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101. Severe COVID-19 Is Characterised by Perturbations in Plasma Amines Correlated with Immune Response Markers, and Linked to Inflammation and Oxidative Stress

Author

Karu, Naama, Kindt, Alida, van Gammeren, A.J., Ermens, Anton, Harms, Amy, Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, Hankemeier, Thomas, Karu, Naama, Kindt, Alida, van Gammeren, A.J., Ermens, Anton, Harms, Amy, Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, and Hankemeier, Thomas

Abstract

The COVID-19 pandemic raised a need to characterise the biochemical response to SARS-CoV-2 infection and find biological markers to identify therapeutic targets. In support of these aims, we applied a range of LC-MS platforms to analyse over 100 plasma samples from patients with varying COVID-19 severity and with detailed clinical information on inflammatory responses (>30 immune markers). The first publication in a series reports the results of quantitative LC-MS/MS profiling of 56 amino acids and derivatives. A comparison between samples taken from ICU and ward patients revealed a notable increase in ten post-translationally modified amino acids that correlated with markers indicative of an excessive immune response: TNF-alpha, neutrophils, markers for macrophage, and leukocyte activation. Severe patients also had increased kynurenine, positively correlated with CRP and cytokines that induce its production. ICU and ward patients with high IL-6 showed decreased levels of 22 immune-supporting and anti-oxidative amino acids and derivatives (e.g., glutathione, GABA). These negatively correlated with CRP and IL-6 and positively correlated with markers indicative of adaptive immune activation. Including corresponding alterations in con-valescing ward patients, the overall metabolic picture of severe COVID-19 reflected enhanced metabolic demands to maintain cell proliferation and redox balance, alongside increased inflammation and oxidative stress.

Published
2022

102. Plasma Oxylipins and Their Precursors Are Strongly Associated with COVID-19 Severity and with Immune Response Markers

Author

Karu, Naama, Kindt, Alida, Lamont, Lieke, van Gammeren, Adriaan, Ermens, Anton, Harms, Amy C., Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, Hankemeier, Thomas, Karu, Naama, Kindt, Alida, Lamont, Lieke, van Gammeren, Adriaan, Ermens, Anton, Harms, Amy C., Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, and Hankemeier, Thomas

Abstract

COVID-19 is characterised by a dysregulated immune response, that involves signalling lipids acting as mediators of the inflammatory process along the innate and adaptive phases. To promote understanding of the disease biochemistry and provide targets for intervention, we applied a range of LC-MS platforms to analyse over 100 plasma samples from patients with varying COVID-19 severity and with detailed clinical information on inflammatory responses (>30 immune markers). The second publication in a series reports the results of quantitative LC-MS/MS profiling of 63 small lipids including oxylipins, free fatty acids, and endocannabinoids. Compared to samples taken from ward patients, intensive care unit (ICU) patients had 2–4-fold lower levels of arachidonic acid (AA) and its cyclooxygenase-derived prostanoids, as well as lipoxygenase derivatives, exhibiting negative correlations with inflammation markers. The same derivatives showed 2–5-fold increases in recovering ward patients, in paired comparison to early hospitalisation. In contrast, ICU patients showed elevated levels of oxylipins derived from poly-unsaturated fatty acids (PUFA) by non-enzymatic peroxidation or activity of soluble epoxide hydrolase (sEH), and these oxylipins positively correlated with markers of macrophage activation. The deficiency in AA enzymatic products and the lack of elevated intermediates of pro-resolving mediating lipids may result from the preference of alternative metabolic conversions rather than diminished stores of PUFA precursors. Supporting this, ICU patients showed 2-to-11-fold higher levels of linoleic acid (LA) and the corresponding fatty acyl glycerols of AA and LA, all strongly correlated with multiple markers of excessive immune response. Our results suggest that the altered oxylipin metabolism disrupts the expected shift from innate immune response to resolution of inflammation.

Published
2022

103. Molecular characterisation and clinical outcome of B-cell precursor acute lymphoblastic leukaemia with IG-MYC rearrangement

Author

Bomken, S, Enshaei, A, Schwalbe, E, Mikulasova, A, Dai, Y, Zaka, M, Fung, K, Bashton, M, Lim, H, Jones, L, Karataraki, N, Winterman, E, Ashby, C, Attarbaschi, A, Bertrand, Y, Bradtke, J, Buldini, B, Burke, G, Cazzaniga, G, Gohring, G, De Groot-Kruseman, H, Haferlach, C, Nigro, L, Parihar, M, Plesa, A, Seaford, E, Sonneveld, E, Strehl, S, Van der Velden, V, Rand, V, Hunger, S, Harrison, C, Bacon, C, Van Delft, F, Loh, M, Moppett, J, Vormoor, J, Walker, B, Moorman, A, Russell, L, Bomken, Simon, Enshaei, Amir, Schwalbe, Edward C, Mikulasova, Aneta, Dai, Yunfeng, Zaka, Masood, Fung, Kent Tm, Bashton, Matthew, Lim, Huezin, Jones, Lisa, Karataraki, Nefeli, Winterman, Emily, Ashby, Cody, Attarbaschi, Andishe, Bertrand, Yves, Bradtke, Jutta, Buldini, Barbara, Burke, G. A. Amos, Cazzaniga, Giovanni, Gohring, Gudrun, De Groot-Kruseman, Hesta A, Haferlach, Claudia, Nigro, Luca Lo, Parihar, Mayur, Plesa, Adriana, Seaford, Emma, Sonneveld, Edwin, Strehl, Sabine, Van der Velden, Vincent Hj, Rand, Vikki, Hunger, Stephen P, Harrison, Christine J, Bacon, Chris M, Van Delft, Frederik W, Loh, Mignon L, Moppett, John, Vormoor, Josef, Walker, Brian A, Moorman, Anthony V, Russell, Lisa J, Bomken, S, Enshaei, A, Schwalbe, E, Mikulasova, A, Dai, Y, Zaka, M, Fung, K, Bashton, M, Lim, H, Jones, L, Karataraki, N, Winterman, E, Ashby, C, Attarbaschi, A, Bertrand, Y, Bradtke, J, Buldini, B, Burke, G, Cazzaniga, G, Gohring, G, De Groot-Kruseman, H, Haferlach, C, Nigro, L, Parihar, M, Plesa, A, Seaford, E, Sonneveld, E, Strehl, S, Van der Velden, V, Rand, V, Hunger, S, Harrison, C, Bacon, C, Van Delft, F, Loh, M, Moppett, J, Vormoor, J, Walker, B, Moorman, A, Russell, L, Bomken, Simon, Enshaei, Amir, Schwalbe, Edward C, Mikulasova, Aneta, Dai, Yunfeng, Zaka, Masood, Fung, Kent Tm, Bashton, Matthew, Lim, Huezin, Jones, Lisa, Karataraki, Nefeli, Winterman, Emily, Ashby, Cody, Attarbaschi, Andishe, Bertrand, Yves, Bradtke, Jutta, Buldini, Barbara, Burke, G. A. Amos, Cazzaniga, Giovanni, Gohring, Gudrun, De Groot-Kruseman, Hesta A, Haferlach, Claudia, Nigro, Luca Lo, Parihar, Mayur, Plesa, Adriana, Seaford, Emma, Sonneveld, Edwin, Strehl, Sabine, Van der Velden, Vincent Hj, Rand, Vikki, Hunger, Stephen P, Harrison, Christine J, Bacon, Chris M, Van Delft, Frederik W, Loh, Mignon L, Moppett, John, Vormoor, Josef, Walker, Brian A, Moorman, Anthony V, and Russell, Lisa J

Abstract

Rarely, immunophenotypically immature B-cell precursor acute lymphoblastic leukaemia (BCP-ALL) carries an immunoglobulin-MYC rearrangement (IG-MYC-r). This can result in diagnostic confusion with Burkitt lymphoma/leukaemia and use of unproven individualised treatment schedules. Here we contrast the molecular characteristics of these conditions and investigate historic clinical outcome data. We identified 90 cases registered on a national BCP-ALL clinical trial/registry. Where present, diagnostic material underwent cytogenetic, exome, methylome and transcriptome analysis. Outcome was analysed to define 3-year event free survival (EFS) and overall survival (OS). IG-MYC-r was identified in diverse cytogenetic backgrounds, co-existing with either: established BCP-ALL specific abnormalities (high hyperdiploidy n=3, KMT2A-rearrangement n=6, iAMP21 n=1, BCR-ABL n=1); BCL2/BCL6-rearrangements (n=15); or, most commonly, as the only defining feature (n=64). Within this final group, precursor-like V(D)J breakpoints predominated (8/9) and KRAS mutations were common (5/11). DNA methylation identified a cluster of V(D)J rearranged cases, clearly distinct from Burkitt leukaemia/lymphoma. Children with IG-MYC-r within that subgroup had 3-year EFS of 47% and OS of 60%, representing a high-risk BCP-ALL. To develop effective management strategies this patient group must be allowed access to contemporary, minimal residual disease adapted, prospective clinical trial protocols.

Published
2022

104. Clofarabine added to intensive treatment in adult patients with newly diagnosed ALL: the HOVON-100 trial.

Author

UCL - SSS/DDUV/MEXP - Médecine expérimentale, UCL - (SLuc) Service d'hématologie, Rijneveld, Anita W, van der Holt, Bronno, de Weerdt, Okke, Biemond, Bart J, van de Loosdrecht, Arjen A, van der Wagen, Lotte E, Bellido, Mar, van Gelder, Michel, van der Velden, Walter J F M, Selleslag, Dominik, van Lammeren-Venema, Daniëlle, Halkes, Constantijn J M, Fijnheer, Rob, Havelange, Violaine, van Sluis, Geerte L, Legdeur, Marie-Cecile, Deeren, Dries, Gadisseur, Alain, Sinnige, Harm A M, Breems, Dimitri A, Jaspers, Aurélie, Legrand, Ollivier, Terpstra, Wim E, Boersma, Rinske S, Mazure, Dominiek, Triffet, Agnes, Tick, Lidwine W, Beel, Karolien, Maertens, Johan A, Beverloo, H Berna, Bakkus, Marleen, Homburg, Christa H E, de Haas, Valerie, van der Velden, Vincent H J, Cornelissen, Jan J, Dutch-Belgian HOVON Cooperative group, UCL - SSS/DDUV/MEXP - Médecine expérimentale, UCL - (SLuc) Service d'hématologie, Rijneveld, Anita W, van der Holt, Bronno, de Weerdt, Okke, Biemond, Bart J, van de Loosdrecht, Arjen A, van der Wagen, Lotte E, Bellido, Mar, van Gelder, Michel, van der Velden, Walter J F M, Selleslag, Dominik, van Lammeren-Venema, Daniëlle, Halkes, Constantijn J M, Fijnheer, Rob, Havelange, Violaine, van Sluis, Geerte L, Legdeur, Marie-Cecile, Deeren, Dries, Gadisseur, Alain, Sinnige, Harm A M, Breems, Dimitri A, Jaspers, Aurélie, Legrand, Ollivier, Terpstra, Wim E, Boersma, Rinske S, Mazure, Dominiek, Triffet, Agnes, Tick, Lidwine W, Beel, Karolien, Maertens, Johan A, Beverloo, H Berna, Bakkus, Marleen, Homburg, Christa H E, de Haas, Valerie, van der Velden, Vincent H J, Cornelissen, Jan J, and Dutch-Belgian HOVON Cooperative group

Abstract

Clofarabine (CLO) is a nucleoside analog with efficacy in relapsed/refractory acute lymphoblastic leukemia (ALL). This randomized phase 3 study aimed to evaluate whether CLO added to induction and whether consolidation would improve outcome in adults with newly diagnosed ALL. Treatment of younger (18-40 years) patients consisted of a pediatric-inspired protocol, and for older patients (41-70 years), a semi-intensive protocol was used. Three hundred and forty patients were randomized. After a median follow-up of 70 months, 5-year event-free survival (EFS) was 50% and 53% for arm A and B (CLO arm). For patients ≤40 years, EFS was 58% vs 65% in arm A vs B, whereas in patients >40 years, EFS was 43% in both arms. Complete remission (CR) rate was 89% in both arms and similar in younger and older patients. Minimal residual disease (MRD) was assessed in 200 patients (60%). Fifty-four of 76 evaluable patients (71%) were MRD- after consolidation 1 in arm A vs 75/81 (93%) in arm B (P = .001). Seventy (42%) patients proceeded to allogeneic hematopoietic stem cell transplantation in both arms. Five-year overall survival (OS) was similar in both arms: 60% vs 61%. Among patients achieving CR, relapse rates were 28% and 24%, and nonrelapse mortality was 16% vs 17% after CR. CLO-treated patients experienced more serious adverse events, more infections, and more often went off protocol. This was most pronounced in older patients. We conclude that, despite a higher rate of MRD negativity, addition of CLO does not improve outcome in adults with ALL, which might be due to increased toxicity. This trial was registered at www.trialregister.nl as #NTR2004.

Published
2022

105. Severe COVID-19 Is Characterised by Perturbations in Plasma Amines Correlated with Immune Response Markers, and Linked to Inflammation and Oxidative Stress

Author

IRAS OH Epidemiology Chemical Agents, Karu, Naama, Kindt, Alida, van Gammeren, A.J., Ermens, Anton, Harms, Amy, Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, Hankemeier, Thomas, IRAS OH Epidemiology Chemical Agents, Karu, Naama, Kindt, Alida, van Gammeren, A.J., Ermens, Anton, Harms, Amy, Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, and Hankemeier, Thomas

Published
2022

106. Plasma Oxylipins and Their Precursors Are Strongly Associated with COVID-19 Severity and with Immune Response Markers

Author

IRAS OH Epidemiology Chemical Agents, Karu, Naama, Kindt, Alida, Lamont, Lieke, van Gammeren, Adriaan, Ermens, Anton, Harms, Amy C., Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, Hankemeier, Thomas, IRAS OH Epidemiology Chemical Agents, Karu, Naama, Kindt, Alida, Lamont, Lieke, van Gammeren, Adriaan, Ermens, Anton, Harms, Amy C., Portengen, Lützen, Vermeulen, Roel, Dik, Willem A, Langerak, Anton W, van der Velden, Vincent H J, and Hankemeier, Thomas

Published
2022

107. TRB sequences targeting ORF1a/b are associated with disease severity in hospitalized COVID-19 patients

Author

Assmann, Jorn L.J.C., Kolijn, P. Martijn, Schrijver, Benjamin, van Gammeren, Adriaan J., Loth, Daan W., Ermens, Ton A.A.M., Dik, Willem A., van der Velden, Vincent H.J., Langerak, Anton W., Assmann, Jorn L.J.C., Kolijn, P. Martijn, Schrijver, Benjamin, van Gammeren, Adriaan J., Loth, Daan W., Ermens, Ton A.A.M., Dik, Willem A., van der Velden, Vincent H.J., and Langerak, Anton W.

Abstract

The potential protective or pathogenic role of the adaptive immune response to SARS-CoV-2 infection has been vigorously debated. While COVID-19 patients consistently generate a T lymphocyte response to SARS-CoV-2 antigens, evidence of significant immune dysregulation in these patients continues to accumulate. In this study, next generation sequencing of the T cell receptor beta chain (TRB) repertoire was conducted in hospitalized COVID-19 patients to determine if immunogenetic differences of the TRB repertoire contribute to disease course severity. Clustering of highly similar TRB CDR3 amino acid sequences across COVID-19 patients yielded 781 shared TRB sequences. The TRB sequences were then filtered for known associations with common diseases such as EBV and CMV. The remaining sequences were cross-referenced to a publicly accessible dataset that mapped COVID-19 specific TCRs to the SARS-CoV-2 genome. We identified 158 SARS-CoV-2 specific TRB sequences belonging to 134 clusters in our COVID-19 patients. Next, we investigated 113 SARS-CoV-2 specific clusters binding only one peptide target in relation to disease course. Distinct skewing of SARS-CoV-2 specific TRB sequences toward the nonstructural proteins (NSPs) encoded within ORF1a/b of the SARS-CoV-2 genome was observed in clusters associated with critical disease course when compared to COVID-19 clusters associated with a severe disease course. These data imply that T-lymphocyte reactivity towards peptides from NSPs of SARS-CoV-2 may not constitute an effective adaptive immune response and thus may negatively affect disease severity.

Published
2022

108. Quality Assessment of a Large Multi-Center Flow Cytometric Dataset of Acute Myeloid Leukemia Patients—A EuroFlow Study

Author

Bras, Anne E., Matarraz, Sergio, Nierkens, Stefan, Fernández, Paula, Philippé, Jan, Aanei, Carmen Mariana, de Mello, Fabiana Vieira, Burgos, Leire, van der Sluijs-Gelling, Alita J., Grigore, Georgiana Emilia, van Dongen, Jacques J.M., Orfao, Alberto, van der Velden, Vincent H.J., Bras, Anne E., Matarraz, Sergio, Nierkens, Stefan, Fernández, Paula, Philippé, Jan, Aanei, Carmen Mariana, de Mello, Fabiana Vieira, Burgos, Leire, van der Sluijs-Gelling, Alita J., Grigore, Georgiana Emilia, van Dongen, Jacques J.M., Orfao, Alberto, and van der Velden, Vincent H.J.

Abstract

Flowcytometric analysis allows for detailed identification and characterization of large numbers of cells in blood, bone marrow, and other body fluids and tissue samples and therefore contributes to the diagnostics of hematological malignancies. Novel data analysis tools allow for multidimensional analysis and comparison of patient samples with reference databases of normal, reactive, and/or leukemia/lymphoma patient samples. Building such reference databases requires strict quality assessment (QA) procedures. Here, we compiled a dataset and developed a QA methodology of the EuroFlow Acute Myeloid Leukemia (AML) database, based on the eight-color EuroFlow AML panel consisting of six different antibody combinations, including four backbone markers. In total, 1142 AML cases and 42 normal bone marrow samples were included in this analysis. QA was performed on 803 AML cases using multidimensional analysis of backbone markers, as well as tube-specific markers, and data were compared using classical analysis employing median and peak expression values. Validation of the QA procedure was performed by re-analysis of >300 cases and by running an independent cohort of 339 AML cases. Initial evaluation of the final cohort confirmed specific immunophenotypic patterns in AML subgroups; the dataset therefore can reliably be used for more detailed exploration of the immunophenotypic variability of AML. Our data show the potential pitfalls and provide possible solutions for constructing large flowcytometric databases. In addition, the provided approach may facilitate the building of other databases and thereby support the development of novel tools for (semi)automated QA and subsequent data analysis.

Published
2022

109. VS38c and CD38-Multiepitope Antibodies Provide Highly Comparable Minimal Residual Disease Data in Patients With Multiple Myeloma

Author

Broijl, Annemiek, de Jong, Augustinus C M, van Duin, Mark, Sonneveld, Pieter, Kühnau, Jesper, van der Velden, Vincent H J, Broijl, Annemiek, de Jong, Augustinus C M, van Duin, Mark, Sonneveld, Pieter, Kühnau, Jesper, and van der Velden, Vincent H J

Abstract

OBJECTIVES: To compare flow cytometric minimal residual disease (MRD) data obtained using the EuroFlow approach, including the CD38-multiepitope (ME) antibody or the VS38c antibody.METHODS: We evaluated 29 bone marrow samples from patients with multiple myeloma (MM), of whom 15 had received daratumumab within the past 6 months. We evaluated MRD data and fluorescence intensities.RESULTS: Qualitative MRD data were 100% concordant between the 2 approaches. In MRD-positive samples (n = 14), MRD levels showed an excellent correlation (R2 = 0.999). Whereas VS38c staining was strong in both normal plasma cells and MM cells, independent of daratumumab treatment, staining intensities for CD38 were lower in MM cells compared with normal plasma cells, and on both cell types CD38 expression was significantly reduced in daratumumab-treated patients.CONCLUSIONS: Both CD38-ME and VS38c allow reliable MRD detection in MM patients, but the high expression of VS38c allows easier identification of MM cells, especially in daratumumab-treated patients.

Published
2022

110. Clofarabine added to intensive treatment in adult patients with newly diagnosed ALL:the HOVON-100 trial

Author

Rijneveld, Anita W., van der Holt, Bronno, de Weerdt, Okke, Biemond, Bart J., van de Loosdrecht, Arjen A., van der Wagen, Lotte E., Bellido, Mar, van Gelder, Michel, van der Velden, Walter J.F.M., Selleslag, Dominik, van Lammeren-Venema, Danie€lle, Halkes, Constantijn J.M., Fijnheer, Rob, Havelange, Violaine, van Sluis, Geerte L., Legdeur, Marie Cecile, Deeren, Dries, Gadisseur, Alain, Sinnige, Harm A.M., Breems, Dimitri A., Jaspers, Aurelie, Legrand, Ollivier, Terpstra, Wim E., Boersma, Rinske S., Mazure, Dominiek, Triffet, Agnes, Tick, Lidwine W., Beel, Karolien, Maertens, Johan A., Beverloo, H. Berna, Bakkus, Marleen, Homburg, Christa H.E., de Haas, Valerie, van der Velden, Vincent H.J., Cornelissen, Jan J., Rijneveld, Anita W., van der Holt, Bronno, de Weerdt, Okke, Biemond, Bart J., van de Loosdrecht, Arjen A., van der Wagen, Lotte E., Bellido, Mar, van Gelder, Michel, van der Velden, Walter J.F.M., Selleslag, Dominik, van Lammeren-Venema, Danie€lle, Halkes, Constantijn J.M., Fijnheer, Rob, Havelange, Violaine, van Sluis, Geerte L., Legdeur, Marie Cecile, Deeren, Dries, Gadisseur, Alain, Sinnige, Harm A.M., Breems, Dimitri A., Jaspers, Aurelie, Legrand, Ollivier, Terpstra, Wim E., Boersma, Rinske S., Mazure, Dominiek, Triffet, Agnes, Tick, Lidwine W., Beel, Karolien, Maertens, Johan A., Beverloo, H. Berna, Bakkus, Marleen, Homburg, Christa H.E., de Haas, Valerie, van der Velden, Vincent H.J., and Cornelissen, Jan J.

Abstract

Clofarabine (CLO) is a nucleoside analog with efficacy in relapsed/refractory acute lymphoblastic leukemia (ALL). This randomized phase 3 study aimed to evaluate whether CLO added to induction and whether consolidation would improve outcome in adults with newly diagnosed ALL. Treatment of younger (18-40 years) patients consisted of a pediatric-inspired protocol, and for older patients (41-70 years), a semi-intensive protocol was used. Three hundred and forty patients were randomized. After a median follow-up of 70 months, 5-year event-free survival (EFS) was 50% and 53% for arm A and B (CLO arm). For patients #40 years, EFS was 58% vs 65% in arm A vs B, whereas in patients .40 years, EFS was 43% in both arms. Complete remission (CR) rate was 89% in both arms and similar in younger and older patients. Minimal residual disease (MRD) was assessed in 200 patients (60%). Fifty-four of 76 evaluable patients (71%) were MRD2 after consolidation 1 in arm A vs 75/81 (93%) in arm B (P 5 .001). Seventy (42%) patients proceeded to allogeneic hematopoietic stem cell transplantation in both arms. Five-year overall survival (OS) was similar in both arms: 60% vs 61%. Among patients achieving CR, relapse rates were 28% and 24%, and nonrelapse mortality was 16% vs 17% after CR. CLO-treated patients experienced more serious adverse events, more infections, and more often went off protocol. This was most pronounced in older patients. We conclude that, despite a higher rate of MRD negativity, addition of CLO does not improve outcome in adults with ALL, which might be due to increased toxicity.

Published
2022

111. Bone Marrow Stromal Cell Regeneration Profile in Treated B-Cell Precursor Acute Lymphoblastic Leukemia Patients:Association with MRD Status and Patient Outcome

Author

Oliveira, Elen, Costa, Elaine S., Ciudad, Juana, Gaipa, Giuseppe, Sedek, Łukasz, Barrena, Susana, Szczepanski, Tomasz, Buracchi, Chiara, Silvestri, Daniela, Siqueira, Patrícia F.R., Mello, Fabiana V., Torres, Rafael C., Oliveira, Leonardo M.R., Fay-Neves, Isabelle V.C., Sonneveld, Edwin, van der Velden, Vincent H.J., Mejstrikova, Esther, Ribera, Josep Maria, Conter, Valentino, Schrappe, Martin, van Dongen, Jacques J.M., Land, Marcelo G.P., Orfao, Alberto, Oliveira, Elen, Costa, Elaine S., Ciudad, Juana, Gaipa, Giuseppe, Sedek, Łukasz, Barrena, Susana, Szczepanski, Tomasz, Buracchi, Chiara, Silvestri, Daniela, Siqueira, Patrícia F.R., Mello, Fabiana V., Torres, Rafael C., Oliveira, Leonardo M.R., Fay-Neves, Isabelle V.C., Sonneveld, Edwin, van der Velden, Vincent H.J., Mejstrikova, Esther, Ribera, Josep Maria, Conter, Valentino, Schrappe, Martin, van Dongen, Jacques J.M., Land, Marcelo G.P., and Orfao, Alberto

Abstract

For the last two decades, measurable residual disease (MRD) has become one of the most powerful independent prognostic factors in B-cell precursor acute lymphoblastic leukemia (BCP-ALL). However, the effect of therapy on the bone marrow (BM) microenvironment and its potential relationship with the MRD status and disease free survival (DFS) still remain to be investigated. Here we analyzed the distribution of mesenchymal stem cells (MSC) and endothelial cells (EC) in the BM of treated BCP-ALL patients, and its relationship with the BM MRD status and patient outcome. For this purpose, the BM MRD status and EC/MSC regeneration profile were analyzed by multiparameter flow cytometry (MFC) in 16 control BM (10 children; 6 adults) and 1204 BM samples from 347 children and 100 adult BCP-ALL patients studied at diagnosis (129 children; 100 adults) and follow-up (824 childhood samples; 151 adult samples). Patients were grouped into a discovery cohort (116 pediatric BCP-ALL patients; 338 samples) and two validation cohorts (74 pediatric BCP-ALL, 211 samples; and 74 adult BCP-ALL patients; 134 samples). Stromal cells (i.e., EC and MSC) were detected at relatively low frequencies in all control BM (16/16; 100%) and in most BCP-ALL follow-up samples (874/975; 90%), while they were undetected in BCP-ALL BM at diagnosis. In control BM samples, the overall percentage of EC plus MSC was higher in children than adults (p = 0.011), but with a similar EC/MSC ratio in both groups. According to the MRD status similar frequencies of both types of BM stromal cells were detected in BCP-ALL BM studied at different time points during the follow-up. Univariate analysis (including all relevant prognostic factors together with the percentage of stromal cells) performed in the discovery cohort was used to select covariates for a multivariate Cox regression model for predicting patient DFS. Of note, an increased percentage of EC (>32%) within the BCP-ALL BM stromal cell compartment at day +78

Published
2022

112. Inotuzumab ozogamicin as single agent in pediatric patients with relapsed and refractory acute lymphoblastic leukemia:results from a phase II trial

Author

Pennesi, Edoardo, Michels, Naomi, Brivio, Erica, van der Velden, Vincent H.J., Jiang, Yilin, Thano, Adriana, Ammerlaan, Anneke J.C., Boer, Judith M., Beverloo, H. Berna, Sleight, Barbara, Chen, Ying, Vormoor-Bürger, Britta, Rives, Susana, Bielorai, Bella, Rössig, Claudia, Petit, Arnaud, Rizzari, Carmelo, Engstler, Gernot, Starý, Jan, Bautista Sirvent, Francisco J., Chen-Santel, Christiane, Bruno, Benedicte, Bertrand, Yves, Rialland, Fanny, Plat, Geneviève, Reinhardt, Dirk, Vinti, Luciana, Von Stackelberg, Arend, Locatelli, Franco, Zwaan, Christian M., Pennesi, Edoardo, Michels, Naomi, Brivio, Erica, van der Velden, Vincent H.J., Jiang, Yilin, Thano, Adriana, Ammerlaan, Anneke J.C., Boer, Judith M., Beverloo, H. Berna, Sleight, Barbara, Chen, Ying, Vormoor-Bürger, Britta, Rives, Susana, Bielorai, Bella, Rössig, Claudia, Petit, Arnaud, Rizzari, Carmelo, Engstler, Gernot, Starý, Jan, Bautista Sirvent, Francisco J., Chen-Santel, Christiane, Bruno, Benedicte, Bertrand, Yves, Rialland, Fanny, Plat, Geneviève, Reinhardt, Dirk, Vinti, Luciana, Von Stackelberg, Arend, Locatelli, Franco, and Zwaan, Christian M.

Abstract

Inotuzumab Ozogamicin is a CD22-directed antibody conjugated to calicheamicin, approved in adults with relapsed or refractory (R/R) B cell acute lymphoblastic leukemia (BCP-ALL). Patients aged 1–18 years, with R/R CD22 + BCP-ALL were treated at the RP2D of 1.8 mg/m2. Using a single-stage design, with an overall response rate (ORR) ≤ 30% defined as not promissing and ORR > 55% as expected, 25 patients needed to be recruited to achieve 80% power at 0.05 significance level. Thirty-two patients were enrolled, 28 were treated, 27 were evaluable for response. The estimated ORR was 81.5% (95%CI: 61.9–93.7%), and 81.8% (18/22) of the responding subjects were minimal residual disease (MRD) negative. The study met its primary endpoint. Median follow up of survivors was 16 months (IQR: 14.49–20.07). One year Event Free Survival was 36.7% (95% CI: 22.2–60.4%), and Overall Survival was 55.1% (95% CI: 39.1−77.7%). Eighteen patients received consolidation (with HSCT and/or CAR T-cells therapy). Sinusoidal obstructive syndrome (SOS) occurred in seven patients. MRD negativity seemed correlated to calicheamicin sensitivity in vitro, but not to CD22 surface expression, saturation, or internalization. InO was effective in this population. The most relevant risk was the occurrence of SOS, particularly when InO treatment was followed by HSCT.

Published
2022

113. Dysregulation of Small Nucleolar RNAs in B-Cell Malignancies

Author

Verbeek, Martijn W.C., Erkeland, Stefan J., van der Velden, Vincent H.J., Verbeek, Martijn W.C., Erkeland, Stefan J., and van der Velden, Vincent H.J.

Abstract

Small nucleolar RNAs (snoRNAs) are responsible for post-transcriptional modification of ribosomal RNAs, transfer RNAs and small nuclear RNAs, and thereby have important regulatory functions in mRNA splicing and protein translation. Several studies have shown that snoRNAs are dysregulated in human cancer and may play a role in cancer initiation and progression. In this review, we focus on the role of snoRNAs in normal and malignant B-cell development. SnoRNA activity appears to be essential for normal B-cell differentiation and dysregulated expression of sno-RNAs is determined in B-cell acute lymphoblastic leukemia, chronic lymphocytic leukemia, B-cell non-Hodgkin’s lymphoma, and plasma cell neoplasms. SnoRNA expression is associated with cytogenetic/molecular subgroups and clinical outcome in patients with B-cell malignancies. Translocations involving snoRNAs have been described as well. Here, we discuss the different aspects of snoRNAs in B-cell malignancies and report on their role in oncogenic transformation, which may be useful for the development of novel diagnostic biomarkers or therapeutic targets.

Published
2022

114. Identification of High-Risk Multiple Myeloma With a Plasma Cell Leukemia-Like Transcriptomic Profile

Author

Hofste Op Bruinink, Davine, Kuiper, Rowan, van Duin, Mark, Cupedo, Tom, van der Velden, Vincent H J, Hoogenboezem, Remco, van der Holt, Bronno, Beverloo, H Berna, Valent, Erik T, Vermeulen, Michael, Gay, Francesca, Broijl, Annemiek, Avet-Loiseau, Hervé, Munshi, Nikhil C, Musto, Pellegrino, Moreau, Philippe, Zweegman, Sonja, van de Donk, Niels W C J, Sonneveld, Pieter, Hofste Op Bruinink, Davine, Kuiper, Rowan, van Duin, Mark, Cupedo, Tom, van der Velden, Vincent H J, Hoogenboezem, Remco, van der Holt, Bronno, Beverloo, H Berna, Valent, Erik T, Vermeulen, Michael, Gay, Francesca, Broijl, Annemiek, Avet-Loiseau, Hervé, Munshi, Nikhil C, Musto, Pellegrino, Moreau, Philippe, Zweegman, Sonja, van de Donk, Niels W C J, and Sonneveld, Pieter

Abstract

PURPOSE: Primary plasma cell leukemia (pPCL) is an aggressive subtype of multiple myeloma, which is distinguished from newly diagnosed multiple myeloma (NDMM) on the basis of the presence of ≥ 20% circulating tumor cells (CTCs). A molecular marker for pPCL is currently lacking, which could help identify NDMM patients with high-risk PCL-like disease, despite not having been recognized as such clinically. METHODS: A transcriptomic classifier for PCL-like disease was bioinformatically constructed and validated by leveraging information on baseline CTC levels, tumor burden, and tumor transcriptomics from 154 patients with NDMM included in the Cassiopeia or HO143 trials and 29 patients with pPCL from the EMN12/HO129 trial. Its prognostic value was assessed in an independent cohort of 2,139 patients with NDMM from the HOVON-65/GMMG-HD4, HOVON-87/NMSG-18, EMN02/HO95, MRC-IX, Total Therapy 2, Total Therapy 3, and MMRF CoMMpass studies. RESULTS: High CTC levels were associated with the expression of 1,700 genes, independent of tumor burden (false discovery rate < 0.05). Of these, 54 genes were selected by leave-one-out cross-validation to construct a transcriptomic classifier representing PCL-like disease. This not only demonstrated a sensitivity of 93% to identify pPCL in the validation cohort but also classified 10% of NDMM tumors as PCL-like. PCL-like MM transcriptionally and cytogenetically resembled pPCL, but presented with significantly lower CTC levels and tumor burden. Multivariate analyses in NDMM confirmed the significant prognostic value of PCL-like status in the context of Revised International Staging System stage, age, and treatment, regarding both progression-free (hazard ratio, 1.64; 95% CI, 1.30 to 2.07) and overall survival (hazard ratio, 1.89; 95% CI, 1.42 to 2.50). CONCLUSION: pPCL was identified on the basis of a specific tumor transcriptome, which was also present in patients with high-risk NDMM, despite not being clinically leukemic. Incorporatin

Published
2022

115. Expert-independent classification of mature B-cell neoplasms using standardized flow cytometry:a multicentric study

Author

Bottcher, Sebastian, Engelmann, Robby, Grigore, Georgiana, Fernandez, Paula, Caetano, Joana, Flores-Montero, Juan, van der Velden, Vincent H.J., Novakova, Michaela, Philippe, Jan, Ritgen, Matthias, Burgos, Leire, Lecrevisse, Quentin, Lange, Sandra, Kalina, Tomas, Velasco, Javier Verde, Rodriguez, Rafael Fluxa, van Dongen, Jacques J.M., Pedreira, Carlos E., Orfao, Alberto, Bottcher, Sebastian, Engelmann, Robby, Grigore, Georgiana, Fernandez, Paula, Caetano, Joana, Flores-Montero, Juan, van der Velden, Vincent H.J., Novakova, Michaela, Philippe, Jan, Ritgen, Matthias, Burgos, Leire, Lecrevisse, Quentin, Lange, Sandra, Kalina, Tomas, Velasco, Javier Verde, Rodriguez, Rafael Fluxa, van Dongen, Jacques J.M., Pedreira, Carlos E., and Orfao, Alberto

Abstract

Reproducible expert-independent flow-cytometric criteria for the differential diagnoses between mature B-cell neoplasms are lacking. We developed an algorithm-driven classification for these lymphomas by flow cytometry and compared it to the WHO gold standard diagnosis. Overall, 662 samples from 662 patients representing 9 disease categories were analyzed at 9 laboratories using the previously published EuroFlow 5-tube-8-color B-cell chronic lymphoproliferative disease antibody panel. Expression levels of all 26 markers from the panel were plotted by B-cell entity to construct a univariate, fully standardized diagnostic reference library. For multivariate data analysis, we subsequently used canonical correlation analysis of 176 training cases to project the multidimensional space of all 26 immunophenotypic parameters into 36 2-dimensional plots for each possible pairwise differential diagnosis. Diagnostic boundaries were fitted according to the distribution of the immunophenotypes of a given differential diagnosis. A diagnostic algorithm based on these projections was developed and subsequently validated using 486 independent cases. Negative predictive values exceeding 92.1% were observed for all disease categories except for follicular lymphoma. Particularly high positive predictive values were returned in chronic lymphocytic leukemia (99.1%), hairy cell leukemia (97.2%), follicular lymphoma (97.2%), and mantle cell lymphoma (95.4%). Burkitt and CD101 diffuse large B-cell lymphomas were difficult to distinguish by the algorithm. A similar ambiguity was observed between marginal zone, lymphoplasmacytic, and CD102 diffuse large B-cell lymphomas. The specificity of the approach exceeded 98% for all entities. The univariate immunophenotypic library and the multivariate expert-independent diagnostic algorithm might contribute to increased reproducibility of future diagnostics in mature B-cell neoplasms.

Published
2022

116. Impact of Pre-Analytical and Analytical Variables Associated with Sample Preparation on Flow Cytometric Stainings Obtained with EuroFlow Panels

Author

Sędek, Łukasz, Flores-Montero, Juan, van der Sluijs, Alita, Kulis, Jan, Marvelde, Jeroen Te, Philippé, Jan, Böttcher, Sebastian, Bitter, Marieke, Caetano, Joana, van der Velden, Vincent H.J., Sonneveld, Edwin, Buracchi, Chiara, Santos, Ana Helena, Lima, Margarida, Szczepański, Tomasz, van Dongen, Jacques J.M., Orfao, Alberto, Sędek, Łukasz, Flores-Montero, Juan, van der Sluijs, Alita, Kulis, Jan, Marvelde, Jeroen Te, Philippé, Jan, Böttcher, Sebastian, Bitter, Marieke, Caetano, Joana, van der Velden, Vincent H.J., Sonneveld, Edwin, Buracchi, Chiara, Santos, Ana Helena, Lima, Margarida, Szczepański, Tomasz, van Dongen, Jacques J.M., and Orfao, Alberto

Abstract

Objective interpretation of FC results may still be hampered by limited technical stan-dardization. The EuroFlow consortium conducted a series of experiments to determine the impact of different variables on the relative distribution and the median fluorescence intensity (MFI) of markers stained on different cell populations, from both healthy donors and patients’ samples with distinct hematological malignancies. The use of different anticoagulants; the time interval between sample collection, preparation, and acquisition; pH of washing buffers; and the use of cell surface membrane-only (SM) vs. cell surface plus intracytoplasmic (SM+CY) staining protocols, were evaluated. Our results showed that only monocytes were represented at higher percentages in EDTA-vs. heparin-anticoagulated samples. Application of SM or SM+CY protocols resulted in slight differences in the percentage of neutrophils and debris determined only with particular antibody combinations. In turn, storage of samples for 24 h at RT was associated with greater percentage of debris and cell doublets when the plasma cell disorder panel was used. Furthermore, 24 h storage of stained cells at RT was selectively detrimental for MFI levels of CD19 and CD45 on mature B-and T-cells (but not on leukemic blasts, clonal B-and plasma cells, neutrophils, and NK cells). The obtained results showed that the variables evaluated might need to be tailored for sample and cell type(s) as well as to the specific markers compared; however, defining of well-balanced boundaries for storage time, staining-to-acquisition delay, and pH of washing buffer would be a valid recommendation for most applications and circumstances described herein.

Published
2022

117. Immunophenotypic Analysis of Acute Megakaryoblastic Leukemia: A EuroFlow Study

Author

Brouwer, Nienke, Matarraz, Sergio, Nierkens, Stefan, Hofmans, Mattias, Nováková, Michaela, da Costa, Elaine Sobral, Fernandez, Paula, Bras, Anne E, de Mello, Fabiana Vieira, Mejstrikova, Ester, Philippé, Jan, Grigore, Georgiana Emilia, Pedreira, Carlos E, van Dongen, Jacques J M, Orfao, Alberto, van der Velden, Vincent H J, On Behalf Of The EuroFlow Consortium, Brouwer, Nienke, Matarraz, Sergio, Nierkens, Stefan, Hofmans, Mattias, Nováková, Michaela, da Costa, Elaine Sobral, Fernandez, Paula, Bras, Anne E, de Mello, Fabiana Vieira, Mejstrikova, Ester, Philippé, Jan, Grigore, Georgiana Emilia, Pedreira, Carlos E, van Dongen, Jacques J M, Orfao, Alberto, van der Velden, Vincent H J, and On Behalf Of The EuroFlow Consortium

Published
2022

119. Implementation of flow cytometry in the diagnostic work-up of myelodysplastic syndromes in a multicenter approach: Report from the Dutch Working Party on Flow Cytometry in MDS

Author

Westers, Theresia M., van der Velden, Vincent H.J., Alhan, Canan, Bekkema, Roelof, Bijkerk, André, Brooimans, Rik A., Cali, Claudia, Dräger, Angelika M., de Haas, Valerie, Homburg, Christa, de Jong, Anja, Kuiper-Kramer, P. (Ellen) A., Leenders, Marije, Lommerse, Ingrid, te Marvelde, Jeroen G., van der Molen-Sinke, Joke K., Moshaver, Bijan, Mulder, Andre B., Preijers, Frank W.M.B., Schindhelm, Roger K., van der Sluijs, Alita, van Wering, Elisabeth R., Westra, August H., and van de Loosdrecht, Arjan A.

Published
2012
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120. Bone Marrow Stromal Cell Regeneration Profile in Treated B-Cell Precursor Acute Lymphoblastic Leukemia Patients: Association with MRD Status and Patient Outcome

Author

Oliveira, Elen, primary, Costa, Elaine S., additional, Ciudad, Juana, additional, Gaipa, Giuseppe, additional, Sedek, Łukasz, additional, Barrena, Susana, additional, Szczepanski, Tomasz, additional, Buracchi, Chiara, additional, Silvestri, Daniela, additional, Siqueira, Patrícia F. R., additional, Mello, Fabiana V., additional, Torres, Rafael C., additional, Oliveira, Leonardo M. R., additional, Fay-Neves, Isabelle V. C., additional, Sonneveld, Edwin, additional, van der Velden, Vincent H. J. van der, additional, Mejstrikova, Esther, additional, Ribera, Josep-Maria, additional, Conter, Valentino, additional, Schrappe, Martin, additional, van Dongen, Jacques J. M. van, additional, Land, Marcelo G. P., additional, and Orfao, Alberto Orfao, additional

Published
2022
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122. Molecular characterisation and clinical outcome of B-cell precursor acute lymphoblastic leukaemia with IG-MYC rearrangement

Author

Bomken, Simon, primary, Enshaei, Amir, additional, Schwalbe, Edward C, additional, Mikulasova, Aneta, additional, Dai, Yunfeng, additional, Zaka, Masood, additional, Fung, Kent TM, additional, Bashton, Matthew, additional, Lim, Huezin, additional, Jones, Lisa, additional, Karataraki, Nefeli, additional, Winterman, Emily, additional, Ashby, Cody, additional, Attarbaschi, Andishe, additional, Bertrand, Yves, additional, Bradtke, Jutte, additional, Buldini, Barbara, additional, Burke, GA Amos, additional, Cazzaniga, Giovanni, additional, Gohring, Gudrun, additional, De Groot-Kruseman, Hesta A, additional, Haferlach, Claudia, additional, Nigro, Luca Lo, additional, Parihar, Mayur, additional, Plesa, Adriana, additional, Seaford, Emma, additional, Sonneveld, Edwin, additional, Strehl, Sabine, additional, Van der Velden, Vincent HJ, additional, Rand, Vikki, additional, Hunger, Stephen P, additional, Harrison, Christine J, additional, Bacon, Chris M, additional, Van Delft, Frederik W, additional, Loh, Mignon L, additional, Moppett, John, additional, Vormoor, Josef, additional, Walker, Brian A, additional, Moorman, Anthony V, additional, and Russell, Lisa J, additional

Published
2022
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124. Additional file 1 of Longitudinal minimal residual disease assessment in multiple myeloma patients in complete remission ��� results from the NMSG flow-MRD substudy within the EMN02/HO95 MM trial

Author

Schmitz, Alexander, Br��ndum, Rasmus Froberg, Johnsen, Hans Erik, Mellqvist, Ulf-Henrik, Waage, Anders, Gimsing, Peter, op Bruinink, Davine Hofste, van der Velden, Vincent, van der Holt, Bronno, Hansson, Markus, Andersen, Niels Frost, Fr��lund, Ulf Christian, Helleberg, Carsten, Schjesvold, Fredrik H., Ahlberg, Lucia, Gulbrandsen, Nina, Andreasson, Bjorn, Lauri, Birgitta, Haukas, Einar, B��dker, Julie St��ve, Roug, Anne Stidsholt, B��gsted, Martin, Severinsen, Marianne T., Gregersen, Henrik, Abildgaard, Niels, Sonneveld, Pieter, and Dybk��r, Karen

Subjects
Data_FILES
Abstract

Additional file 1.

Published
2022
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127. Impact of Pre-Analytical and Analytical Variables Associated with Sample Preparation on Flow Cytometric Stainings Obtained with EuroFlow Panels

Author

Sędek, Łukasz, primary, Flores-Montero, Juan, additional, van der Sluijs, Alita, additional, Kulis, Jan, additional, te Marvelde, Jeroen, additional, Philippé, Jan, additional, Böttcher, Sebastian, additional, Bitter, Marieke, additional, Caetano, Joana, additional, van der Velden, Vincent H. J., additional, Sonneveld, Edwin, additional, Buracchi, Chiara, additional, Santos, Ana Helena, additional, Lima, Margarida, additional, Szczepański, Tomasz, additional, van Dongen, Jacques J. M., additional, and Orfao, Alberto, additional

Published
2022
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129. Flow cytometric analysis of myelodysplasia: Pre‐analytical and technical issues—Recommendations from the European LeukemiaNet.

Author

van der Velden, Vincent H. J., Preijers, Frank, Johansson, Ulrika, Westers, Theresia M., Dunlop, Alan, Porwit, Anna, Béné, Marie C., Valent, Peter, te Marvelde, Jeroen, Wagner‐Ballon, Orianne, Oelschlaegel, Uta, Saft, Leonie, Kordasti, Sharham, Ireland, Robin, Cremers, Eline, Alhan, Canan, Duetz, Carolien, Hobo, Willemijn, Chapuis, Nicolas, and Fontenay, Michaela

Published
2023
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131. Clinical application of flow cytometry in patients with unexplained cytopenia and suspected myelodysplastic syndrome: A report of the European LeukemiaNet International MDS‐Flow Cytometry Working Group

Author

van de Loosdrecht, Arjan A., primary, Kern, Wolfgang, additional, Porwit, Anna, additional, Valent, Peter, additional, Kordasti, Sharham, additional, Cremers, Eline, additional, Alhan, Canan, additional, Duetz, Carolien, additional, Dunlop, Alan, additional, Hobo, Willemijn, additional, Preijers, Frank, additional, Wagner‐Ballon, Orianne, additional, Chapuis, Nicolas, additional, Fontenay, Michaela, additional, Bettelheim, Peter, additional, Eidenschink‐Brodersen, Lisa, additional, Font, Patricia, additional, Johansson, Ulrika, additional, Loken, Michael R., additional, te Marvelde, Jeroen G., additional, Matarraz, Sergio, additional, Ogata, Kiyoyuki, additional, Oelschlaegel, Uta, additional, Orfao, Alberto, additional, Psarra, Katherina, additional, Subirá, Dolores, additional, Wells, Denise A., additional, Béné, Marie C., additional, Della Porta, Matteo G., additional, Burbury, Kate, additional, Bellos, Frauke, additional, van der Velden, Vincent H. J., additional, Westers, Theresia M., additional, Saft, Leonie, additional, and Ireland, Robin, additional

Published
2021
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132. Flow cytometric analysis of myelodysplasia: Pre‐analytical and technical issues—Recommendations from the European LeukemiaNet

Author

van der Velden, Vincent H. J., primary, Preijers, Frank, additional, Johansson, Ulrika, additional, Westers, Theresia M., additional, Dunlop, Alan, additional, Porwit, Anna, additional, Béné, Marie C., additional, Valent, Peter, additional, te Marvelde, Jeroen, additional, Wagner‐Ballon, Orianne, additional, Oelschlaegel, Uta, additional, Saft, Leonie, additional, Kordasti, Sharham, additional, Ireland, Robin, additional, Cremers, Eline, additional, Alhan, Canan, additional, Duetz, Carolien, additional, Hobo, Willemijn, additional, Chapuis, Nicolas, additional, Fontenay, Michaela, additional, Bettelheim, Peter, additional, Eidenshink‐Brodersen, Lisa, additional, Font, Patricia, additional, Loken, Michael R., additional, Matarraz, Sergio, additional, Ogata, Kiyoyuki, additional, Orfao, Alberto, additional, Psarra, Katherina, additional, Subirá, Dolores, additional, Wells, Denise A., additional, Della Porta, Matteo G., additional, Burbury, Kate, additional, Bellos, Frauke, additional, Weiß, Elisabeth, additional, Kern, Wolfgang, additional, and van de Loosdrecht, Arjan, additional

Published
2021
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133. NGS-Based MRD Quantitation: An Alternative to qPCR Validated on a Large Consecutive Cohort of Children with ALL

Author

Svaton, Michael, primary, Skotnicova, Aneta, additional, Reznickova, Leona, additional, Rennerova, Andrea, additional, Valova, Tatana, additional, Kotrova, Michaela, additional, van der Velden, Vincent H.J., additional, Brüggemann, Monika, additional, Darzentas, Nikos, additional, Langerak, Anton W., additional, Zuna, Jan, additional, Stary, Jan, additional, Trka, Jan, additional, and Fronkova, Eva, additional

Published
2021
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134. Impact of Maintenance Arm on Prognostic Value of MRD after Induction Treatment in MCL R2 Elderly Trial , a Mantle Cell Lymphoma Network Study

Author

Delfau, Marie-Helene, primary, Macintyre, Elizabeth A., additional, Callanan, Mary B., additional, Pott, Christiane, additional, Van Der Velden, Vincent H.J., additional, Homburg, Christa, additional, Garcia-Sanz, Ramon, additional, Gameiro, Paula, additional, Gomes Da Silva, Maria, additional, Klapper, Wolfram, additional, Oberic, Lucie, additional, Feugier, Pierre, additional, Safar, Violaine, additional, Casasnovas, Olivier, additional, Dreyling, Martin H., additional, and Ribrag, Vincent, additional

Published
2021
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135. A Phase I/II Study of Bosutinib in Pediatric Patients with Resistant/Intolerant or Newly Diagnosed Philadelphia Chromosome-Positive Chronic Myeloid Leukemia, Study ITCC (Innovative Therapies for Children with Cancer European Consortium) 054 and COG (Children's Oncology Group Consortium) AAML1921: Results from the Phase I Trial in Resistant/Intolerant Patients

Author

Pennesi, Edoardo, primary, Brivio, Erica, additional, Willemse, Marieke E., additional, Huitema, Alwin D. R., additional, Chandra, Saurabh, additional, Vijayakumar, Ashwini, additional, Van Der Velden, Vincent H.J., additional, Beverloo, H. Berna, additional, Durairaj, Chandra, additional, Viqueira, Andrea, additional, Ingrosso, Antonella, additional, Locatelli, Franco, additional, Motwani, Jayashree, additional, Bourquin, Jean-Pierre, additional, Bautista Sirvent, Francisco J., additional, Rizzari, Carmelo, additional, Petit, Arnaud, additional, Lancaster, Donna, additional, Metzler, Markus, additional, Bertrand, Yves, additional, Murillo-Sanjuán, Laura, additional, Bukowkinski, Andrew J., additional, Krystal, Julie, additional, Van Der Sluis, Inge M., additional, Roth, Michael E., additional, Van Tinteren, Harm, additional, Hijiya, Nobuko, additional, and Zwaan, Christian M., additional

Published
2021
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136. Minimal Residual Disease and Outcome Characteristics in Infant KMT2A-Germline Acute Lymphoblastic Leukemia Treated on the Interfant-06 Protocol

Author

Stutterheim, Janine, primary, De Lorenzo, Paola, additional, Van Der Sluis, Inge M., additional, Alten, Julia, additional, Ancliffe, Philip, additional, Attarbaschi, Andishe, additional, Aversa, Luis Alberto, additional, Boer, Judith M., additional, Biondi, Andrea, additional, Brethon, Benoit, additional, Diaz, Paulina, additional, Gazzaniga, Giovanni, additional, Escherich, Gabriele, additional, Ferster, Alina, additional, Kotecha, Rishi S, additional, Lausen, Birgitte, additional, Leung, Alex WK, additional, Locatelli, Franco, additional, Silverman, Lewis B., additional, Stary, Jan, additional, Szczepanski, Tomasz, additional, Van Der Velden, Vincent H.J., additional, Vora, Ajay, additional, Zuna, Jan, additional, Schrappe, Martin, additional, Grazia Valsecchi, Maria, additional, and Pieters, Rob, additional

Published
2021
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137. High Levels of Circulating Tumor Cells Are Associated with Increased Bone Marrow Proliferation in Newly Diagnosed Multiple Myeloma Patients

Author

Fokkema, Cathelijne, primary, de Jong, Madelon M.E., additional, Tahri, Sabrin, additional, Kellermayer, Zoltan, additional, den Hollander, Chelsea, additional, Vermeulen, Michael, additional, Papazian, Natalie, additional, Duin, Mark van, additional, Wevers, Michiel J.W., additional, Sanders, Mathijs A., additional, van der Velden, Vincent H.J., additional, Sonneveld, Pieter, additional, Broyl, Annemiek, additional, and Cupedo, Tom, additional

Published
2021
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138. The tumor suppressor MIR139 is silenced by POLR2M to promote AML oncogenesis

Author

Stavast, Christiaan J., primary, van Zuijen, Iris, additional, Karkoulia, Elena, additional, Özçelik, Arman, additional, van Hoven-Beijen, Antoinette, additional, Leon, Leticia G., additional, Voerman, Jane S. A., additional, Janssen, George M. C., additional, van Veelen, Peter A., additional, Burocziova, Monika, additional, Brouwer, Rutger W. W., additional, van IJcken, Wilfred F. J., additional, Maas, Alex, additional, Bindels, Eric M., additional, van der Velden, Vincent H. J., additional, Schliehe, Christopher, additional, Katsikis, Peter D., additional, Alberich-Jorda, Meritxell, additional, and Erkeland, Stefan J., additional

Published
2021
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141. Potential and pitfalls of whole transcriptome-based immunogenetic marker identification in acute lymphoblastic leukemia; a EuroMRD and EuroClonality-NGS Working Group study

Author

van der Velden, Vincent H. J., Brueggemann, Monika, Cazzaniga, Giovanni, Scheijen, Blanca, Tops, Bastiaan, Trka, Jan, Pal, Karol, Haenzelmann, Sonja, Fazio, Grazia, Songia, Simona, Langerak, Anton W., Darzentas, Nikos, van der Velden, Vincent H. J., Brueggemann, Monika, Cazzaniga, Giovanni, Scheijen, Blanca, Tops, Bastiaan, Trka, Jan, Pal, Karol, Haenzelmann, Sonja, Fazio, Grazia, Songia, Simona, Langerak, Anton W., and Darzentas, Nikos

Published
2021

142. Automated identification of leukocyte subsets improves standardization of database-guided expert-supervised diagnostic orientation in acute leukemia: a EuroFlow study

Author

Lhermitte, L, Barreau, S, Morf, D, Fernandez, P, Grigore, G, Barrena, S, de Bie, Maaike, Flores-Montero, J, Brüggemann, M, Mejstrikova, E, Nierkens, S, Burgos, L, Caetano, J, Gaipa, G, Buracchi, C, Costa, ES, Sedek, L, Szczepa?ski, T, Aanei, CM, van der Sluijs-Gelling, A, Delgado, AH, Fluxa, R, Lecrevisse, Q, Pedreira, CE, Dongen, JJM, Orfao, A, van der Velden, Vincent, Lhermitte, L, Barreau, S, Morf, D, Fernandez, P, Grigore, G, Barrena, S, de Bie, Maaike, Flores-Montero, J, Brüggemann, M, Mejstrikova, E, Nierkens, S, Burgos, L, Caetano, J, Gaipa, G, Buracchi, C, Costa, ES, Sedek, L, Szczepa?ski, T, Aanei, CM, van der Sluijs-Gelling, A, Delgado, AH, Fluxa, R, Lecrevisse, Q, Pedreira, CE, Dongen, JJM, Orfao, A, and van der Velden, Vincent

Abstract

Precise classification of acute leukemia (AL) is crucial for adequate treatment. EuroFlow has previously designed an AL orientation tube (ALOT) to guide toward the relevant classification panel and final diagnosis. In this study, we designed and validated an algorithm for automated (database-supported) gating and identification (AGI tool) of cell subsets within samples stained with ALOT. A reference database of normal peripheral blood (PB, n = 41) and bone marrow (BM; n = 45) samples analyzed with the ALOT was constructed, and served as a reference for the AGI tool to automatically identify normal cells. Populations not unequivocally identified as normal cells were labeled as checks and were classified by an expert. Additional normal BM (n = 25) and PB (n = 43) and leukemic samples (n = 109), analyzed in parallel by experts and the AGI tool, were used to evaluate the AGI tool. Analysis of normal PB and BM samples showed low percentages of checks (<3% in PB, <10% in BM), with variations between different laboratories. Manual analysis and AGI analysis of normal and leukemic samples showed high levels of correlation between cell numbers (r2 > 0.95 for all cell types in PB and r2 > 0.75 in BM) and resulted in highly concordant classification of leukemic cells by our previously published automated database-guided expert-supervised orientation tool for immunophenotypic diagnosis and classification of acute leukemia (Compass tool). Similar data were obtained using alternative, commercially available tubes, confirming the robustness of the developed tools. The AGI tool represents an innovative step in minimizing human intervention and requirements in expertise, toward a “sample-in and result-out” approach which may result in more objective and reproducible data analysis and diagnostics. The AGI tool may improve quality of immunophenotyping in individual laboratories, since high percentages of checks in normal samples are an alert on the

Published
2021

143. Minimal residual disease, long-term outcome, and IKZF1 deletions in children and adolescents with Down syndrome and acute lymphocytic leukaemia:a matched cohort study

Author

Michels, Naomi, Boer, Judith M., Enshaei, Amir, Sutton, Rosemary, Heyman, Mats, Ebert, Sabine, Fiocco, Marta, de Groot-Kruseman, Hester A., van der Velden, Vincent H.J., Barbany, Gisela, Escherich, Gabriele, Vora, Ajay, Trahair, Toby, Dalla-Pozza, Luciano, Pieters, Rob, zur Stadt, Udo, Schmiegelow, Kjeld, Moorman, Anthony V., Zwaan, C. Michel, den Boer, Monique L., Michels, Naomi, Boer, Judith M., Enshaei, Amir, Sutton, Rosemary, Heyman, Mats, Ebert, Sabine, Fiocco, Marta, de Groot-Kruseman, Hester A., van der Velden, Vincent H.J., Barbany, Gisela, Escherich, Gabriele, Vora, Ajay, Trahair, Toby, Dalla-Pozza, Luciano, Pieters, Rob, zur Stadt, Udo, Schmiegelow, Kjeld, Moorman, Anthony V., Zwaan, C. Michel, and den Boer, Monique L.

Abstract

Background: Patients with Down syndrome and acute lymphocytic leukaemia are at an increased risk of treatment-related mortality and relapse, which is influenced by unfavourable genetic aberrations (eg, IKZF1 deletion). We aimed to investigate the potential underlying effect of Down syndrome versus the effects of adverse cancer genetics on clinical outcome. Method: Patients (aged 1–23 years) with Down syndrome and acute lymphocytic leukaemia and matched non-Down syndrome patients with acute lymphocytic leukaemia (matched controls) from eight trials (DCOG ALL10 and ALL11, ANZCHOG ALL8, AIEOP-BFM ALL2009, UKALL2003, NOPHO ALL2008, CoALL 07-03, and CoALL 08-09) done between 2002 and 2018 across various countries (the Netherlands, the UK, Australia, Denmark, Finland, Iceland, Norway, Sweden, and Germany) were included. Participants were matched (1:3) for clinical risk factors and genetics, including IKZF1 deletion. The primary endpoint was the comparison of MRD levels (absolute MRD levels were categorised into two groups, low [<0·0001] and high [≥0·0001]) between patients with Down syndrome and acute lymphocytic leukaemia and matched controls, and the secondary outcomes were comparison of long-term outcomes (event-free survival, overall survival, relapse, and treatment-related mortality [TRM]) between patients with Down syndrome and acute lymphocytic leukaemia and matched controls. Two matched cohorts were formed: for MRD analyses and for long-term outcome analyses. For both cohorts, matching was based on induction regimen; for the long-term outcome cohort, matching also included MRD-guided treatment group. We used mixed-effect models, Cox models, and competing risk for statistical analyses. Findings: Of 251 children and adolescents with Down syndrome and acute lymphocytic leukaemia, 136 were eligible for analyses and matched to 407 (of 8426) non-Down syndrome patients with acute lymphocytic leukaemia (matched controls). 113 patients with Down syndrome and acute ly

Published
2021

144. Clinical Implications of Minimal Residual Disease Detection in Infants With KMT2A-Rearranged Acute Lymphoblastic Leukemia Treated on the Interfant-06 Protocol

Author

Stutterheim, J, van der Sluis, I, de Lorenzo, P, Alten, J, Ancliffe, P, Attarbaschi, A, Brethon, B, Biondi, A, Campbell, M, Cazzaniga, G, Escherich, G, Ferster, A, Kotecha, R, Lausen, B, Li, C, Lo Nigro, L, Locatelli, F, Marschalek, R, Meyer, C, Schrappe, M, Stary, J, Vora, A, Zuna, J, van der Velden, V, Szczepanski, T, Valsecchi, M, Pieters, R, Stutterheim, Janine, van der Sluis, Inge M, de Lorenzo, Paola, Alten, Julia, Ancliffe, Philip, Attarbaschi, Andishe, Brethon, Benoit, Biondi, Andrea, Campbell, Myriam, Cazzaniga, Giovanni, Escherich, Gabriele, Ferster, Alina, Kotecha, Rishi S, Lausen, Birgitte, Li, Chi Kong, Lo Nigro, Luca, Locatelli, Franco, Marschalek, Rolf, Meyer, Claus, Schrappe, Martin, Stary, Jan, Vora, Ajay, Zuna, Jan, van der Velden, Vincent H J, Szczepanski, Tomasz, Valsecchi, Maria Grazia, Pieters, Rob, Stutterheim, J, van der Sluis, I, de Lorenzo, P, Alten, J, Ancliffe, P, Attarbaschi, A, Brethon, B, Biondi, A, Campbell, M, Cazzaniga, G, Escherich, G, Ferster, A, Kotecha, R, Lausen, B, Li, C, Lo Nigro, L, Locatelli, F, Marschalek, R, Meyer, C, Schrappe, M, Stary, J, Vora, A, Zuna, J, van der Velden, V, Szczepanski, T, Valsecchi, M, Pieters, R, Stutterheim, Janine, van der Sluis, Inge M, de Lorenzo, Paola, Alten, Julia, Ancliffe, Philip, Attarbaschi, Andishe, Brethon, Benoit, Biondi, Andrea, Campbell, Myriam, Cazzaniga, Giovanni, Escherich, Gabriele, Ferster, Alina, Kotecha, Rishi S, Lausen, Birgitte, Li, Chi Kong, Lo Nigro, Luca, Locatelli, Franco, Marschalek, Rolf, Meyer, Claus, Schrappe, Martin, Stary, Jan, Vora, Ajay, Zuna, Jan, van der Velden, Vincent H J, Szczepanski, Tomasz, Valsecchi, Maria Grazia, and Pieters, Rob

Abstract

Purpose: Infant acute lymphoblastic leukemia (ALL) is characterized by a high incidence of KMT2A gene rearrangements and poor outcome. We evaluated the value of minimal residual disease (MRD) in infants with KMT2A-rearranged ALL treated within the Interfant-06 protocol, which compared lymphoid-style consolidation (protocol IB) versus myeloid-style consolidation (araC, daunorubicin, etoposide/mitoxantrone, araC, etoposide). Materials and methods: MRD was measured in 249 infants by DNA-based polymerase chain reaction of rearranged KMT2A, immunoglobulin, and/or T-cell receptor genes, at the end of induction (EOI) and end of consolidation (EOC). MRD results were classified as negative, intermediate (< 5 × 10-4), and high (≥ 5 × 10-4). Results: EOI MRD levels predicted outcome with 6-year disease-free survival (DFS) of 60.2% (95% CI, 43.2 to 73.6), 45.0% (95% CI, 28.3 to 53.1), and 33.8% (95% CI, 23.8 to 44.1) for infants with negative, intermediate, and high EOI MRD levels, respectively (P = .0039). EOC MRD levels were also predictive of outcome, with 6-year DFS of 68.2% (95% CI, 55.2 to 78.1), 40.1% (95% CI, 28.1 to 51.9), and 11.9% (95% CI, 2.6 to 29.1) for infants with negative, intermediate, and high EOC MRD levels, respectively (P < .0001). Analysis of EOI MRD according to the type of consolidation treatment showed that infants treated with lymphoid-style consolidation had 6-year DFS of 78.2% (95% CI, 51.4 to 91.3), 47.2% (95% CI, 33.0 to 60.1), and 23.2% (95% CI, 12.1 to 36.4) for negative, intermediate, and high MRD levels, respectively (P < .0001), while for myeloid-style-treated patients the corresponding figures were 45.0% (95% CI, 23.9 to 64.1), 41.3% (95% CI, 23.2 to 58.5), and 45.9% (95% CI, 29.4 to 60.9). Conclusion: This study provides support for the idea that induction therapy selects patients for subsequent therapy; infants with high EOI MRD may benefit from AML-like consolidation (DFS 45.9% v 23.2%), whereas patients with low EOI MRD may bene

Published
2021

145. Clinical Implications of Minimal Residual Disease Detection in Infants With KMT2A-Rearranged Acute Lymphoblastic Leukemia Treated on the Interfant-06 Protocol

Author

Stutterheim, Janine, van der Sluis, Inge M., de Lorenzo, Paola, Alten, Julia, Ancliffe, Philip, Attarbaschi, Andishe, Brethon, Benoit, Biondi, Andrea, Campbell, Myriam, Cazzaniga, Giovanni, Escherich, Gabriele, Ferster, Alina, Kotecha, Rishi S., Lausen, Birgitte, Li, Chi Kong, Lo Nigro, Luca, Locatelli, Franco, Marschalek, Rolf, Meyer, Claus, Schrappe, Martin, Stary, Jan, Vora, Ajay, Zuna, Jan, van der Velden, Vincent H.J., Szczepanski, Tomasz, Valsecchi, Maria Grazia, Pieters, Rob, Stutterheim, Janine, van der Sluis, Inge M., de Lorenzo, Paola, Alten, Julia, Ancliffe, Philip, Attarbaschi, Andishe, Brethon, Benoit, Biondi, Andrea, Campbell, Myriam, Cazzaniga, Giovanni, Escherich, Gabriele, Ferster, Alina, Kotecha, Rishi S., Lausen, Birgitte, Li, Chi Kong, Lo Nigro, Luca, Locatelli, Franco, Marschalek, Rolf, Meyer, Claus, Schrappe, Martin, Stary, Jan, Vora, Ajay, Zuna, Jan, van der Velden, Vincent H.J., Szczepanski, Tomasz, Valsecchi, Maria Grazia, and Pieters, Rob

Abstract

PURPOSE: Infant acute lymphoblastic leukemia (ALL) is characterized by a high incidence of KMT2A gene rearrangements and poor outcome. We evaluated the value of minimal residual disease (MRD) in infants with KMT2A-rearranged ALL treated within the Interfant-06 protocol, which compared lymphoid-style consolidation (protocol IB) versus myeloid-style consolidation (araC, daunorubicin, etoposide/mitoxantrone, araC, etoposide). MATERIALS AND METHODS: MRD was measured in 249 infants by DNA-based polymerase chain reaction of rearranged KMT2A, immunoglobulin, and/or T-cell receptor genes, at the end of induction (EOI) and end of consolidation (EOC). MRD results were classified as negative, intermediate (< 5 × 10-4), and high (≥ 5 × 10-4). RESULTS: EOI MRD levels predicted outcome with 6-year disease-free survival (DFS) of 60.2% (95% CI, 43.2 to 73.6), 45.0% (95% CI, 28.3 to 53.1), and 33.8% (95% CI, 23.8 to 44.1) for infants with negative, intermediate, and high EOI MRD levels, respectively (P = .0039). EOC MRD levels were also predictive of outcome, with 6-year DFS of 68.2% (95% CI, 55.2 to 78.1), 40.1% (95% CI, 28.1 to 51.9), and 11.9% (95% CI, 2.6 to 29.1) for infants with negative, intermediate, and high EOC MRD levels, respectively (P < .0001). Analysis of EOI MRD according to the type of consolidation treatment showed that infants treated with lymphoid-style consolidation had 6-year DFS of 78.2% (95% CI, 51.4 to 91.3), 47.2% (95% CI, 33.0 to 60.1), and 23.2% (95% CI, 12.1 to 36.4) for negative, intermediate, and high MRD levels, respectively (P < .0001), while for myeloid-style-treated patients the corresponding figures were 45.0% (95% CI, 23.9 to 64.1), 41.3% (95% CI, 23.2 to 58.5), and 45.9% (95% CI, 29.4 to 60.9). CONCLUSION: This study provides support for the idea that induction therapy selects patients for subsequent therapy; infants with high EOI MRD may benefit from AML-like consolidation (DFS 45.9% v 23.2%), whereas patients with low EOI MRD may b

Published
2021

146. B-cell regeneration profile and minimal residual disease status in bone marrow of treated multiple myeloma patients

Author

de Pontes, Robéria Mendonça, Flores-Montero, Juan, Sanoja-Flores, Luzalba, Puig, Noemi, Pessoa de Magalhães, Roberto J., Corral-Mateos, Alba, Salgado, Anna Beatriz, García-Sánchez, Omar, Pérez-Morán, José, Mateos, Maria Victoria, Burgos, Leire, Paiva, Bruno, Marvelde, Jeroen Te, van der Velden, Vincent H.J., Aguilar, Carlos, Bárez, Abelardo, García-Mateo, Aranzazú, Labrador, Jorge, Leoz, Pilar, Aguilera-Sanz, Carmen, Durie, Brian, van Dongen, Jacques J.M., Maiolino, Angelo, da Costa, Elaine Sobral, Orfao, Alberto, de Pontes, Robéria Mendonça, Flores-Montero, Juan, Sanoja-Flores, Luzalba, Puig, Noemi, Pessoa de Magalhães, Roberto J., Corral-Mateos, Alba, Salgado, Anna Beatriz, García-Sánchez, Omar, Pérez-Morán, José, Mateos, Maria Victoria, Burgos, Leire, Paiva, Bruno, Marvelde, Jeroen Te, van der Velden, Vincent H.J., Aguilar, Carlos, Bárez, Abelardo, García-Mateo, Aranzazú, Labrador, Jorge, Leoz, Pilar, Aguilera-Sanz, Carmen, Durie, Brian, van Dongen, Jacques J.M., Maiolino, Angelo, da Costa, Elaine Sobral, and Orfao, Alberto

Abstract

B-cell regeneration during therapy has been considered as a strong prognostic factor in multiple myeloma (MM). However, the effects of therapy and hemodilution in bone marrow (BM) B-cell recovery have not been systematically evaluated during follow-up. MM (n = 177) and adult (≥50y) healthy donor (HD; n = 14) BM samples were studied by next-generation flow (NGF) to simultaneously assess measurable residual disease (MRD) and residual normal B-cell populations. BM hemodilution was detected in 41 out of 177 (23%) patient samples, leading to lower total B-cell, B-cell precursor (BCP) and normal plasma cell (nPC) counts. Among MM BM, decreased percentages (vs. HD) of BCP, transitional/naïve B-cell (TBC/NBC) and nPC populations were observed at diagnosis. BM BCP increased after induction therapy, whereas TBC/NBC counts remained abnormally low. At day+100 postautologous stem cell transplantation, a greater increase in BCP with recovered TBC/NBC cell numbers but persistently low memory B-cell and nPC counts were found. At the end of therapy, complete response (CR) BM samples showed higher CD19− nPC counts vs. non-CR specimens. MRD positivity was associated with higher BCP and nPC percentages. Hemodilution showed a negative impact on BM B-cell distribution. Different BM B-cell regeneration profiles are present in MM at diagnosis and after therapy with no significant association with patient outcome.

Published
2021

147. Increased group 2 innate lymphoid cells in peripheral blood of adults with mastocytosis

Author

van der Ploeg, Esmee K., Hermans, Maud A.W., van der Velden, Vincent H.J., Dik, Willem A., van Daele, Paul L.A., Stadhouders, Ralph, van der Ploeg, Esmee K., Hermans, Maud A.W., van der Velden, Vincent H.J., Dik, Willem A., van Daele, Paul L.A., and Stadhouders, Ralph

Abstract

Background: Systemic mastocytosis is a hematological disease in which aberrant mast cells accumulate because of gain-of-function mutations in the KIT receptor. Group 2 innate lymphoid cells (ILC2s) are effector cells of type 2 immune responses that also express KIT and colocalize with mast cells at barrier tissue sites. In mouse models, mast cell-ILC2 crosstalk can drive local inflammation. However, a possible role for ILC2s in the pathophysiology of mastocytosis remains unexplored. Objective: We sought to characterize circulating ILC2s in a clinically diverse cohort of patients with mastocytosis. Methods: We included 21 adults with systemic mastocytosis and 18 healthy controls. Peripheral blood ILC2 abundance and phenotype were analyzed by flow cytometry and correlated to clinical characteristics, including the presence of the D816V KIT mutation. Results: ILC2 levels were significantly higher in D816V+ patients with mastocytosis compared with D816V− patients or healthy controls. We observed increased proportions of KIT+ ILC2s among patients with mastocytosis, regardless of D816V status. Patients with skin involvement and itch showed the highest levels of ILC2s, which was independent from atopy or serum tryptase levels. Allele-specific quantitative PCR showed that the vast majority of ILC2s did not carry the D816V mutation. Conclusions: Our findings suggest a role for ILC2s and pathogenic ILC2-mast cell crosstalk in mastocytosis. We hypothesize that a high cutaneous D816V+ mast cell burden alters the skin microenvironment to induce chronic local ILC2 activation and their dissemination into the circulation. Activated ILC2s could contribute to skin symptoms by producing inflammatory mediators and by further augmenting mast cell mediator release.

Published
2021

148. Antibodies Against Angiotensin II Receptor Type 1 and Endothelin A Receptor Are Associated With an Unfavorable COVID19 Disease Course

Author

Miedema, Jelle, Schreurs, Marco, van der Sar – van der Brugge, Simone, Paats, Marthe, Baart, Sara, Bakker, Marleen, Hoek, Rogier, Dik, Willem Arnout, Endeman, Henrik, Van Der Velden, Vincent, van Gammeren, Adriaan, Ermens, Antonius, Aerts, Joachim G., Thüsen, Jan Von Der, Miedema, Jelle, Schreurs, Marco, van der Sar – van der Brugge, Simone, Paats, Marthe, Baart, Sara, Bakker, Marleen, Hoek, Rogier, Dik, Willem Arnout, Endeman, Henrik, Van Der Velden, Vincent, van Gammeren, Adriaan, Ermens, Antonius, Aerts, Joachim G., and Thüsen, Jan Von Der

Abstract

Background: Lung histopathology demonstrates vasculopathy in a subset of deceased COVID19 patients, which resembles histopathology observed in antibody-mediated lung transplant rejection. Autoantibodies against angiotensin II type 1 receptor (AT1R) and Endothelin receptor Type A (ETAR) have been demonstrated in antibody-mediated rejection and may also be associated with severe COVID19 infection. Objective To assess AT1R and ETAR auto-antibodies in COVID19 patients and controls, and explore their association with disease course. Methods: 65 hospitalized patients with COVID19 infection were included. Clinical and laboratory findings were retrospectively assessed. Patients with unfavorable disease course, admitted at the intensive care unit and/or deceased during hospital admission (n=33) were compared to admitted COVID19 patients with favorable disease course (n=32). The presence of antinuclear antibodies (ANA) and auto-antibodies against AT1R or ETAR in peripheral blood were compared between COVID19 with unfavorable and favorable disease course and age matched controls (n=20). Results: The presence of ANA was not significantly different between COVID19 patients with unfavorable (n=7/33; 21%) and favorable disease course (n=6/32; 19%) (p= 0.804) and controls (n=3/20; 15%). Auto-antibodies against AT1R were significantly increased in unfavorable disease course (median 14.59 U/mL, IQR 11.28 – 19.89) compared to favorable disease course (median 10.67 U/mL, IQR 8.55 – 13.0, p< 0.01). ETAR antibody titers were also significantly increased in unfavorable disease course (median 7.21, IQR 5.0 – 10.45) as compared to favorable disease course (median 4.0, IQR 3.0 – 6.0, p <0.05). Conclusion: Auto-antibodies against AT1R and ETAR are significantly increased in COVID19 patients with an unfavorable disease course.

Published
2021

149. Standardised immunophenotypic analysis of myeloperoxidase in acute leukaemia

Author

Bras, Anne E., Osmani, Zgjim, de Haas, Valerie, Jongen-Lavrencic, Mojca, te Marvelde, Jeroen G., Zwaan, C. Michel, Mejstrikova, Ester, Fernandez, Paula, Szczepanski, Tomasz, Orfao, Alberto, van Dongen, Jacques J.M., van der Velden, Vincent H.J., Bras, Anne E., Osmani, Zgjim, de Haas, Valerie, Jongen-Lavrencic, Mojca, te Marvelde, Jeroen G., Zwaan, C. Michel, Mejstrikova, Ester, Fernandez, Paula, Szczepanski, Tomasz, Orfao, Alberto, van Dongen, Jacques J.M., and van der Velden, Vincent H.J.

Abstract

Given its myeloid-restricted expression, myeloperoxidase (MPO) is typically used for lineage assignment (myeloid vs. lymphoid) during acute leukaemia (AL) diagnostics. In the present study, a robust flow cytometric definition for MPO positivity was established based on the standardised EuroFlow protocols, the standardised Acute Leukaemia Orientation Tube and 1734 multicentre AL cases (with confirmed assay stability). The best diagnostic performance was achieved by defining MPO positivity as ≥20% of the AL cells exceeding a lymphocyte-based threshold. The methodology employed should be applicable to any form of standardised flow cytometry.

Published
2021

150. Minimal residual disease (MRD) detection in acute lymphoblastic leukaemia based on fusion genes and genomic deletions:towards MRD for all

Author

Kuiper, Roland P., Hoogeveen, Patricia G., Bladergroen, Reno, van Dijk, Freerk, Sonneveld, Edwin, van Leeuwen, Frank N., Boer, Judith, Sergeeva, Irina, Feitsma, Harma, den Boer, Monique L., van der Velden, Vincent H.J., Kuiper, Roland P., Hoogeveen, Patricia G., Bladergroen, Reno, van Dijk, Freerk, Sonneveld, Edwin, van Leeuwen, Frank N., Boer, Judith, Sergeeva, Irina, Feitsma, Harma, den Boer, Monique L., and van der Velden, Vincent H.J.

Abstract

Minimal residual disease (MRD) diagnostics are implemented in most clinical protocols for patients with acute lymphoblastic leukaemia (ALL) and are mostly performed using rearranged immunoglobulin (IG) and/or T-cell receptor (TR) gene rearrangements as molecular polymerase chain reaction targets. Unfortunately, in 5–10% of patients no or no sensitive IG/TR targets are available, and patients therefore cannot be stratified appropriately. In the present study, we used fusion genes and genomic deletions as alternative MRD targets in these patients, which retrospectively revealed appropriate MDR stratification in 79% of patients with no (sensitive) IG/TR target, and a different risk group stratification in more than half of the cases.

Published
2021

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