compared with those showing typical histology. The newly developed prognostic score combining histologic and clinical features allows allocating NLPHL patients to defined risk groups.

Published

2013

9. The prognostic impact of variant histology in nodular lymphocyte-predominant Hodgkin lymphoma: a report from the German Hodgkin Study Group (GHSG)

Author

Hartmann, Sylvia, Eichenauer, Dennis A., Plütschow, Annette, Mottok, Anja, Bob, Roshanak, Koch, Karoline, Bernd, Heinz-Wolfram, Cogliatti, Sergio, Hummel, Michael, Feller, Alfred C., Ott, German, Möller, Peter, Rosenwald, Andreas, Stein, Harald, Hansmann, Martin-Leo, Engert, Andreas, and Klapper, Wolfram

Abstract

Nodular lymphocyte–predominant Hodgkin lymphoma (NLPHL) accounts for approximately 5% of all Hodgkin lymphoma cases. The aim of this study was to evaluate the prognostic implication of histopathologic NLPHL variants. Biopsies of 423 NLPHL patients treated within 9 prospective clinical trials performed by the German Hodgkin Study Group were classified as tumor cell–rich cases (n = 10), typical NLPHL (n = 308), or histopathologic variants (n = 105). Histopathologic variants were characterized by the presence of lymphoma cells outside the B-cell nodules or B-cell depletion of the microenvironment. Compared with typical NLPHL, histopathologic variants were associated with advanced disease (29.5% vs 14.6%, P= .0012) and a higher relapse rate (18.1% vs 6.5% at 5 years, P= .0009). Variant histology represented an independent prognostic factor (odds ratio = 2.955) in a multivariate model of progression/relapse. A prognostic score, including the risk factors variant histopathologic growth pattern, low serum albumin, and male gender, was derived from this model and allowed the definition of 3 distinct risk groups. NLPHL patients presenting with histopathologic variants have a poorer outcome compared with those showing typical histology. The newly developed prognostic score combining histologic and clinical features allows allocating NLPHL patients to defined risk groups.

Published

2013

10. MYC status in concert with BCL2 and BCL6 expression predicts outcome in diffuse large B-cell lymphoma

Author

Horn, Heike, Ziepert, Marita, Becher, Claudia, Barth, Thomas F.E., Bernd, Heinz-Wolfram, Feller, Alfred C., Klapper, Wolfram, Hummel, Michael, Stein, Harald, Hansmann, Martin-Leo, Schmelter, Christopher, Möller, Peter, Cogliatti, Sergio, Pfreundschuh, Michael, Schmitz, Norbert, Trümper, Lorenz, Siebert, Reiner, Loeffler, Markus, Rosenwald, Andreas, and Ott, German

Abstract

MYC rearrangements occur in 5% to 10% of diffuse large B-cell lymphomas (DLBCL) and confer an increased risk to cyclophosphamide, hydroxydaunorubicin, oncovin, and prednisone (CHOP) and rituximab (R)–CHOP treated patients. We investigated the prognostic relevance of MYC-, BCL2- and BCL6-rearrangements and protein expression in a prospective randomized trial. Paraffin-embedded tumor samples from 442 de novo DLBCL treated within the RICOVER study of the German High-Grade Non-Hodgkin Lymphoma Study Group (DSHNHL) were investigated using immunohistochemistry and fluorescence in situ hybridization (FISH) to detect protein expression and breaks of MYC, BCL2, and BCL6. Rearrangements of MYC, BCL2, and BCL6were detected in 8.8%, 13.5%, and 28.7%, respectively. Protein overexpression of MYC (>40%) was encountered in 31.8% of tumors; 79.6% and 82.8% of tumors expressed BCL2 and BCL6, respectively. MYCtranslocations, MYChigh, BCL2high, and BCL6low protein expressions were associated with inferior survival. In multivariate Cox regression modeling, protein expression patterns of MYC, BCL2 and BCL6, and MYCrearrangements were predictive of outcome and provided prognostic information independent of the International Prognostic Index (IPI) for overall survival and event-free survival. A combined immunohistochemical or FISH/immunohistochemical score predicts outcome in DLBCL patients independent of the IPI and identifies a subset of 15% of patients with dismal prognosis in the high-risk IPI group following treatment with R-CHOP. Registered at http://www.cancer.gov/clinicaltrials: RICOVER trial of the DSHNHL is NCT 00052936.

Published

2013

11. MYC status in concert with BCL2 and BCL6 expression predicts outcome in diffuse large B-cell lymphoma

Author

Horn, Heike, Ziepert, Marita, Becher, Claudia, Barth, Thomas F. E., Bernd, Heinz-Wolfram, Feller, Alfred C., Klapper, Wolfram, Hummel, Michael, Stein, Harald, Hansmann, Martin-Leo, Schmelter, Christopher, Möller, Peter, Cogliatti, Sergio, Pfreundschuh, Michael, Schmitz, Norbert, Trümper, Lorenz, Siebert, Reiner, Loeffler, Markus, Rosenwald, Andreas, and Ott, German

Abstract

MYC rearrangements occur in 5% to 10% of diffuse large B-cell lymphomas (DLBCL) and confer an increased risk to cyclophosphamide, hydroxydaunorubicin, oncovin, and prednisone (CHOP) and rituximab (R)–CHOP treated patients. We investigated the prognostic relevance of MYC-, BCL2- and BCL6-rearrangements and protein expression in a prospective randomized trial. Paraffin-embedded tumor samples from 442 de novo DLBCL treated within the RICOVER study of the German High-Grade Non-Hodgkin Lymphoma Study Group (DSHNHL) were investigated using immunohistochemistry and fluorescence in situ hybridization (FISH) to detect protein expression and breaks of MYC, BCL2, and BCL6. Rearrangements of MYC, BCL2, and BCL6 were detected in 8.8%, 13.5%, and 28.7%, respectively. Protein overexpression of MYC (>40%) was encountered in 31.8% of tumors; 79.6% and 82.8% of tumors expressed BCL2 and BCL6, respectively. MYC translocations, MYChigh, BCL2high, and BCL6low protein expressions were associated with inferior survival. In multivariate Cox regression modeling, protein expression patterns of MYC, BCL2 and BCL6, and MYC rearrangements were predictive of outcome and provided prognostic information independent of the International Prognostic Index (IPI) for overall survival and event-free survival. A combined immunohistochemical or FISH/immunohistochemical score predicts outcome in DLBCL patients independent of the IPI and identifies a subset of 15% of patients with dismal prognosis in the high-risk IPI group following treatment with R-CHOP. Registered at http://www.cancer.gov/clinicaltrials: RICOVER trial of the DSHNHL is NCT 00052936.

Published

2013

12. Immunoblastic morphology but not the immunohistochemical GCB/nonGCB classifier predicts outcome in diffuse large B-cell lymphoma in the RICOVER-60 trial of the DSHNHL

Author

Ott, German, Ziepert, Marita, Klapper, Wolfram, Horn, Heike, Szczepanowski, Monika, Bernd, Heinz-Wolfram, Thorns, Christoph, Feller, Alfred C., Lenze, Dido, Hummel, Michael, Stein, Harald, Müller-Hermelink, Hans-Konrad, Frank, Matthias, Hansmann, Martin-Leo, Barth, Thomas F. E., Möller, Peter, Cogliatti, Sergio, Pfreundschuh, Michael, Schmitz, Norbert, Trümper, Lorenz, Loeffler, Markus, and Rosenwald, Andreas

Abstract

The survival of diffuse large B-cell lymphoma patients varies considerably, reflecting the molecular diversity of tumors. In view of the controversy whether cytologic features, immunohistochemical markers or gene expression signatures may capture this molecular diversity, we investigated which features provide prognostic information in a prospective trial in the R-CHOP treatment era. Within the cohort of DLBCLs patients treated in the RICOVER-60 trial of the German High-Grade Lymphoma Study Group (DSHNHL), we tested the prognostic impact of IB morphology in 949 patients. The expression of immunohistochemical markers CD5, CD10, BCL2, BCL6, human leukocyte antigen (HLA)–DR, interferon regulatory factor-4/multiple myeloma-1 (IRF4/MUM1), and Ki-67 was assessed in 506 patients. Expression of the immunohistochemical markers tested was of modest, if any, prognostic relevance. Moreover, the Hans algorithm using the expression patterns of CD10, BCL6, and interferon regulatory factor-4/multiple myeloma-1 failed to show prognostic significance in the entire cohort as well as in patient subgroups. IB morphology, however, emerged as a robust, significantly adverse prognostic factor in multivariate analysis, and its diagnosis showed a good reproducibility among expert hematopathologists. We conclude, therefore, that IB morphology in DLBCL is likely to capture some of the adverse molecular alterations that are currently not detectable in a routine diagnostic setting, and that its recognition has significant prognostic power.

Published

2010

13. Immunoblastic morphology but not the immunohistochemical GCB/nonGCB classifier predicts outcome in diffuse large B-cell lymphoma in the RICOVER-60 trial of the DSHNHL

Author

Ott, German, Ziepert, Marita, Klapper, Wolfram, Horn, Heike, Szczepanowski, Monika, Bernd, Heinz-Wolfram, Thorns, Christoph, Feller, Alfred C., Lenze, Dido, Hummel, Michael, Stein, Harald, Müller-Hermelink, Hans-Konrad, Frank, Matthias, Hansmann, Martin-Leo, Barth, Thomas F.E., Möller, Peter, Cogliatti, Sergio, Pfreundschuh, Michael, Schmitz, Norbert, Trümper, Lorenz, Loeffler, Markus, and Rosenwald, Andreas

Abstract

The survival of diffuse large B-cell lymphoma patients varies considerably, reflecting the molecular diversity of tumors. In view of the controversy whether cytologic features, immunohistochemical markers or gene expression signatures may capture this molecular diversity, we investigated which features provide prognostic information in a prospective trial in the R-CHOP treatment era. Within the cohort of DLBCLs patients treated in the RICOVER-60 trial of the German High-Grade Lymphoma Study Group (DSHNHL), we tested the prognostic impact of IB morphology in 949 patients. The expression of immunohistochemical markers CD5, CD10, BCL2, BCL6, human leukocyte antigen (HLA)–DR, interferon regulatory factor-4/multiple myeloma-1 (IRF4/MUM1), and Ki-67 was assessed in 506 patients. Expression of the immunohistochemical markers tested was of modest, if any, prognostic relevance. Moreover, the Hans algorithm using the expression patterns of CD10, BCL6, and interferon regulatory factor-4/multiple myeloma-1 failed to show prognostic significance in the entire cohort as well as in patient subgroups. IB morphology, however, emerged as a robust, significantly adverse prognostic factor in multivariate analysis, and its diagnosis showed a good reproducibility among expert hematopathologists. We conclude, therefore, that IB morphology in DLBCL is likely to capture some of the adverse molecular alterations that are currently not detectable in a routine diagnostic setting, and that its recognition has significant prognostic power.

Published

2010

14. A cytomorphological and immunohistochemical profile of aggressive B-cell lymphoma: high clinical impact of a cumulative immunohistochemical outcome predictor score

Author

Höller, Sylvia, Horn, Heike, Lohr, Andreas, Mäder, Uwe, Katzenberger, Tiemo, Kalla, Jörg, Bernd, Heinz-Wolfram, Went, Philip, Ott, M., Müller-Hermelink, Hans, Rosenwald, Andreas, and Ott, German

Abstract

Abstract: We analyzed morphological and immunohistochemical features in 174 aggressive B-cell lymphomas of nodal and extranodal origin. Morphological features included presence or absence of a follicular component and cytologic criteria according to the Kiel classification, whereas immunohistochemical studies included expression of CD10, BCL-2, BCL-6, IRF4/MUM1, HLA-DR, p53, Ki-67 and the assessment of plasmacytoid differentiation. Patients were treated with a CHOP-like regimen. While the presence or absence of either CD10, BCL-6 and IRF4/MUM1 reactivity or plasmacytoid differentiation did not identify particular cytomorphologic or site-specific subtypes, we found that expression of CD10 and BCL-6, and a low reactivity for IRF4/MUM1 were favourable prognostic indicators. In contrast, BCL-2 expression and presence of a monotypic cytoplasmic immunoglobulin expression was associated with an unfavourable prognosis in univariate analyses. Meta-analysis of these data resulted in the development of a cumulative immunohistochemical outcome predictor score (CIOPS) enabling the recognition of four distinct prognostic groups. Multivariate analysis proved this score to be independent of the international prognostic index. Such a cumulative immunohistochemical scoring approach might provide a valuable alternative in the recognition of defined risk types of aggressive B-cell lymphomas.

Published

2009

15. Ki-67 as a prognostic marker in mantle cell lymphoma—consensus guidelines of the pathology panel of the European MCL Network

Author

Klapper, Wolfram, Hoster, Eva, Determann, Olaf, Oschlies, Ilske, van der Laak, Jeroen, Berger, Françoise, Bernd, Heinz, Cabeçadas, José, Campo, Elias, Cogliatti, Sergio, Hansmann, Martin, Kluin, Philip, Kodet, Roman, Krivolapov, Yuri, Loddenkemper, Christoph, Stein, Harald, Möller, Peter, Barth, Thomas, Müller-Hermelink, Konrad, Rosenwald, Andreas, Ott, German, Pileri, Stefano, Ralfkiaer, Elisabeth, Rymkiewicz, Grzegorz, van Krieken, Johan, Wacker, Hans, Unterhalt, Michael, Hiddemann, Wolfgang, and Dreyling, Martin

Abstract

Abstract: Mantle cell lymphoma (MCL) has a heterogeneous clinical course and is mainly an aggressive B cell non-Hodgkin lymphoma; however, there are some indolent cases The Ki-67 index, defined by the percentage of Ki-67-positive lymphoma cells on histopathological slides, has been shown to be a very powerful prognostic biomarker. The pathology panel of the European MCL Network evaluated methods to assess the Ki-67 index including stringent counting, digital image analysis, and estimation by eyeballing. Counting of 2 × 500 lymphoma cells is the gold standard to assess the Ki-67 index since this value has been shown to predict survival in prospective randomized trials of the European MCL Network. Estimation by eyeballing and digital image analysis showed a poor concordance with the gold standard (concordance correlation coefficients [CCC] between 0.29 and 0.61 for eyeballing and CCC of 0.24 and 0.37 for two methods of digital image analysis, respectively). Counting a reduced number of lymphoma cells (2 × 100 cells) showed high interobserver agreement (CCC = 0.74). Pitfalls of the Ki-67 index are discussed and guidelines and recommendations for assessing the Ki-67 index in MCL are given.

Published

2009

16. New insights into the biology and origin of mature aggressive B-cell lymphomas by combined epigenomic, genomic, and transcriptional profiling

Author

Martín-Subero, José I., Kreuz, Markus, Bibikova, Marina, Bentink, Stefan, Ammerpohl, Ole, Wickham-Garcia, Eliza, Rosolowski, Maciej, Richter, Julia, Lopez-Serra, Lidia, Ballestar, Esteban, Berger, Hilmar, Agirre, Xabier, Bernd, Heinz-Wolfram, Calvanese, Vincenzo, Cogliatti, Sergio B., Drexler, Hans G., Fan, Jian-Bing, Fraga, Mario F., Hansmann, Martin L., Hummel, Michael, Klapper, Wolfram, Korn, Bernhard, Küppers, Ralf, MacLeod, Roderick A. F., Möller, Peter, Ott, German, Pott, Christiane, Prosper, Felipe, Rosenwald, Andreas, Schwaenen, Carsten, Schübeler, Dirk, Seifert, Marc, Stürzenhofecker, Benjamin, Weber, Michael, Wessendorf, Swen, Loeffler, Markus, Trümper, Lorenz, Stein, Harald, Spang, Rainer, Esteller, Manel, Barker, David, Hasenclever, Dirk, and Siebert, Reiner

Abstract

Lymphomas are assumed to originate at different stages of lymphocyte development through chromosomal aberrations. Thus, different lymphomas resemble lymphocytes at distinct differentiation stages and show characteristic morphologic, genetic, and transcriptional features. Here, we have performed a microarray-based DNA methylation profiling of 83 mature aggressive B-cell non-Hodgkin lymphomas (maB-NHLs) characterized for their morphologic, genetic, and transcriptional features, including molecular Burkitt lymphomas and diffuse large B-cell lymphomas. Hierarchic clustering indicated that methylation patterns in maB-NHLs were not strictly associated with morphologic, genetic, or transcriptional features. By supervised analyses, we identified 56 genes de novo methylated in all lymphoma subtypes studied and 22 methylated in a lymphoma subtype–specific manner. Remarkably, the group of genes de novo methylated in all lymphoma subtypes was significantly enriched for polycomb targets in embryonic stem cells. De novo methylated genes in all maB-NHLs studied were expressed at low levels in lymphomas and normal hematopoietic tissues but not in nonhematopoietic tissues. These findings, especially the enrichment for polycomb targets in stem cells, indicate that maB-NHLs with different morphologic, genetic, and transcriptional background share a similar stem cell–like epigenetic pattern. This suggests that maB-NHLs originate from cells with stem cell features or that stemness was acquired during lymphomagenesis by epigenetic remodeling.

Published

2009

17. New insights into the biology and origin of mature aggressive B-cell lymphomas by combined epigenomic, genomic, and transcriptional profiling

Author

Martín-Subero, José I., Kreuz, Markus, Bibikova, Marina, Bentink, Stefan, Ammerpohl, Ole, Wickham-Garcia, Eliza, Rosolowski, Maciej, Richter, Julia, Lopez-Serra, Lidia, Ballestar, Esteban, Berger, Hilmar, Agirre, Xabier, Bernd, Heinz-Wolfram, Calvanese, Vincenzo, Cogliatti, Sergio B., Drexler, Hans G., Fan, Jian-Bing, Fraga, Mario F., Hansmann, Martin L., Hummel, Michael, Klapper, Wolfram, Korn, Bernhard, Küppers, Ralf, MacLeod, Roderick A.F., Möller, Peter, Ott, German, Pott, Christiane, Prosper, Felipe, Rosenwald, Andreas, Schwaenen, Carsten, Schübeler, Dirk, Seifert, Marc, Stürzenhofecker, Benjamin, Weber, Michael, Wessendorf, Swen, Loeffler, Markus, Trümper, Lorenz, Stein, Harald, Spang, Rainer, Esteller, Manel, Barker, David, Hasenclever, Dirk, and Siebert, Reiner

Abstract

Lymphomas are assumed to originate at different stages of lymphocyte development through chromosomal aberrations. Thus, different lymphomas resemble lymphocytes at distinct differentiation stages and show characteristic morphologic, genetic, and transcriptional features. Here, we have performed a microarray-based DNA methylation profiling of 83 mature aggressive B-cell non-Hodgkin lymphomas (maB-NHLs) characterized for their morphologic, genetic, and transcriptional features, including molecular Burkitt lymphomas and diffuse large B-cell lymphomas. Hierarchic clustering indicated that methylation patterns in maB-NHLs were not strictly associated with morphologic, genetic, or transcriptional features. By supervised analyses, we identified 56 genes de novo methylated in all lymphoma subtypes studied and 22 methylated in a lymphoma subtype–specific manner. Remarkably, the group of genes de novo methylated in all lymphoma subtypes was significantly enriched for polycomb targets in embryonic stem cells. De novo methylated genes in all maB-NHLs studied were expressed at low levels in lymphomas and normal hematopoietic tissues but not in nonhematopoietic tissues. These findings, especially the enrichment for polycomb targets in stem cells, indicate that maB-NHLs with different morphologic, genetic, and transcriptional background share a similar stem cell–like epigenetic pattern. This suggests that maB-NHLs originate from cells with stem cell features or that stemness was acquired during lymphomagenesis by epigenetic remodeling.

Published

2009

18. Molecular profiling of pediatric mature B-cell lymphoma treated in population-based prospective clinical trials

Author

Klapper, Wolfram, Szczepanowski, Monika, Burkhardt, Birgit, Berger, Hilmar, Rosolowski, Maciej, Bentink, Stefan, Schwaenen, Carsten, Wessendorf, Swen, Spang, Rainer, Möller, Peter, Hansmann, Martin Leo, Bernd, Heinz-Wolfram, Ott, German, Hummel, Michael, Stein, Harald, Loeffler, Markus, Trümper, Lorenz, Zimmermann, Martin, Reiter, Alfred, and Siebert, Reiner

Abstract

The spectrum of entities, the therapeutic strategy, and the outcome of mature aggressive B-cell non-Hodgkin lymphomas (maB-NHLs) differs between children and adolescents on the one hand and adult patients on the other. Whereas adult maB-NHLs have been studied in detail, data on molecular profiling of pediatric maB-NHLs are hitherto lacking. We analyzed 65 cases of maB-NHL from patients up to 18 years of age by gene expression profiling, matrix comparative genomic hybridization (CGH), fluorescent in situ hybridization (FISH), and immunohistochemistry. The majority of the analyzed pediatric patients were treated within prospective trials (n = 49). We compared this group to a series of 182 previously published cases of adult maB-NHL. Gene expression profiling reclassified 31% of morphologically defined diffuse large B-cell lymphomas as molecular Burkitt lymphoma (mBL). The subgroups obtained by molecular reclassification did not show any difference in outcome in children treated with the NHL-Berlin-Frankfurt-Muenster (BFM) protocols. No differences were detectable between pediatric and adult mBL with regard to gene expression or chromosomal imbalances. This is the first report on molecular profiling of pediatric B-NHL showing mBL to be much more prominent in children than suggested by morphologic assessment. Based on molecular profiling mBL is a molecularly homogeneous disease across children and adults.

Published

2008

19. Molecular profiling of pediatric mature B-cell lymphoma treated in population-based prospective clinical trials

Author

Klapper, Wolfram, Szczepanowski, Monika, Burkhardt, Birgit, Berger, Hilmar, Rosolowski, Maciej, Bentink, Stefan, Schwaenen, Carsten, Wessendorf, Swen, Spang, Rainer, Möller, Peter, Hansmann, Martin Leo, Bernd, Heinz-Wolfram, Ott, German, Hummel, Michael, Stein, Harald, Loeffler, Markus, Trümper, Lorenz, Zimmermann, Martin, Reiter, Alfred, and Siebert, Reiner

Abstract

The spectrum of entities, the therapeutic strategy, and the outcome of mature aggressive B-cell non-Hodgkin lymphomas (maB-NHLs) differs between children and adolescents on the one hand and adult patients on the other. Whereas adult maB-NHLs have been studied in detail, data on molecular profiling of pediatric maB-NHLs are hitherto lacking. We analyzed 65 cases of maB-NHL from patients up to 18 years of age by gene expression profiling, matrix comparative genomic hybridization (CGH), fluorescent in situ hybridization (FISH), and immunohistochemistry. The majority of the analyzed pediatric patients were treated within prospective trials (n = 49). We compared this group to a series of 182 previously published cases of adult maB-NHL. Gene expression profiling reclassified 31% of morphologically defined diffuse large B-cell lymphomas as molecular Burkitt lymphoma (mBL). The subgroups obtained by molecular reclassification did not show any difference in outcome in children treated with the NHL-Berlin-Frankfurt-Muenster (BFM) protocols. No differences were detectable between pediatric and adult mBL with regard to gene expression or chromosomal imbalances. This is the first report on molecular profiling of pediatric B-NHL showing mBL to be much more prominent in children than suggested by morphologic assessment. Based on molecular profiling mBL is a molecularly homogeneous disease across children and adults.

Published

2008

20. Elektrochemische Synthesen, V Phosphansubstituierte Metallcarbonyle der Eisengruppe/ Electrochemical Syntheses, V Phosphane Substituted Metal Carbonyls of the Iron Group Elements

Author

Grobe, Joseph and Schneider, Bernd Heinz

Abstract

The electrochemical synthesis of iron, cobalt, and nickel carbonyl derivatives with phosphane ligands from metal anodes is described.

Published

1981

21. Elektrochemische Synthesen, IV Metallcarbonylverbindungen der Eisengruppe/Electrochemical Syntheses, IV Metal Carbonyl Compounds of the Iron Group Elements

Author

Grobe, Joseph and Schneider, Bernd Heinz

Abstract

The electrochemical synthesis of iron, cobalt, and nickel carbonyl compounds from metal acetylacetonates of oxidation state + II or + III and from metal anodes is described, solvent effects and the problem of cluster formation are discussed.

Published

1981

22. Elektrochemische Synthesen, X Katalytische Anwendung elektrochemischer Systeme: Cyclooligomerisation von Acetylen / Electrochemical Syntheses, X Catalytic Application of Electrochemical Systems: Cyclooligomerization of Acetylene

Author

Grobe, Joseph, Schneider, Bernd Heinz, and Zimmermann, Heinz

Abstract

Following known procedures for the preparation of nickel complexes as precursors to active contact species for the cyclooligomerization of acetylene we report the electrochemical formation of Ni(CO)2(PPh3)2and its use in a one-pot trimerization of acetylene to benzene. Further investigations demonstrate the possibility to simultaneously produce and use as catalysts active nickel solvates generated from nickel anodes for the cyclization of acetylene to benzene and/or cyclooctatetraene.

Published

1984

23. Ki-67 predicts outcome in advanced-stage mantle cell lymphoma patients treated with anti-CD20 immunochemotherapy: results from randomized trials of the European MCL Network and the German Low Grade Lymphoma Study Group

Author

Determann, Olaf, Hoster, Eva, Ott, German, Wolfram Bernd, Heinz, Loddenkemper, Christoph, Leo Hansmann, Martin, Barth, Thomas E. F., Unterhalt, Michael, Hiddemann, Wolfgang, Dreyling, Martin, and Klapper, Wolfram

Abstract

Clinical outcome of mantle cell lymphoma (MCL) is highly heterogeneous. Tumor cell proliferation as assessed by the Ki-67 index has been shown to yield prognostic information on MCL in many studies using heterogeneously treated patient cohorts. The prognostic value of the Ki-67 index in patients treated with anti-CD20 therapy has not been studied so far. We analyzed the Ki-67 index at primary diagnosis in 249 advanced-stage MCL patients treated within randomized trials. Ki-67 showed high prognostic relevance for overall survival (relative risk 1.27 for 10% higher Ki-67, P < .001), also independently from clinical prognostic factors. The 3 groups with different Ki-67 index of less than 10%, 10% to less than 30%, and 30% or more showed significantly different overall survival in patients treated with CHOP (P = .001) as well as in patients treated with CHOP in combination with anti-CD20 therapy (R-CHOP, P = .013). Thus, the Ki-67 index remains an important prognostic marker in the era of anti-CD20 therapy. The Euro-pean MCL study is registered at www.ClinicalTrials.gov as #NCT00016887.

Published

2008

24. Ki-67 predicts outcome in advanced-stage mantle cell lymphoma patients treated with anti-CD20 immunochemotherapy: results from randomized trials of the European MCL Network and the German Low Grade Lymphoma Study Group

Author

Determann, Olaf, Hoster, Eva, Ott, German, Wolfram Bernd, Heinz, Loddenkemper, Christoph, Leo Hansmann, Martin, Barth, Thomas E.F., Unterhalt, Michael, Hiddemann, Wolfgang, Dreyling, Martin, and Klapper, Wolfram

Abstract

Clinical outcome of mantle cell lymphoma (MCL) is highly heterogeneous. Tumor cell proliferation as assessed by the Ki-67 index has been shown to yield prognostic information on MCL in many studies using heterogeneously treated patient cohorts. The prognostic value of the Ki-67 index in patients treated with anti-CD20 therapy has not been studied so far. We analyzed the Ki-67 index at primary diagnosis in 249 advanced-stage MCL patients treated within randomized trials. Ki-67 showed high prognostic relevance for overall survival (relative risk 1.27 for 10% higher Ki-67, P< .001), also independently from clinical prognostic factors. The 3 groups with different Ki-67 index of less than 10%, 10% to less than 30%, and 30% or more showed significantly different overall survival in patients treated with CHOP (P= .001) as well as in patients treated with CHOP in combination with anti-CD20 therapy (R-CHOP, P= .013). Thus, the Ki-67 index remains an important prognostic marker in the era of anti-CD20 therapy. The Euro-pean MCL study is registered at www.ClinicalTrials.govas #NCT00016887.

Published

2008

25. The Clinical Impact of the Cell-of-Origin Classification and the MYC+/BCL2+ Double Expresser Status in DLBCL Treated within Prospective Clinical Trials of the Dshnhl

Author

Staiger, Annette M., Ziepert, Marita, Horn, Heike, Scott, David W., Barth, Thomas F. E., Bernd, Heinz-Wolfram, Feller, Alfred C., Klapper, Wolfram, Hummel, Michael, Stein, Harald, Lenze, Dido, Hansmann, Martin-Leo, Hartmann, Sylvia, Moeller, Peter, Cogliatti, Sergio, Lenz, Georg, Truemper, Lorenz H., Loeffler, Markus, Schmitz, Norbert, Pfreundschuh, Michael, Rosenwald, Andreas, and Ott, German

Abstract

Scott: NanoString Technologies: Patents & Royalties: named inventor on a patent for molecular subtyping of DLBCL that has been licensed to NanoString Technologies. Klapper:Roche, Novartis, Amgen, Takeda: Research Funding.

Published

2016

26. The Clinical Impact of the Cell-of-Origin Classification and the MYC+/BCL2+ Double Expresser Status in DLBCL Treated within Prospective Clinical Trials of the Dshnhl

Author

Staiger, Annette M., Ziepert, Marita, Horn, Heike, Scott, David W., Barth, Thomas F.E., Bernd, Heinz-Wolfram, Feller, Alfred C., Klapper, Wolfram, Hummel, Michael, Stein, Harald, Lenze, Dido, Hansmann, Martin-Leo, Hartmann, Sylvia, Moeller, Peter, Cogliatti, Sergio, Lenz, Georg, Truemper, Lorenz H., Loeffler, Markus, Schmitz, Norbert, Pfreundschuh, Michael, Rosenwald, Andreas, and Ott, German

Abstract

The Lymph2Cx Cell-of-origin (COO) assay enables the identification of molecular GCB and ABC subtypes of diffuse large B-cell lymphomas (DLBCL) using RNA from formalin-fixed paraffin-embedded (FFPE) samples. In order to explore the prognostic power of this COO assay within the frame of prospectively randomized clinical trials for the first time, we retrospectively performed COO analyses in patient samples from two clinical trials (RICOVER-60: n=360 and R-MegaCHOEP: n=92) of the German High Grade Lymphoma Study Group (DSHNHL) using the Nanostring nCounter®-platform. Immunohistochemistry was done for MYC, FOXP1, LMO2, GCET1, CD5, CD10, BCL2, BCL6, IRF4/MUM1 protein expression, and fluorescence in-situ hybridization was performed for MYC, BCL2and BCL6genes with break-apart probes. COO classification was successfully obtained from 414 samples (326/360 (91%) and 88/92 (96%) FFPE samples from the RICOVER60 and R-MegaCHOEP trials, respectively). In the RICOVER-60 study (patients aged > 60 and <80 years), 42% of tumors were classified as ABC-DLBCL, 44% as GCB-DLBCL, and 14% as unclassified. In the R-MegaCHOEP-trial (patient age 18 to 60 years) 27% were of ABC-type, 60% of GCB-type, and 13% were unclassified. Molecular classification provided by the Lymph2Cx correlated well with IPI factors and stringently with the presence or absence of genetic alterations. Upon FISH analysis, 41/44 (93%) BCL2translocations and all double or triple hit constellations involving MYC/BCL2or MYC/BCL2/BCL6were encountered in the GCB group. A higher proportion of MYCbreaks also clustered in GCB DLBCL (14% in GCB vs. 3% in ABC) in RICOVER-60 (p=0.005). In contrast, BCL6translocations were equally distributed in the RICOVER-60 trial while a higher proportion of BCL6translocations was observed in the ABC-subtype in the R-MegaCHOEP trial.

Published

2016

27. A chromosomal translocation in cyclin D1–negative/cyclin D2–positive mantle cell lymphoma fuses the CCND2gene to the IGKlocus

Author

Gesk, Stefan, Klapper, Wolfram, Martín-Subero, José I., Nagel, Inga, Harder, Lana, Fu, Kai, Bernd, Heinz-Wolfram, Weisenburger, Dennis D., Parwaresch, Reza, and Siebert, Reiner

Published

2006

28. A chromosomal translocation in cyclin D1–negative/cyclin D2–positive mantle cell lymphoma fuses the CCND2 gene to the IGK locus

Author

Gesk, Stefan, Klapper, Wolfram, Martín-Subero, José I., Nagel, Inga, Harder, Lana, Fu, Kai, Bernd, Heinz-Wolfram, Weisenburger, Dennis D., Parwaresch, Reza, and Siebert, Reiner

Published

2006

29. Tumor Cell Proliferation (Ki-67 Index) Overcomes Cytology and Growth Pattern As Prognostic Factor in Mantle-Cell Lymphoma – Results from Randomized Trials of the European MCL Network

Author

Hoster, Eva, Rosenwald, Andreas, Berger, Francoise, Bernd, Heinz-Wolfram, Hartmann, Sylvia, Loddenkemper, Christoph, Barth, Thomas, Brousse, Nicole, Pileri, Stefano, Rymkiewicz, Grzegorz, Kodet, Roman, Unterhalt, Michael, Kluin-Nelemans, Johanna C., Hermine, Olivier, Hiddemann, Wolfgang, Dreyling, Martin H., and Klapper, Wolfram

Abstract

Dreyling: Roche: Honoraria, Research Funding. Klapper:Roche: Research Funding.

Published

2014

30. Tumor Cell Proliferation (Ki-67 Index) Overcomes Cytology and Growth Pattern As Prognostic Factor in Mantle-Cell Lymphoma – Results from Randomized Trials of the European MCL Network

Author

Hoster, Eva, Rosenwald, Andreas, Berger, Francoise, Bernd, Heinz-Wolfram, Hartmann, Sylvia, Loddenkemper, Christoph, Barth, Thomas, Brousse, Nicole, Pileri, Stefano, Rymkiewicz, Grzegorz, Kodet, Roman, Unterhalt, Michael, Kluin-Nelemans, Johanna C., Hermine, Olivier, Hiddemann, Wolfgang, Dreyling, Martin H., and Klapper, Wolfram

Abstract

On Behalf of the European MCL Pathology Panel

Published

2014

31. The Prognostic Impact Of Gene Rearrangements and Protein Expression Of MYC, BCL2 and BCL6 In Young High-Risk Patients With DLBCL

Author

Horn, Heike, Ziepert, Marita, Barth, Thomas F.E., Bernd, Heinz-Wolfram, Wartenberg, Martin, Feller, Alfred C., Klapper, Wolfram, Hummel, Michael, Stein, Harald, Lenze, Dido, Hartmann, Sylvia, Hansmann, Martin-Leo, Möller, Peter, Cogliatti, Sergio, Pfreundschuh, Michael, Trümper, Lorenz, Löffler, Markus, Ott, German, Schmitz, Norbert, and Rosenwald, Andreas

Abstract

A number of retrospective analyses have looked into the prognostic implication of MYC, BCL2 and BCL6 rearrangements and protein expression for MYC, BCL2 and BCL6 in patients with diffuse large B-cell lymphoma (DLBCL). Many of these studies suffer from small patient cohorts and differing or unknown treatment strategies (with or without Rituximab) administered to patients under study. Furthermore, the median age of these patients was relatively high. We for the first time report on the prognostic consequences of MYC, BCL2 and BCL6 alterations in younger (18-60 years) high-risk patients (aaIPI 2 or 3) with DLBCL.The MegaCHOEP study (Schmitz et al. Lancet Oncology 2012: 13, 1250) randomized patients to 8xCHOEP-14 or sequential high-dose therapy supported by repeated infusions of autologous stem cells. Both treatment arms included 6 infusions of R (375 mg/ sqm). The median patient age was 48 years, and 27% of patients scored an aaIPI of 3. Paraffin-embedded tumor samples from 112 de novo DLBCL were investigated using immunohistochemistry for MYC, BCL2, and BCL6, and fluorescence in-situ hybridisation (FISH) to detect breaks of MYC, BCL2 and BCL6.Rearrangements of MYC, BCL2 and BCL6 were detected in 13.6%, 20.7% and 30.9% of DLBCL, respectively. A double or triple hit constellation occurred in 10.8%. Presence of BCL2 breaks (RR=4.7, 95% CI: 1.8-12.2) and MYC breaks (RR=2.4, 95% CI: 0.8-7.5), but not of BCL6 breaks were associated with inferior overall survival in univariate and multivariate analyses adjusted for aaIPI and treatment arm. Protein overexpression of MYC ≥30% (RR=2.4, 95% CI: 0.9-6.5), but not BCL2 (≥60%) or BCL6 (≥30%) indicated inferior overall survival. BCL2 overexpression was associated with inferior EFS (RR=2.2, 95% CI: 0.9-5.5) and PFS (RR=2.8, 95% CI: 1.0-8.2). If the same cutpoint for BCL2 used for a similar analysis in elderly patients treated on the RICOVER-60 trial (Horn et al. Blood 2013) was applied, no differences in EFS or PFS were observed.Rearrangements of MYC and BCL2 seem to be relevant prognostic factors also in young high-risk patients. The frequencies of MYC and BCL2 rearrangements are not substantially higher than reported for other, mostly elderly patient groups carrying IPI scores from 0 - 5; it seems unlikely, therefore, that the rearrangements described here (completely) explain the poor prognosis of young, high-risk patients. The prognostic role of BCL2, BCL6, and MYC as well as other biological risk factors must be validated in independent data sets.No relevant conflicts of interest to declare.

Published

2013

32. The Prognostic Impact Of Gene Rearrangements and Protein Expression Of MYC, BCL2 and BCL6 In Young High-Risk Patients With DLBCL

Author

Horn, Heike, Ziepert, Marita, Barth, Thomas F.E., Bernd, Heinz-Wolfram, Wartenberg, Martin, Feller, Alfred C., Klapper, Wolfram, Hummel, Michael, Stein, Harald, Lenze, Dido, Hartmann, Sylvia, Hansmann, Martin-Leo, Möller, Peter, Cogliatti, Sergio, Pfreundschuh, Michael, Trümper, Lorenz, Löffler, Markus, Ott, German, Schmitz, Norbert, and Rosenwald, Andreas

Abstract

A number of retrospective analyses have looked into the prognostic implication of MYC, BCL2and BCL6rearrangements and protein expression for MYC, BCL2 and BCL6 in patients with diffuse large B-cell lymphoma (DLBCL). Many of these studies suffer from small patient cohorts and differing or unknown treatment strategies (with or without Rituximab) administered to patients under study. Furthermore, the median age of these patients was relatively high. We for the first time report on the prognostic consequences of MYC, BCL2 and BCL6 alterations in younger (18-60 years) high-risk patients (aaIPI 2 or 3) with DLBCL.

Published

2013

33. Cell Proliferation (Ki-67) As Prognostic Marker in Mantle Cell Lymphoma.

Author

Hoster, Eva, Klapper, Wolfram, Rosenwald, Andreas, Bernd, Heinz-Wolfram, Hartmann, Sylvia, Loddenkemper, Christoph, Barth, Thomas F.E., Hiddemann, Wolfgang, Unterhalt, Michael, Kluin-Nelemans, Hanneke C., Hermine, Olivier, and Dreyling, Martin

Abstract

The percentage of proliferating cells evaluated on diagnostic tumor samples has been shown to be of high prognostic relevance in Mantle Cell Lymphoma (MCL) patients. As MCL is relatively rare, evaluation of proliferation has so far mostly been based on smaller patient cohorts that were retrospectively collected and inhomogenously treated. In 2004, the European MCL Network initiated two large European randomized trials for younger (“MCL Younger” trial) and older (“MCL Elderly” trial) MCL patients, primary results of which have recently been reported (Kluin-Nelemans et al., NEJM 2012, Hermine et al., ASH 2010). We aimed to clarify the prognostic relevance of the proliferation marker Ki-67 using pooled data from these two trials.Patients with histologically confirmed and previously untreated MCL of stages II-IV up to 65 years of age were randomly assigned in “MCL Younger” to either 6 cycles R-CHOP followed by myeloablative radio-chemotherapy and autologous stem cell transplantation (ASCT), or 6 cycles alternating R-CHOP/R-DHAP followed by high-dose-Ara-C containing conditioning and ASCT. Patients aged 60 years or older and not eligible for high-dose therapy were randomly assigned in “MCL Elderly” to either 8 cycles of R-CHOP or 6 cycles of R-FC; responding patients were subsequently randomized to either interferon-alpha or rituximab maintenance until progression. Histological diagnosis was confirmed by central review within the European MCL Pathology Panel. The percentage of Ki-67 positive cells was counted on diagnostic lymphoma samples among 2 times 100 cells by the central pathology labs according to published consensus guidelines (Klapper et al., J Hematopathology 2009). The outcome measures were time to treatment failure (TTF) from treatment initiation to stable disease, progression, or death from any cause, and overall survival (OS) from trial registration to death from any cause. We investigated the prognostic value of proliferation as a quantitative marker with regards to TTF and OS in univariable Cox regression and evaluated the previously established cut-off values of 10% and 30% (Determann et al., Blood 2008) using Kaplan-Meier estimates and log rank tests. We also adjusted for clinical prognostic factors (MIPI, Hoster et al., Blood 2008).Counted Ki-67 values were available in 51% (543) of 1057 randomized patients (material not available, 30%; Ki-67 evaluation not possible due to technical reasons, 16%). The origin of tumor tissue was lymph node in 81%, gastrointestinal tract in 12%, bone marrow in 4% and other in 3%. The median proliferation rate was 20% (range, 0–97%; interquartile range, 12–34%) and did not significantly differ between tissue origins. In univariable analysis, a 10% higher proliferation rate was associated with hazard ratios of 1.18 (95% confidence interval, 1.12 to 1.25, p<0.0001) for TTF and 1.23 (95% CI, 1.15 to 1.31, p<0.0001) for OS. Patients with Ki-67 ≥ 30% had median TTF and OS of 19 and 45 months compared to 64 months and not reached with Ki-67 < 30% (p<0.0001 each). Patients with Ki-67 < 30% and either ≥ 10% or < 10% had similar TTF and OS. The separation of a high risk group as defined by Ki-67 ≥ 30% was consistently seen within “MCL Younger” and “MCL Elderly” as well as within the 4 different induction treatment arms. The prognostic impact of proliferation was independent of the MIPI prognostic score (adjusted hazard ratio for TTF, 1.11, 95% CI, 1.05 – 1.17, p=0.0005; for OS, 1.14, 1.07–1.23, p=0.0001), which was also independently highly prognostic (p<0.0001). Almost identical results were seen when the analyses were restricted to lymph node samples.Cell proliferation was confirmed as important biological prognostic marker independent of clinical prognostic factors on a large cohort of MCL patients uniformly treated within clinical trials. Since the evaluation of Ki-67 has been standardized, guidelines (e.g. Dreyling et al., Ann Onc, in press) recommend applying this parameter in clinical routine. Further analyses will focus on the joint correlation of Ki-67, MIPI and minimal residual disease with outcome to potentially allow a more individualized therapeutic approach in MCL patients.On behalf of the European Mantle Cell Lymphoma Network.No relevant conflicts of interest to declare.

Published

2012

34. Cell Proliferation (Ki-67) As Prognostic Marker in Mantle Cell Lymphoma.

Author

Hoster, Eva, Klapper, Wolfram, Rosenwald, Andreas, Bernd, Heinz-Wolfram, Hartmann, Sylvia, Loddenkemper, Christoph, Barth, Thomas F.E., Hiddemann, Wolfgang, Unterhalt, Michael, Kluin-Nelemans, Hanneke C., Hermine, Olivier, and Dreyling, Martin

Abstract

Abstract 2677

Published

2012

35. Buchbesprechung: Knochenmarksdiagnostik, Lehrbuch und Atlas, 1. Aufl.

Author

Bernd, Heinz-Wolfram

Published

2008