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

Author

Young, E, Noerenberg, D, Mansouri, L, Ljungström, V, Frick, M, Sutton, L-A, Blakemore, SJ, Galan-Sousa, J, Plevova, K, Baliakas, P, Rossi, D, Clifford, R, Roos-Weil, D, Navrkalova, V, Dörken, B, Schmitt, CA, Smedby, KE, Juliusson, G, Giacopelli, B, Blachly, JS, Belessi, C, Panagiotidis, P, Chiorazzi, N, Davi, F, Langerak, AW, Oscier, D, Schuh, A, Gaidano, G, Ghia, P, Xu, W, Fan, L, Bernard, OA, Nguyen-Khac, F, Rassenti, L, Li, J, Kipps, TJ, Stamatopoulos, K, Pospisilova, S, Zenz, T, Oakes, CC, Strefford, JC, Rosenquist, R, and Damm, F

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Oncology and Carcinogenesis, Cancer, Hematology, Rare Diseases, Lymphoma, Clinical Research, Genetics, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, Adult, Aged, Early Growth Response Protein 2, Female, Genes, p53, Humans, Leukemia, Lymphocytic, Chronic, B-Cell, Male, Middle Aged, Mutation, Proportional Hazards Models, Clinical Sciences, Immunology, Cardiovascular medicine and haematology, Clinical sciences, Oncology and carcinogenesis
Abstract

Recurrent mutations within EGR2 were recently reported in advanced-stage chronic lymphocytic leukemia (CLL) patients and associated with a worse outcome. To study their prognostic impact, 2403 CLL patients were examined for mutations in the EGR2 hotspot region including a screening (n=1283) and two validation cohorts (UK CLL4 trial patients, n=366; CLL Research Consortium (CRC) patients, n=490). Targeted deep-sequencing of 27 known/postulated CLL driver genes was also performed in 38 EGR2-mutated patients to assess concurrent mutations. EGR2 mutations were detected in 91/2403 (3.8%) investigated cases, and associated with younger age at diagnosis, advanced clinical stage, high CD38 expression and unmutated IGHV genes. EGR2-mutated patients frequently carried ATM lesions (42%), TP53 aberrations (18%) and NOTCH1/FBXW7 mutations (16%). EGR2 mutations independently predicted shorter time-to-first-treatment (TTFT) and overall survival (OS) in the screening cohort; they were confirmed associated with reduced TTFT and OS in the CRC cohort and independently predicted short OS from randomization in the UK CLL4 cohort. A particularly dismal outcome was observed among EGR2-mutated patients who also carried TP53 aberrations. In summary, EGR2 mutations were independently associated with an unfavorable prognosis, comparable to CLL patients carrying TP53 aberrations, suggesting that EGR2-mutated patients represent a new patient subgroup with very poor outcome.

Published
2017

2. A complementary role of multiparameter flow cytometry and high-throughput sequencing for minimal residual disease detection in chronic lymphocytic leukemia: an European Research Initiative on CLL study

Author

Rawstron, AC, Fazi, C, Agathangelidis, A, Villamor, N, Letestu, R, Nomdedeu, J, Palacio, C, Stehlikova, O, Kreuzer, K-A, Liptrot, S, O'Brien, D, de Tute, RM, Marinov, I, Hauwel, M, Spacek, M, Dobber, J, Kater, AP, Gambell, P, Soosapilla, A, Lozanski, G, Brachtl, G, Lin, K, Boysen, J, Hanson, C, Jorgensen, JL, Stetler-Stevenson, M, Yuan, C, Broome, HE, Rassenti, L, Craig, F, Delgado, J, Moreno, C, Bosch, F, Egle, A, Doubek, M, Pospisilova, S, Mulligan, S, Westerman, D, Sanders, CM, Emerson, R, Robins, HS, Kirsch, I, Shanafelt, T, Pettitt, A, Kipps, TJ, Wierda, WG, Cymbalista, F, Hallek, M, Hillmen, P, Montserrat, E, and Ghia, P

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Hematology, Rare Diseases, Orphan Drug, Cancer, Lymphoma, Adolescent, Adult, Antigens, CD, Combined Modality Therapy, Europe, Female, Flow Cytometry, Follow-Up Studies, High-Throughput Nucleotide Sequencing, Humans, Immunophenotyping, Leukemia, Lymphocytic, Chronic, B-Cell, Male, Neoplasm Staging, Neoplasm, Residual, Prognosis, Young Adult, Clinical Sciences, Immunology, Cardiovascular medicine and haematology, Clinical sciences, Oncology and carcinogenesis
Abstract

In chronic lymphocytic leukemia (CLL) the level of minimal residual disease (MRD) after therapy is an independent predictor of outcome. Given the increasing number of new agents being explored for CLL therapy, using MRD as a surrogate could greatly reduce the time necessary to assess their efficacy. In this European Research Initiative on CLL (ERIC) project we have identified and validated a flow-cytometric approach to reliably quantitate CLL cells to the level of 0.0010% (10(-5)). The assay comprises a core panel of six markers (i.e. CD19, CD20, CD5, CD43, CD79b and CD81) with a component specification independent of instrument and reagents, which can be locally re-validated using normal peripheral blood. This method is directly comparable to previous ERIC-designed assays and also provides a backbone for investigation of new markers. A parallel analysis of high-throughput sequencing using the ClonoSEQ assay showed good concordance with flow cytometry results at the 0.010% (10(-4)) level, the MRD threshold defined in the 2008 International Workshop on CLL guidelines, but it also provides good linearity to a detection limit of 1 in a million (10(-6)). The combination of both technologies would permit a highly sensitive approach to MRD detection while providing a reproducible and broadly accessible method to quantify residual disease and optimize treatment in CLL.

Published
2016

3. EE82 A Cost-Utility Analysis of the MyPal eHealth Application, an ePro Intervention Aiming to Foster Palliative Care of Cancer Patients: Results From a Randomized Clinical Trial in 4 European Countries

Author

Naoum, P., primary, Athanasakis, K., additional, Radova, L., additional, Bonotis, P., additional, Scarfo, L., additional, Doubek, M., additional, Ghia, P., additional, Kazantzaki, E., additional, Pontikoglou, C., additional, Pospisilova, S., additional, Rosenquist, R., additional, Ekström Smedby, K., additional, and Pavi, E., additional

Published
2023
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4. FOXO1‐RICTOR AXIS INDUCES AKT PHOSPHORYLATION DURING CLL CELL ADAPTATION TO BCR INHIBITORS: IMPLICATIONS FOR COMBINATORIAL THERAPY

Author

Ondrisova, L., primary, Seda, V., additional, Hoferkova, E., additional, Chiodin, G., additional, Hlavac, K., additional, Kostalova, L., additional, Pavlasova, G. Mladonicka, additional, Filip, D., additional, Zeni, P. Faria, additional, Oppelt, J., additional, Panovska, A., additional, Plevova, K., additional, Pospisilova, S., additional, Simkovic, M., additional, Vrbacky, F., additional, Lysak, D., additional, Fernandes, S. M., additional, Davids, M. S., additional, Maiques‐Diaz, A., additional, Charalampopoulou, S., additional, Martin‐Subero, J. I., additional, Brown, J. R., additional, Doubek, M., additional, Forconi, F., additional, Mayer, J., additional, and Mraz, M., additional

Published
2023
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5. ERIC recommendations for TP53 mutation analysis in chronic lymphocytic leukemia—update on methodological approaches and results interpretation

Author

Malcikova, J., Tausch, E., Rossi, D., Sutton, L. A., Soussi, T., Zenz, T., Kater, A. P., Niemann, C. U., Gonzalez, D., Davi, F., Gonzalez Diaz, M., Moreno, C., Gaidano, G., Stamatopoulos, K., Rosenquist, R., Stilgenbauer, S., Ghia, P., Pospisilova, S., and on behalf of the European Research Initiative on Chronic Lymphocytic Leukemia (ERIC) — TP53 network

Published
2018
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7. STAT3 and TP53 mutations associate with poor prognosis in anaplastic large cell lymphoma

Author

Lobello, C, Tichy, B, Bystry, V, Radova, L, Filip, D, Mraz, M, Montes-Mojarro, I, Prokoph, N, Larose, H, Liang, H, Sharma, G, Mologni, L, Belada, D, Kamaradova, K, Fend, F, Gambacorti Passerini, C, Merkel, O, Turner, S, Janikova, A, Pospisilova, S, Lobello C., Tichy B., Bystry V., Radova L., Filip D., Mraz M., Montes-Mojarro I. -A., Prokoph N., Larose H., Liang H. -C., Sharma G. G., Mologni L., Belada D., Kamaradova K., Fend F., Gambacorti Passerini C., Merkel O., Turner S. D., Janikova A., Pospisilova S., Lobello, C, Tichy, B, Bystry, V, Radova, L, Filip, D, Mraz, M, Montes-Mojarro, I, Prokoph, N, Larose, H, Liang, H, Sharma, G, Mologni, L, Belada, D, Kamaradova, K, Fend, F, Gambacorti Passerini, C, Merkel, O, Turner, S, Janikova, A, Pospisilova, S, Lobello C., Tichy B., Bystry V., Radova L., Filip D., Mraz M., Montes-Mojarro I. -A., Prokoph N., Larose H., Liang H. -C., Sharma G. G., Mologni L., Belada D., Kamaradova K., Fend F., Gambacorti Passerini C., Merkel O., Turner S. D., Janikova A., and Pospisilova S.

Published
2021

9. P614: SUBCLONAL ARCHITECTURE OF CHROMOSOMES REVEALED BY SINGLE-CELL ANALYSIS OF GENE EXPRESSION IN A PATIENT WITH CLONAL EVOLUTION OF RELAPSING/REFRACTORY CLL

Author

Kotaskova, J., primary, Kurucova, T., additional, Reblova, K., additional, Valisova, M., additional, Zavacka, K., additional, Mareckova, A., additional, Bohunova, M., additional, Pavlova, S., additional, Malcikova, J., additional, Navrkalova, V., additional, Jarosova, M., additional, Doubek, M., additional, Plevova, K., additional, and Pospisilova, S., additional

Published
2022
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13. P1282: DISEASE-SPECIFIC U1 SPLICEOSOMAL RNA MUTATIONS IN MATURE B-CELL NEOPLASMS

Author

Nadeu, F., primary, Shuai, S., additional, Clot, G., additional, Hilton, L. K., additional, Diaz-Navarro, A., additional, Martín, S., additional, Royo, R., additional, Baumann, T., additional, Kulis, M., additional, López-Oreja, I., additional, Cossio, M., additional, Lu, J., additional, Ljungström, V., additional, Young, E., additional, Plevova, K., additional, Knisbacher, B. A., additional, Lin, Z., additional, Hahn, C. K., additional, Bousquets, P., additional, Alcoceba, M., additional, González, M., additional, Colado, E., additional, Aymerich, M., additional, Terol, M. J., additional, Rivas-Delgado, A., additional, Enjuanes, A., additional, Ruiz-Gaspà, S., additional, Chatzikonstantinou, T., additional, Hägerstrand, D., additional, Jylhä, C., additional, Skaftason, A., additional, Mansouri, L., additional, Stranska, K., additional, Doubek, M., additional, van Gastel-Mol, E. J., additional, Davis, Z., additional, Walewska, R., additional, Scarfò, L., additional, Trentin, L., additional, Visentin, A., additional, Parikh, S. A., additional, Rabe, K. G., additional, Moia, R., additional, Armand, M., additional, Rossi, D., additional, Davi, F., additional, Gaidano, G., additional, Kay, N. E., additional, Shanafelt, T., additional, Ghia, P., additional, Oscier, D., additional, Langerak, A. W., additional, Beà, S., additional, López-Guillermo, A., additional, Neuberg, D., additional, Wu, C. J., additional, Getz, G., additional, Pospisilova, S., additional, Stamatopoulos, K., additional, Rosenquist, R., additional, Huber, W., additional, Zenz, T., additional, Colomer, D., additional, Martín-Subero, J. I., additional, Delgado, J., additional, Morin, R. D., additional, Stein, L. D., additional, Puente, X. S., additional, and Campo, E., additional

Published
2022
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14. IL10RA modulates crizotinib sensitivity in NPM1-ALK+ anaplastic large cell lymphoma

Author

Prokoph, N, Probst, N, Lee, L, Monahan, J, Matthews, J, Liang, H, Bahnsen, K, Montes-Mojarro, I, Karaca-Atabay, E, Sharma, G, Malik, V, Larose, H, Forde, S, Ducray, S, Lobello, C, Wang, Q, Luan, S, Pospisilova, S, Gambacorti Passerini, C, Burke, G, Pervez, S, Attarbaschi, A, Janikova, A, Pacquement, H, Landman-Parker, J, Lambilliotte, A, Schleiermacher, G, Klapper, W, Jauch, R, Woessmann, W, Vassal, G, Kenner, L, Merkel, O, Mologni, L, Chiarle, R, Brugieres, L, Geoerger, B, Barbieri, I, Turner, S, Prokoph N., Probst N. A., Lee L. C., Monahan J. M., Matthews J. D., Liang H. -C., Bahnsen K., Montes-Mojarro I. A., Karaca-Atabay E., Sharma G. G., Malik V., Larose H., Forde S. D., Ducray S. P., Lobello C., Wang Q., Luan S. -L., Pospisilova S., Gambacorti Passerini C., Burke G. A. A., Pervez S., Attarbaschi A., Janikova A., Pacquement H., Landman-Parker J., Lambilliotte A., Schleiermacher G., Klapper W., Jauch R., Woessmann W., Vassal G., Kenner L., Merkel O., Mologni L., Chiarle R., Brugieres L., Geoerger B., Barbieri I., Turner S. D., Prokoph, N, Probst, N, Lee, L, Monahan, J, Matthews, J, Liang, H, Bahnsen, K, Montes-Mojarro, I, Karaca-Atabay, E, Sharma, G, Malik, V, Larose, H, Forde, S, Ducray, S, Lobello, C, Wang, Q, Luan, S, Pospisilova, S, Gambacorti Passerini, C, Burke, G, Pervez, S, Attarbaschi, A, Janikova, A, Pacquement, H, Landman-Parker, J, Lambilliotte, A, Schleiermacher, G, Klapper, W, Jauch, R, Woessmann, W, Vassal, G, Kenner, L, Merkel, O, Mologni, L, Chiarle, R, Brugieres, L, Geoerger, B, Barbieri, I, Turner, S, Prokoph N., Probst N. A., Lee L. C., Monahan J. M., Matthews J. D., Liang H. -C., Bahnsen K., Montes-Mojarro I. A., Karaca-Atabay E., Sharma G. G., Malik V., Larose H., Forde S. D., Ducray S. P., Lobello C., Wang Q., Luan S. -L., Pospisilova S., Gambacorti Passerini C., Burke G. A. A., Pervez S., Attarbaschi A., Janikova A., Pacquement H., Landman-Parker J., Lambilliotte A., Schleiermacher G., Klapper W., Jauch R., Woessmann W., Vassal G., Kenner L., Merkel O., Mologni L., Chiarle R., Brugieres L., Geoerger B., Barbieri I., and Turner S. D.

Abstract

Anaplastic large cell lymphoma (ALCL) is a T-cell malignancy predominantly driven by a hyperactive anaplastic lymphoma kinase (ALK) fusion protein. ALK inhibitors, such as crizotinib, provide alternatives to standard chemotherapy with reduced toxicity and side effects. Children with lymphomas driven by nucleophosmin 1 (NPM1)-ALK fusion proteins achieved an objective response rate to ALK inhibition therapy of 54% to 90% in clinical trials; however, a subset of patients progressed within the first 3 months of treatment. The mechanism for the development of ALK inhibitor resistance is unknown. Through genome-wide clustered regularly interspaced short palindromic repeats (CRISPR) activation and knockout screens in ALCL cell lines, combined with RNA sequencing data derived from ALK inhibitor-relapsed patient tumors, we show that resistance to ALK inhibition by crizotinib in ALCL can be driven by aberrant upregulation of interleukin 10 receptor subunit alpha (IL10RA). Elevated IL10RA expression rewires the STAT3 signaling pathway, bypassing otherwise critical phosphorylation by NPM1-ALK. IL-10RA expression does not correlate with response to standard chemotherapy in pediatric patients, suggesting that a combination of crizotinib and chemotherapy could prevent ALK inhibitor resistance-specific relapse.

Published
2020

16. Recurrent mutations refine prognosis in chronic lymphocytic leukemia

Author

Baliakas, P, Hadzidimitriou, A, Sutton, L-A, Rossi, D, Minga, E, Villamor, N, Larrayoz, M, Kminkova, J, Agathangelidis, A, Davis, Z, Tausch, E, Stalika, E, Kantorova, B, Mansouri, L, Scarfò, L, Cortese, D, Navrkalova, V, Rose-Zerilli, M J J, Smedby, K E, Juliusson, G, Anagnostopoulos, A, Makris, A M, Navarro, A, Delgado, J, Oscier, D, Belessi, C, Stilgenbauer, S, Ghia, P, Pospisilova, S, Gaidano, G, Campo, E, Strefford, J C, Stamatopoulos, K, and Rosenquist, R

Published
2015
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18. Memory B-cell like chronic lymphocytic leukaemia is associated with specific methylation profile of WNT5A promoter and undetectable expression of WNT5A gene

Author

Poppova, L, Pavlova, S, Gonzalez, B, Kotaskova, J, Plevova, K, Dumbovic, G, Janovska, P, Bystry, V, Panovska, A, Bezdekova, L, Maslejova, S, Brychtova, Y, Doubek, M, Krzyzankova, M, Borsky, M, Mayer, J, Bryja, V, Alonso, S, and Pospisilova, S

Subjects
m-CLL, methylation, WNT5A, i-CLL, chronic lymphocytic leukaemia
Abstract

Genome methylation profiles define naive-like (n-CLL), memory-like (m-CLL), and intermediate (i-CLL) subsets of chronic lymphocytic leukaemia (CLL). The profiles can be easily determined by the analysis of the five-CpG signature. m-CLL, i-CLL, and n-CLL with the good, intermediate, and poor prognoses, respectively, differ by the somatic hypermutation status of the immunoglobulin heavy chain variable gene (IGHV), a widely used prognostic predictor in CLL. We have previously shown that the expression of WNT5A, encoding a ROR1 ligand, distinguishes patients with the worse outcome within the prognostically favourable IGHV-mutated subgroup. To analyse the mechanisms controlling WNT5A expression, we investigated the methylation status of 54 CpG sites within the WNT5A promoter and its relation to the WNT5A gene expression. In a cohort of 59 CLL patients balanced for combinations of IGHV and WNT5A statuses, we identified three promoter CpG sites whose methylation level correlated with the WNT5A expression within the IGHV-mutated subgroup. Further, we complemented our data with the methylation status of the five-CpG signature. IGHV-mutated/WNT5A-negative and IGHV-mutated/WNT5A-positive cases overlapped with m-CLL and i-CLL methylation subgroups, respectively, while most IGHV-unmutated samples were assigned to n-CLL. Median methylation levels of all the three CpG sites in the WNT5A promoter were lowest in i-CLL. Finally, a detailed analysis of m-CLL and i-CLL showed that undetectable WNT5A expression predicts longer treatment-free survival with higher statistical significance than the classification according to the five-CpG signature. To conclude, a favourable m-CLL subgroup is associated with mutated IGHV and undetectable WNT5A expression due to its promoter methylation.

Published
2022

20. Distinct patterns of novel gene mutations in poor-prognostic stereotyped subsets of chronic lymphocytic leukemia: the case of SF3B1 and subset #2

Author

Strefford, J C, Sutton, L-A, Baliakas, P, Agathangelidis, A, Malčíková, J, Plevova, K, Scarfó, L, Davis, Z, Stalika, E, Cortese, D, Cahill, N, Pedersen, L B, di Celle, P F, Tzenou, T, Geisler, C, Panagiotidis, P, Langerak, A W, Chiorazzi, N, Pospisilova, S, Oscier, D, Davi, F, Belessi, C, Mansouri, L, Ghia, P, Stamatopoulos, K, and Rosenquist, R

Published
2013
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21. Higher-order connections between stereotyped subsets: implications for improved patient classification in CLL

Author

Agathangelidis, A. Chatzidimitriou, A. Gemenetzi, K. Giudicelli, V. Karypidou, M. Plevova, K. Davis, Z. Yan, X.-J. Jeromin, S. Schneider, C. Pedersen, L.B. Tschumper, R.C. Sutton, L.-A. Baliakas, P. Scarfò, L. van Gastel, E.J. Armand, M. Tausch, E. Biderman, B. Baer, C. Bagnara, D. Navarro, A. Langlois de Septenville, A. Guido, V. Mitterbauer-Hohendanner, G. Dimovski, A. Brieghel, C. Lawless, S. Meggendorfer, M. Brazdilova, K. Ritgen, M. Facco, M. Tresoldi, C. Visentin, A. Patriarca, A. Catherwood, M. Bonello, L. Sudarikov, A. Vanura, K. Roumelioti, M. Skuhrova Francova, H. Moysiadis, T. Veronese, S. Giannopoulos, K. Mansouri, L. Karan-Djurasevic, T. Sandaltzopoulos, R. Bödör, C. Fais, F. Kater, A. Panovska, I. Rossi, D. Alshemmari, S. Panagiotidis, P. Costeas, P. Espinet, B. Antic, D. Foroni, L. Montillo, M. Trentin, L. Stavroyianni, N. Gaidano, G. Francia di Celle, P. Niemann, C. Campo, E. Anagnostopoulos, A. Pott, C. Fischer, K. Hallek, M. Oscier, D. Stilgenbauer, S. Haferlach, C. Jelinek, D. Chiorazzi, N. Pospisilova, S. Lefranc, M.-P. Kossida, S. Langerak, A.W. Belessi, C. Davi, F. Rosenquist, R. Ghia, P. Stamatopoulos, K. ERIC, the European Research Initiative on CLL

Subjects
hemic and lymphatic diseases
Abstract

Chronic lymphocytic leukemia (CLL) is characterized by the existence of subsets of patients with (quasi)identical, stereotyped B-cell receptor (BcR) immunoglobulins. Patients in certain major stereotyped subsets often display remarkably consistent clinicobiological profiles, suggesting that the study of BcR immunoglobulin stereotypy in CLL has important implications for understanding disease pathophysiology and refining clinical decision-making. Nevertheless, several issues remain open, especially pertaining to the actual frequency of BcR immunoglobulin stereotypy and major subsets, as well as the existence of higher-order connections between individual subsets. To address these issues, we investigated clonotypic IGHV-IGHD-IGHJ gene rearrangements in a series of 29 856 patients with CLL, by far the largest series worldwide. We report that the stereotyped fraction of CLL peaks at 41% of the entire cohort and that all 19 previously identified major subsets retained their relative size and ranking, while 10 new ones emerged; overall, major stereotyped subsets had a cumulative frequency of 13.5%. Higher-level relationships were evident between subsets, particularly for major stereotyped subsets with unmutated IGHV genes (U-CLL), for which close relations with other subsets, termed “satellites,” were identified. Satellite subsets accounted for 3% of the entire cohort. These results confirm our previous notion that major subsets can be robustly identified and are consistent in relative size, hence representing distinct disease variants amenable to compartmentalized research with the potential of overcoming the pronounced heterogeneity of CLL. Furthermore, the existence of satellite subsets reveals a novel aspect of repertoire restriction with implications for refined molecular classification of CLL. Key Points: • In a series of 29 856 CLL patients, the incidence of BcR stereotypy peaked at 41%. • Higher-order relations exist between stereotyped subsets, particularly for those from U-CLL, for which satellite subsets were identified. © 2021 American Society of Hematology

Published
2021

22. Genomic arrays identify high-risk chronic lymphocytic leukemia with genomic complexity: a multi-center study

Author

Leeksma, A.C., Baliakas, P., Moysiadis, T., Puiggros, A., Plevova, K., Kevie-Kersemaekers, A.M. van der, Posthuma, H., Rodriguez-Vicente, A.E., Tran, A.N., Barbany, G., Mansouri, L., Gunnarsson, R., Parker, H., Berg, Eva van den, Bellido, M., Davis, Z., Wall, M., Scarpelli, I., Österborg, A., Hansson, L., Jarosova, M., Ghia, P., Poddighe, P., Espinet, B., Pospisilova, S., Tam, C., Ysebaert, L., Nguyen-Khac, F., Oscier, D., Haferlach, C., Schoumans, J., Stevens-Kroef, M.J.P.L., Eldering, E., Stamatopoulos, K., Rosenquist, R., Strefford, J.C., Mellink, C., Kater, A.P., Leeksma, A.C., Baliakas, P., Moysiadis, T., Puiggros, A., Plevova, K., Kevie-Kersemaekers, A.M. van der, Posthuma, H., Rodriguez-Vicente, A.E., Tran, A.N., Barbany, G., Mansouri, L., Gunnarsson, R., Parker, H., Berg, Eva van den, Bellido, M., Davis, Z., Wall, M., Scarpelli, I., Österborg, A., Hansson, L., Jarosova, M., Ghia, P., Poddighe, P., Espinet, B., Pospisilova, S., Tam, C., Ysebaert, L., Nguyen-Khac, F., Oscier, D., Haferlach, C., Schoumans, J., Stevens-Kroef, M.J.P.L., Eldering, E., Stamatopoulos, K., Rosenquist, R., Strefford, J.C., Mellink, C., and Kater, A.P.

Abstract

Contains fulltext : 229392.pdf (publisher's version ) (Open Access)

Published
2021

23. The Effect of SF3B1 Mutation on the DNA Damage Response and Nonsense-Mediated mRNA Decay in Cancer

Author

Leeksma, A.C., Derks, I.A.M., Kasem, M.H., Kilic, E., Klein, A., Jager, M.J, Loosdrecht, A.A. van de, Jansen, J.H., Navrkalova, V., Faber, L.M., Zaborsky, N., Egle, A., Zenz, T., Pospisilova, S., Abdel-Wahab, O., Kater, A.P., Eldering, E., Leeksma, A.C., Derks, I.A.M., Kasem, M.H., Kilic, E., Klein, A., Jager, M.J, Loosdrecht, A.A. van de, Jansen, J.H., Navrkalova, V., Faber, L.M., Zaborsky, N., Egle, A., Zenz, T., Pospisilova, S., Abdel-Wahab, O., Kater, A.P., and Eldering, E.

Abstract

Contains fulltext : 235808.pdf (Publisher’s version ) (Open Access)

Published
2021

24. The Effect of SF3B1 Mutation on the DNA Damage Response and Nonsense-Mediated mRNA Decay in Cancer

Author

Leeksma, A.C. (Alexander C.), Derks, I.A.M. (Ingrid), Kasem, M.H. (M. Haidar), Kiliç, E. (Emine), Klein, A. (Annelies) de, Jager, M.J. (Martine), Loosdrecht, A.A. (Arjan) van de, Jansen, J.H. (Joop H.), Navrkalova, V. (Veronika), Faber, L.M. (L.), Zaborsky, N. (Nadja), Egle, A. (Alexander), Zenz, T. (Thorsten), Pospisilova, S. (Sarka), Abdel-Wahab, O. (Omar), Kater, A.P. (Arnon), Eldering, E. (Eric), Leeksma, A.C. (Alexander C.), Derks, I.A.M. (Ingrid), Kasem, M.H. (M. Haidar), Kiliç, E. (Emine), Klein, A. (Annelies) de, Jager, M.J. (Martine), Loosdrecht, A.A. (Arjan) van de, Jansen, J.H. (Joop H.), Navrkalova, V. (Veronika), Faber, L.M. (L.), Zaborsky, N. (Nadja), Egle, A. (Alexander), Zenz, T. (Thorsten), Pospisilova, S. (Sarka), Abdel-Wahab, O. (Omar), Kater, A.P. (Arnon), and Eldering, E. (Eric)

Abstract

Recurrent mutations in splicing factor 3B subunit 1 (SF3B1) have been identified in several malignancies and are associated with an increased expression of 3’ cryptic transcripts as a result of alternative branchpoint recognition. A large fraction of cryptic transcripts associated with SF3B1 mutations is expected to be sensitive for RNA degradation via nonsense-mediated mRNA decay (NMD). Several studies indicated alterations in various signaling pathways in SF3B1-mutated cells, including an impaired DNA damage respons

Published
2021
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25. Genomic arrays identify high-risk chronic lymphocytic leukemia with genomic complexity: a multicenter study

Author

Leeksma, AC, Baliakas, P, Moysiadis, T, Puiggros, A, Plevova, K, van der Kevie-Kersemaekers, A-M, Posthuma, H, Rodriguez-Vicente, AE, Tran, AN, Barbany, G, Mansouri, L, Gunnarsson, R, Parker, H, van den Berg, E, Bellido, M, Davis, Z, Wall, M, Scarpelli, I, Osterborg, A, Hansson, L, Jarosova, M, Ghia, P, Poddighe, P, Espinet, B, Pospisilova, S, Tam, C, Ysebaert, L, Nguyen-Khac, F, Oscier, D, Haferlach, C, Schoumans, J, Stevens-Kroef, M, Eldering, E, Stamatopoulos, K, Rosenquist, R, Strefford, JC, Mellink, C, Kater, AP, Leeksma, AC, Baliakas, P, Moysiadis, T, Puiggros, A, Plevova, K, van der Kevie-Kersemaekers, A-M, Posthuma, H, Rodriguez-Vicente, AE, Tran, AN, Barbany, G, Mansouri, L, Gunnarsson, R, Parker, H, van den Berg, E, Bellido, M, Davis, Z, Wall, M, Scarpelli, I, Osterborg, A, Hansson, L, Jarosova, M, Ghia, P, Poddighe, P, Espinet, B, Pospisilova, S, Tam, C, Ysebaert, L, Nguyen-Khac, F, Oscier, D, Haferlach, C, Schoumans, J, Stevens-Kroef, M, Eldering, E, Stamatopoulos, K, Rosenquist, R, Strefford, JC, Mellink, C, and Kater, AP

Abstract

Complex karyotype (CK) identified by chromosome-banding analysis (CBA) has shown prognostic value in chronic lymphocytic leukemia (CLL). Genomic arrays offer high-resolution genome-wide detection of copy-number alterations (CNAs) and could therefore be well equipped to detect the presence of a CK. Current knowledge on genomic arrays in CLL is based on outcomes of single center studies, in which different cutoffs for CNA calling were used. To further determine the clinical utility of genomic arrays for CNA assessment in CLL diagnostics, we retrospectively analyzed 2293 arrays from 13 diagnostic laboratories according to established standards. CNAs were found outside regions captured by CLL FISH probes in 34% of patients, and several of them including gains of 8q, deletions of 9p and 18p (p<0.01) were linked to poor outcome after correction for multiple testing. Patients (n=972) could be divided in three distinct prognostic subgroups based on the number of CNAs. Only high genomic complexity (high-GC), defined as ≥5 CNAs emerged as an independent adverse prognosticator on multivariable analysis for time to first treatment (Hazard ratio: 2.15, 95% CI: 1.36-3.41; p=0.001) and overall survival (Hazard ratio: 2.54, 95% CI: 1.54-4.17; p<0.001; n=528). Lowering the size cutoff to 1 Mb in 647 patients did not significantly improve risk assessment. Genomic arrays detected more chromosomal abnormalities and performed at least as well in terms of risk stratification compared to simultaneous chromosome banding analysis as determined in 122 patients. Our findings highlight genomic array as an accurate tool for CLL risk stratification.

Published
2021

26. The Effect of SF3B1 Mutation on the DNA Damage Response and Nonsense-Mediated mRNA Decay in Cancer

Author

Leeksma, AC, Derks, IAMF, Kasem, MH, Kiliç, Emine, de Klein, Annelies, Jager, MJ, de Loosdrecht, AAV, Jansen, JH, Navrkalova, V, Faber, LM, Zaborsky, N, Egle, A, Zenz, T, Pospisilova, S, Abdel-Wahab, O, Kater, AP, Eldering, E, Leeksma, AC, Derks, IAMF, Kasem, MH, Kiliç, Emine, de Klein, Annelies, Jager, MJ, de Loosdrecht, AAV, Jansen, JH, Navrkalova, V, Faber, LM, Zaborsky, N, Egle, A, Zenz, T, Pospisilova, S, Abdel-Wahab, O, Kater, AP, and Eldering, E

Abstract

Recurrent mutations in splicing factor 3B subunit 1 (SF3B1) have been identified in several malignancies and are associated with an increased expression of 3’ cryptic transcripts as a result of alternative branchpoint recognition. A large fraction of cryptic transcripts associated with SF3B1 mutations is expected to be sensitive for RNA degradation via nonsense-mediated mRNA decay (NMD). Several studies indicated alterations in various signaling pathways in SF3B1-mutated cells, including an impaired DNA damage response (DDR) in chronic lymphocytic leukemia (CLL). In this study, we investigated isogenic cell lines and treatment naïve primary CLL samples without any TP53 and/or ATM defect, and found no significant effects of SF3B1 mutations on the ATM/p53 response, phosphorylation of H2AX and sensitivity to fludarabine. Cryptic transcripts associated with SF3B1 mutation status were observed at relatively low levels compared to the canonical transcripts and were validated as target for mRNA degradation via NMD. Expression of cryptic transcripts increased after NMD inhibition. In conclusion, our results confirm involvement of NMD in the biological effects of SF3B1 mutations. Further studies may elucidate whether SF3B1-mutant patients could benefit from NMD modulatory agents.

Published
2021

28. Antigen receptor stereotypy across B-cell lymphoproliferations: the case of IGHV4-59/IGKV3-20 receptors with rheumatoid factor activity

Author

Kostareli, E, Gounari, M, Janus, A, Murray, F, Brochet, X, Giudicelli, V, Pospisilova, S, Oscier, D, Foroni, L, di Celle, P F, Tichy, B, Pedersen, L B, Jurlander, J, Ponzoni, M, Kouvatsi, A, Anagnostopoulos, A, Thompson, K, Darzentas, N, Lefranc, M-P, Belessi, C, Rosenquist, R, Davi, F, Ghia, P, and Stamatopoulos, K

Published
2012
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29. TP53 mutation profile in chronic lymphocytic leukemia: evidence for a disease specific profile from a comprehensive analysis of 268 mutations

Author

Zenz, T, Vollmer, D, Trbusek, M, Smardova, J, Benner, A, Soussi, T, Helfrich, H, Heuberger, M, Hoth, P, Fuge, M, Denzel, T, Häbe, S, Malcikova, J, Kuglik, P, Truong, S, Patten, N, Wu, L, Oscier, D, Ibbotson, R, Gardiner, A, Tracy, I, Lin, K, Pettitt, A, Pospisilova, S, Mayer, J, Hallek, M, Döhner, H, and Stilgenbauer, S

Published
2010
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34. Cytogenetic complexity in chronic lymphocytic leukemia: Definitions, associations, and clinical impact

Author

Baliakas, P. Jeromin, S. Iskas, M. Puiggros, A. Plevova, K. Nguyen-Khac, F. Davis, Z. Matteo Rigolin, G. Visentin, A. Xochelli, A. Delgado, J. Baran-Marszak, F. Stalika, E. Abrisqueta, P. Durechova, K. Papaioannou, G. Eclache, V. DImou, M. Iliakis, T. Collado, R. Doubek, M. Calasanz, M.J. Ruiz-Xiville, N. Moreno, C. Jarosova, M. Leeksma, A.C. Panayiotidis, P. Podgornik, H. Cymbalista, F. Anagnostopoulos, A. Trentin, L. Stavroyianni, N. Davi, F. Ghia, P. Kater, A.P. Cuneo, A. Pospisilova, S. Espinet, B. Athanasiadou, A. Oscier, D. Haferlach, C. Stamatopoulos, K. on behalf of ERIC, the European Research Initiative on CLL

Abstract

Recent evidence suggests that complex karyotype (CK) defined by the presence of ≥3 chromosomal aberrations (structural and/or numerical) identified by using chromosomebanding analysis (CBA) may be relevant for treatment decision-making in chronic lymphocytic leukemia (CLL). However, many challenges toward the routine clinical application of CBA remain. In a retrospective study of 5290 patients with available CBA data, we explored both clinicobiological associations and the clinical impact of CK in CLL. We found that patients with ≥5 abnormalities, defined as high-CK, exhibit uniformly dismal clinical outcomes, independently of clinical stage, TP53 aberrations (deletion of chromosome 17p and/or TP53 mutations [TP53abs]), and the expression of somatically hypermutated (M-CLL) or unmutated immunoglobulin heavy variable genes. Thus, they contrasted with CK cases with 3 or 4 aberrations (low-CK and intermediate-CK, respectively) who followed aggressive disease courses only in the presence of TP53abs. At the other end of the spectrum, patients with CK and +12,+19 displayed an exceptionally indolent profile. Building upon CK, TP53abs, and immunoglobulin heavy variable gene somatic hypermutation status, we propose a novel hierarchical model in which patients with high-CK exhibit the worst prognosis, whereas those with mutated CLL lacking CK or TP53abs, as well as CK with +12,+19, show the longest overall survival. Thus, CK should not be axiomatically considered unfavorable in CLL, representing a heterogeneous group with variable clinical behavior. High-CK with ≥5 chromosomal aberrations emerges as prognostically adverse, independent of other biomarkers. Prospective clinical validation is warranted before ultimately incorporating high-CK in risk stratification of CLL. © 2019 by The American Society of Hematology.

Published
2019

35. DNA methylation profiles in chronic lymphocytic leukemia patients treated with chemoimmunotherapy

Author

Tsagiopoulou, M. Papakonstantinou, N. Moysiadis, T. Mansouri, L. Ljungström, V. Duran-Ferrer, M. Malousi, A. Queirós, A.C. Plevova, K. Bhoi, S. Kollia, P. Oscier, D. Anagnostopoulos, A. Trentin, L. Ritgen, M. Pospisilova, S. Stavroyianni, N. Ghia, P. Martin-Subero, J.I. Pott, C. Rosenquist, R. Stamatopoulos, K.

Subjects
hemic and lymphatic diseases
Abstract

Background: In order to gain insight into the contribution of DNA methylation to disease progression of chronic lymphocytic leukemia (CLL), using 450K Illumina arrays, we determined the DNA methylation profiles in paired pre-treatment/relapse samples from 34 CLL patients treated with chemoimmunotherapy, mostly (n = 31) with the fludarabine-cyclophosphamide-rituximab (FCR) regimen. Results: The extent of identified changes in CLL cells versus memory B cells from healthy donors was termed "epigenetic burden" (EB) whereas the number of changes between the pre-treatment versus the relapse sample was termed "relapse changes" (RC). Significant (p < 0.05) associations were identified between (i) high EB and short time-to-first-treatment (TTFT); and, (ii) few RCs and short time-to-relapse. Both the EB and the RC clustered in specific genomic regions and chromatin states, including regulatory regions containing binding sites of transcription factors implicated in B cell and CLL biology. Conclusions: Overall, we show that DNA methylation in CLL follows different dynamics in response to chemoimmunotherapy. These epigenetic alterations were linked with specific clinical and biological features. © 2019 The Author(s).

Published
2019

36. Cytogenetic complexity in chronic lymphocytic leukemia: definitions, associations, and clinical impact

Author

Baliakas, P, Jeromin, S, Iskas, M, Puiggros, A, Plevova, K, Nguyen-Khac, F, Davis, Z, Rigolin, GM, Visentin, A, Xochelli, A, Delgado, J, Baran-Marszak, F, Stalika, E, Abrisqueta, P, Durechova, K, Papaioannou, G, Eclache, V, Dimou, M, Iliakis, T, Collado, R, Doubek, M, Calasanz, MJ, Ruiz-Xiville, N, Moreno, C, Jarosova, M, Leeksma, AC, Panayiotidis, P, Podgornik, H, Cymbalista, F, Anagnostopoulos, A, Trentin, L, Stavroyianni, N, Davi, F, Ghia, P, Kater, AP, Cuneo, A, Pospisilova, S, Espinet, B, Athanasiadou, A, Oscier, D, Haferlach, C, Stamatopoulos, K, and ERIC European Res Initiative CLL

Abstract

Recent evidence suggests that complex karyotype (CK) defined by the presence of >= 3 chromosomal aberrations (structural and/or numerical) identified by using chromosome-banding analysis (CBA) may be relevant for treatment decision-making in chronic lymphocytic leukemia (CLL). However, many challenges toward the routine clinical application of CBA remain. In a retrospective study of 5290 patients with available CBA data, we explored both clinicobiological associations and the clinical impact of CK in CLL. We found that patients with >= 5 abnormalities, defined as high-CK, exhibit uniformly dismal clinical outcomes, independently of clinical stage, TP53 aberrations (deletion of chromosome 17p and/or TP53 mutations [TP53abs]), and the expression of somatically hypermutated (M-CLL) or unmutated immunoglobulin heavy variable genes. Thus, they contrasted with CK cases with 3 or 4 aberrations (low-CK and intermediate-CK, respectively) who followed aggressive disease courses only in the presence of TP53abs. At the other end of the spectrum, patients with CK and 112,119 displayed an exceptionally indolent profile. Building upon CK, TP53abs, and immunoglobulin heavy variable gene somatic hyper-mutation status, we propose a novel hierarchical model in which patients with high-CK exhibit the worst prognosis, whereas those with mutated CLL lacking CK or TP53abs, as well as CK with 112,119, show the longest overall survival. Thus, CK should not be axiomatically considered unfavorable in CLL, representing a heterogeneous group with variable clinical behavior. High-CK with >= 5 chromosomal aberrations emerges as prognostically adverse, independent of other biomarkers. Prospective clinical validation is warranted before ultimately incorporating high-CK in risk stratification of CLL.

Published
2019

37. Disease-biased and shared characteristics of the immunoglobulin gene repertoires in marginal zone B cell lymphoproliferations

Author

Xochelli, A. Bikos, V. Polychronidou, E. Galigalidou, C. Agathangelidis, A. Charlotte, F. Moschonas, P. Davis, Z. Colombo, M. Roumelioti, M. Sutton, L.-A. Groenen, P. van den Brand, M. Boudjoghra, M. Algara, P. Traverse-Glehen, A. Ferrer, A. Stalika, E. Karypidou, M. Kanellis, G. Kalpadakis, C. Mollejo, M. Pangalis, G. Vlamos, P. Amini, R.-M. Pospisilova, S. Gonzalez, D. Ponzoni, M. Anagnostopoulos, A. Giudicelli, V. Lefranc, M.-P. Espinet, B. Panagiotidis, P. Piris, M.A. Du, M.-Q. Rosenquist, R. Papadaki, T. Belessi, C. Ferrarini, M. Oscier, D. Tzovaras, D. Ghia, P. Davi, F. Hadzidimitriou, A. Stamatopoulos, K.

Abstract

The B cell receptor immunoglobulin (Ig) gene repertoires of marginal zone (MZ) lymphoproliferations were analyzed in order to obtain insight into their ontogenetic relationships. Our cohort included cases with MZ lymphomas (n = 488), i.e. splenic (SMZL), nodal (NMZL) and extranodal (ENMZL), as well as provisional entities (n = 76), according to the WHO classification. The most striking Ig gene repertoire skewing was observed in SMZL. However, restrictions were also identified in all other MZ lymphomas studied, particularly ENMZL, with significantly different Ig gene distributions depending on the primary site of involvement. Cross-entity comparisons of the MZ Ig sequence dataset with a large dataset of Ig sequences (MZ-related or not; n = 65 837) revealed four major clusters of cases sharing homologous (‘public’) heavy variable complementarity-determining region 3. These clusters included rearrangements from SMZL, ENMZL (gastric, salivary gland, ocular adnexa), chronic lymphocytic leukemia, but also rheumatoid factors and non-malignant splenic MZ cells. In conclusion, different MZ lymphomas display biased immunogenetic signatures indicating distinct antigen exposure histories. The existence of rare public stereotypes raises the intriguing possibility that common, pathogen-triggered, immune-mediated mechanisms may result in diverse B lymphoproliferations due to targeting versatile progenitor B cells and/or operating in particular microenvironments. Copyright © 2018 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd. Copyright © 2018 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published
2019

39. Disease-biased and shared characteristics of the immunoglobulin gene repertoires in marginal zone B cell lymphoproliferations

Author

Xochelli, A., Bikos, V., Polychronidou, E., Galigalidou, C., Agathangelidis, A., Charlotte, F., Moschonas, P., Davis, Z., Colombo, M., Roumelioti, M., Sutton, L.A., Groenen, P.J., Brand, M. van den, Boudjoghra, M., Algara, P., Traverse-Glehen, A., Ferrer, A., Stalika, E., Karypidou, M., Kanellis, G., Kalpadakis, C., Mollejo, M., Pangalis, G., Vlamos, P., Amini, R.M., Pospisilova, S., Gonzalez, D., Ponzoni, M., Anagnostopoulos, A., Giudicelli, V., Lefranc, M.P., Espinet, B., Panagiotidis, P., Piris, M.A., Du, M.Q., Rosenquist, R., Papadaki, T., Belessi, C., Ferrarini, M., Oscier, D., Tzovaras, D., Ghia, P., Davi, F., Hadzidimitriou, A., Stamatopoulos, K., Xochelli, A., Bikos, V., Polychronidou, E., Galigalidou, C., Agathangelidis, A., Charlotte, F., Moschonas, P., Davis, Z., Colombo, M., Roumelioti, M., Sutton, L.A., Groenen, P.J., Brand, M. van den, Boudjoghra, M., Algara, P., Traverse-Glehen, A., Ferrer, A., Stalika, E., Karypidou, M., Kanellis, G., Kalpadakis, C., Mollejo, M., Pangalis, G., Vlamos, P., Amini, R.M., Pospisilova, S., Gonzalez, D., Ponzoni, M., Anagnostopoulos, A., Giudicelli, V., Lefranc, M.P., Espinet, B., Panagiotidis, P., Piris, M.A., Du, M.Q., Rosenquist, R., Papadaki, T., Belessi, C., Ferrarini, M., Oscier, D., Tzovaras, D., Ghia, P., Davi, F., Hadzidimitriou, A., and Stamatopoulos, K.

Abstract

Contains fulltext : 203155.pdf (Publisher’s version ) (Closed access), The B cell receptor immunoglobulin (Ig) gene repertoires of marginal zone (MZ) lymphoproliferations were analyzed in order to obtain insight into their ontogenetic relationships. Our cohort included cases with MZ lymphomas (n = 488), i.e. splenic (SMZL), nodal (NMZL) and extranodal (ENMZL), as well as provisional entities (n = 76), according to the WHO classification. The most striking Ig gene repertoire skewing was observed in SMZL. However, restrictions were also identified in all other MZ lymphomas studied, particularly ENMZL, with significantly different Ig gene distributions depending on the primary site of involvement. Cross-entity comparisons of the MZ Ig sequence dataset with a large dataset of Ig sequences (MZ-related or not; n = 65 837) revealed four major clusters of cases sharing homologous ('public') heavy variable complementarity-determining region 3. These clusters included rearrangements from SMZL, ENMZL (gastric, salivary gland, ocular adnexa), chronic lymphocytic leukemia, but also rheumatoid factors and non-malignant splenic MZ cells. In conclusion, different MZ lymphomas display biased immunogenetic signatures indicating distinct antigen exposure histories. The existence of rare public stereotypes raises the intriguing possibility that common, pathogen-triggered, immune-mediated mechanisms may result in diverse B lymphoproliferations due to targeting versatile progenitor B cells and/or operating in particular microenvironments. Copyright (c) 2018 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published
2019

40. The use of Human Inflammatory Response and Autoimmunity RT2 lncRNA PCR Array for plasma examination in breast cancer patients prior to therapy

Author

Sterbova M, Iveta Zednikova, Santorova-Pospisilova S, Petra Tesarova, Marie Korabecna, and Eva Pazourkova

Subjects
Regulation of gene expression, Cancer Research, business.industry, Inflammatory response, RNA, Cancer, HOTAIR, Breast Neoplasms, medicine.disease_cause, medicine.disease, Polymerase Chain Reaction, Autoimmunity, Gene Expression Regulation, Neoplastic, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Oncology, 030220 oncology & carcinogenesis, Cancer research, medicine, Humans, RNA, Long Noncoding, GAS5, business
Abstract

Long non-coding RNAs (lncRNAs) are defined as RNA molecules longer than 200 nucleotides with poor protein-coding capacity and key functions in regulation of gene expression. Dysregulations of lncRNAs (e.g. HOTAIR and MALAT I) were detected in plasma of breast cancer (BC) patients. Plasma samples are examined as liquid biopsies for purposes of non-invasive diagnostics therefore the research of plasma lncRNAs as potential plasma biomarkers became highly topical. 84 lncRNAs were profiled in 18 plasma samples - 9 BC patients and 9 age-matched healthy - using Human Inflammatory Response & Autoimmunity RT2 lncRNA PCR Array. Total RNA from plasma samples was isolated using miRNeasy Serum/Plasma Kit. Although a pre-amplification recommended for quantification from small starting RNA amounts was used, only 3 lncRNAs (A2ML1-AS1, GAS5 and SNHG5) were detected in all plasma samples. A total of 72 lncRNAs (e.g. HOTAIR or MALAT I) were detected only in some samples and 9 lncRNAs were not detected in any samples. No significant differences were observed in levels of plasma lncRNAs between the BC patients and healthy controls despite the fact that our panel contained also the lncRNAs whose levels were previously reported as significantly different in plasma or cancer tissues (e.g. GAS5, HOTAIR, MALAT I) in BC patients. Detection of lncRNAs in plasma is due to their low concentrations quite difficult as compared with tissues. Our findings suggest that analysis of plasma lncRNAs using this technology is not suitable for use as non-invasive diagnostic tool in BC patients.

Published
2018

41. Reproducible diagnosis of chronic lymphocytic leukemia by flow cytometry:An European Research Initiative on CLL (ERIC) & European Society for Clinical Cell Analysis (ESCCA) Harmonisation project

Author

Rawstron, AC, Kreuzer, K-A, Soosapilla, A, Spacek, M, Stehlikova, O, Gambell, P, McIver-Brown, N, Villamor, N, Psarra, K, Arroz, M, Milani, R, de la Serna, J, Cedena, MT, Jaksic, O, Nomdedeu, J, Moreno, C, Rigolin, GM, Cuneo, A, Johansen, P, Johnsen, HE, Rosenquist, R, Niemann, CU, Kern, W, Westerman, D, Trneny, M, Mulligan, S, Doubek, M, Pospisilova, S, Hillmen, P, Oscier, D, Hallek, M, Ghia, P, Montserrat, E, Rawstron, Andy C., Kreuzer, Karl-Anton, Soosapilla, Asha, Spacek, Martin, Stehlikova, Olga, Gambell, Peter, McIver-Brown, Neil, Villamor, Neu, Psarra, Katherina, Arroz, Maria, Milani, Raffaella, de la Serna, Javier, Cedena, M. Teresa, Jaksic, Ozren, Nomdedeu, Josep, Moreno, Carol, Rigolin, Gian Matteo, Cuneo, Antonio, Johansen, Preben, Johnsen, Hans E., Rosenquist, Richard, Niemann, Carsten Utoft, Kern, Wolfgang, Westerman, David, Trneny, Marek, Mulligan, Stephen, Doubek, Michael, Pospisilova, Sarka, Hillmen, Peter, Oscier, David, Hallek, Michael, Ghia, Paolo, and Montserrat, Emili

Subjects
chronic lymphocytic leukemia, diagnosis, flow cytometry, 2734, Histology, Cell Biology, Clinical Laboratory Medicine, Reproducibility of Results, Pilot Projects, Original Articles, Leukemia, Lymphocytic, Chronic, B-Cell, NO, Immunophenotyping, diagnosi, Klinisk laboratoriemedicin, immune system diseases, hemic and lymphatic diseases, Biomarkers, Tumor, Humans, Original Article, Retrospective Studies
Abstract

The diagnostic criteria for CLL rely on morphology and immunophenotype. Current approaches have limitations affecting reproducibility and there is no consensus on the role of new markers. The aim of this project was to identify reproducible criteria and consensus on markers recommended for the diagnosis of CLL. ERIC/ESCCA members classified 14 of 35 potential markers as “required” or “recommended” for CLL diagnosis, consensus being defined as >75% and >50% agreement, respectively. An approach to validate “required” markers using normal peripheral blood was developed. Responses were received from 150 participants with a diagnostic workload >20 CLL cases per week in 23/150 (15%), 5–20 in 82/150 (55%), and 97% concordance with current approaches. A pilot study to validate staining quality was completed in 11 centers. Markers considered as “required” for the diagnosis of CLL by the participants in this study (CD19, CD5, CD20, CD23, Kappa, and Lambda) are consistent with current diagnostic criteria and practice. Importantly, a reproducible approach to validate and apply these markers in individual laboratories has been identified. Finally, a consensus “recommended” panel of markers to refine diagnosis in borderline cases (CD43, CD79b, CD81, CD200, CD10, and ROR1) has been defined and will be prospectively evaluated. © 2017 International Clinical Cytometry Society.

Published
2018

42. No improvement in long-term survival over time for chronic lymphocytic leukemia patients in stereotyped subsets #1 and #2 treated with chemo(Immuno)therapy

Author

Baliakas, P. Mattsson, M. Hadzidimitriou, A. Minga, E. Agathangelidis, A. Sutton, L.-A. Scarfo, L. Davis, Z. Yan, X.-J. Plevova, K. Sandberg, Y. Vojdeman, F.J. Tzenou, T. Chu, C.C. Veronese, S. Mansouri, L. Smedby, K.E. Giudicelli, V. Nguyen-Khac, F. Panagiotidis, P. Juliusson, G. Anagnostopoulos, A. Lefranc, M.-P. Trentin, L. Catherwood, M. Montillo, M. Niemann, C.U. Langerak, A.W. Pospisilova, S. Stavroyianni, N. Chiorazzi, N. Oscier, D. Jelinek, D.F. Shanafelt, T. Darzentas, N. Belessi, C. Davi, F. Ghia, P. Rosenquist, R. Stamatopoulos, K.

Published
2018

43. PS1137 COMPLEX STRUCTURAL VARIANTS LEAD TO GENE INACTIVATION RATHER THAN EXPRESSION OF DE NOVO FUSION GENES IN CHRONIC LYMPHOCYTIC LEUKEMIA

Author

Plevova, K., primary, Hynst, J., additional, Zavacka, K., additional, Jarosova, M., additional, Rausch, T., additional, Ondrouskova, E., additional, Radova, L., additional, Pavlova, S., additional, Malcikova, J., additional, Panovska, A., additional, Brychtova, Y., additional, Doubek, M., additional, Benes, V., additional, and Pospisilova, S., additional

Published
2019
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44. PS1133 GENOMIC ARRAYS IDENTIFY HIGH-RISK CHRONIC LYMPHOCYTIC LEUKEMIA WITH GENOMIC COMPLEXITY: A MULTI-CENTER STUDY

Author

Leeksma, A., primary, Baliakas, P., additional, Moysiadis, T., additional, Mellink, C., additional, Puiggros, A., additional, Plevova, K., additional, van der Kevie, A.-M., additional, Tran, A.N., additional, Gunnarsson, R., additional, Parker, H., additional, van den Berg, E., additional, Ghia, P., additional, Espinet, B., additional, Pospisilova, S., additional, Tam, C., additional, Ysebaert, L., additional, Jarosova, M., additional, Nguyen-Khac, F., additional, Oscier, D., additional, Haferlach, C., additional, Schoumans, J., additional, Stevens-Kroef, M., additional, Eldering, E., additional, Stamatopoulos, K., additional, Rosenquist, R., additional, Strefford, J., additional, and Kater, A., additional

Published
2019
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45. INTERNATIONAL PROGNOSTIC SCORE FOR EARLY STAGE CHRONIC LYMPHOCYTIC LEUKEMIA (IPS-A)

Author

Condoluci, A., primary, Terzi di Bergamo, L., additional, Langerbeins, P., additional, Hoechstetter, M., additional, Herling, C., additional, De Paoli, L., additional, Delgado, J., additional, Gentile, M., additional, Doubek, M., additional, Mauro, F.R., additional, Chiodin, G., additional, Mattsson, M., additional, Bahlo, J., additional, Cutrona, G., additional, Kotaskova, J., additional, Deambrogi, C., additional, Moia, R., additional, Gerber, B., additional, Zucca, E., additional, Ghielmini, M., additional, Cavalli, F., additional, Stüssi, G., additional, Neri, A., additional, Ferrarini, M., additional, Rosenquist, R., additional, Forconi, F., additional, Foà, R., additional, Pospisilova, S., additional, Morabito, F., additional, Wierda, W.G., additional, Montserrat, E., additional, Gaidano, G., additional, Hallek, M., additional, and Rossi, D., additional

Published
2019
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47. No improvement in long-term survival over time for chronic lymphocytic leukemia patients in stereotyped subsets #1 and #2 treated with chemo(Immuno)therapy

Author

Baliakas, P. (P.), Mattsson, M. (Mattias), Hadzidimitriou, A. (A.), Minga, E. (Evangelia), Agathangelidis, A. (Andreas), Sutton, L.-A. (L.), Scarfó, L. (L.), Davis, Z. (Zadie), Yan, X.-J. (Xiao-Jie), Plevova, K. (K.), Sandberg, Y. (Yorick), Vojdeman, F.J. (Fie Juhl), Tzenou, T. (T.), Chu, C.C. (Charles C.), Veronese, S. (Silvio), Mansouri, A. (Ahmed), Smedby, O., Giudicelli, V. (Veronique), Nguyen-Khac, F. (Florence), Panagiotidis, P. (P.), Juliusson, G. (Gunnar), Anagnostopoulos, C. (Constantinos), Lefranc, M.-P. (Marie-Paule), Trentin, L. (Livio), Catherwood, M. (M.), Montillo, M. (Marco), Niemann, C.U. (Carsten U.), Langerak, A.W. (Anton), Pospisilova, S. (Sarka), Stavroyianni, N. (Niki), Chiorazzi, N. (Nicholas), Oscier, D.G. (David Graham), Jelinek, D.F. (Diane F.), Shanafelt, T. (Tait), Darzentas, N. (Nikos), Belessi, C. (C.), Davi, F. (Frédéric), Ghia, P. (Paolo), Rosenquist, R. (R.), Stamatopoulos, K. (Kostas), Baliakas, P. (P.), Mattsson, M. (Mattias), Hadzidimitriou, A. (A.), Minga, E. (Evangelia), Agathangelidis, A. (Andreas), Sutton, L.-A. (L.), Scarfó, L. (L.), Davis, Z. (Zadie), Yan, X.-J. (Xiao-Jie), Plevova, K. (K.), Sandberg, Y. (Yorick), Vojdeman, F.J. (Fie Juhl), Tzenou, T. (T.), Chu, C.C. (Charles C.), Veronese, S. (Silvio), Mansouri, A. (Ahmed), Smedby, O., Giudicelli, V. (Veronique), Nguyen-Khac, F. (Florence), Panagiotidis, P. (P.), Juliusson, G. (Gunnar), Anagnostopoulos, C. (Constantinos), Lefranc, M.-P. (Marie-Paule), Trentin, L. (Livio), Catherwood, M. (M.), Montillo, M. (Marco), Niemann, C.U. (Carsten U.), Langerak, A.W. (Anton), Pospisilova, S. (Sarka), Stavroyianni, N. (Niki), Chiorazzi, N. (Nicholas), Oscier, D.G. (David Graham), Jelinek, D.F. (Diane F.), Shanafelt, T. (Tait), Darzentas, N. (Nikos), Belessi, C. (C.), Davi, F. (Frédéric), Ghia, P. (Paolo), Rosenquist, R. (R.), and Stamatopoulos, K. (Kostas)

Published
2018
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48. Reproducible diagnosis of chronic lymphocytic leukemia by flow cytometry: An European Research Initiative on CLL (ERIC) & European Society for Clinical Cell Analysis (ESCCA) Harmonisation project

Author

Rawstron, AC, Kreuzer, K-A, Soosapilla, A, Spacek, M, Stehlikova, O, Gambell, P, McIver-Brown, N, Villamor, N, Psarra, K, Arroz, M, Milani, R, de la Serna, J, Teresa Cedena, M, Jaksic, O, Nomdedeu, J, Moreno, C, Rigolin, GM, Cuneo, A, Johansen, P, Johnsen, HE, Rosenquist, R, Niemann, CU, Kern, W, Westerman, D, Trneny, M, Mulligan, S, Doubek, M, Pospisilova, S, Hillmen, P, Oscier, D, Hallek, M, Ghia, P, Montserrat, E, Rawstron, AC, Kreuzer, K-A, Soosapilla, A, Spacek, M, Stehlikova, O, Gambell, P, McIver-Brown, N, Villamor, N, Psarra, K, Arroz, M, Milani, R, de la Serna, J, Teresa Cedena, M, Jaksic, O, Nomdedeu, J, Moreno, C, Rigolin, GM, Cuneo, A, Johansen, P, Johnsen, HE, Rosenquist, R, Niemann, CU, Kern, W, Westerman, D, Trneny, M, Mulligan, S, Doubek, M, Pospisilova, S, Hillmen, P, Oscier, D, Hallek, M, Ghia, P, and Montserrat, E

Published
2018

49. ERIC recommendations for TP53 mutation analysis in chronic lymphocytic leukemia-update on methodological approaches and results interpretation

Author

Malcikova, J, Tausch, E, Rossi, D, Sutton, L A, Soussi, T; https://orcid.org/0000-0001-8184-3293, Zenz, T, Kater, A P, Niemann, C U, Gonzalez, D, Davi, F, Gonzalez Diaz, M, Moreno, C, Gaidano, G, Stamatopoulos, K, Rosenquist, R, Stilgenbauer, S, Ghia, P; https://orcid.org/0000-0003-3750-7342, Pospisilova, S, Malcikova, J, Tausch, E, Rossi, D, Sutton, L A, Soussi, T; https://orcid.org/0000-0001-8184-3293, Zenz, T, Kater, A P, Niemann, C U, Gonzalez, D, Davi, F, Gonzalez Diaz, M, Moreno, C, Gaidano, G, Stamatopoulos, K, Rosenquist, R, Stilgenbauer, S, Ghia, P; https://orcid.org/0000-0003-3750-7342, and Pospisilova, S

Abstract

In chronic lymphocytic leukemia (CLL), TP53 gene defects, due to deletion of the 17p13 locus and/or mutation(s) within the TP53 gene, are associated with resistance to chemoimmunotherapy and a particularly dismal clinical outcome. On these grounds, analysis of TP53 aberrations has been incorporated into routine clinical diagnostics to improve patient stratification and optimize therapeutic decisions. The predictive implications of TP53 aberrations have increasing significance in the era of novel targeted therapies, i.e., inhibitors of B-cell receptor (BcR) signaling and anti-apoptotic BCL2 family members, owing to their efficacy in patients with TP53 defects. In this report, the TP53 Network of the European Research Initiative on Chronic Lymphocytic Leukemia (ERIC) presents updated recommendations on the methodological approaches for TP53 mutation analysis. Moreover, it provides guidance to ensure that the analysis is performed in a timely manner for all patients requiring treatment and that the data is interpreted and reported in a consistent, standardized, and accurate way. Since next-generation sequencing technologies are gaining prominence within diagnostic laboratories, this report also offers advice and recommendations for the interpretation of TP53 mutation data generated by this methodology.

Published
2018

50. No improvement in long-term survival over time for chronic lymphocytic leukemia patients in stereotyped subsets #1 and #2 treated with chemo(immuno)therapy

Author

Baliakas, P, Mattsson, M, Hadzidimitriou, A, Minga, E, Agathangelidis, A, Sutton, LA, Scarfo, L, Davis, Z, Yan, XJ, Plevova, K, Sandberg, Yorick, Vojdeman, FJ, Tzenou, T, Chu, CC, Veronese, S, Mansouri, L, Smedby, KE, Giudicelli, V, Nguyen-Khac, F, Panagiotidis, P, Juliusson, G, Anagnostopoulos, A, Lefranc, MP, Trentin, L, Catherwood, M, Montillo, M, Niemann, CU, Langerak, Ton, Pospisilova, S, Stavroyianni, N, Chiorazzi, N, Oscier, D, Jelinek, DF, Shanafelt, T, Darzentas, N, Belessi, C, Davi, F, Ghia, P, Rosenquist, R, Stamatopoulos, K, Baliakas, P, Mattsson, M, Hadzidimitriou, A, Minga, E, Agathangelidis, A, Sutton, LA, Scarfo, L, Davis, Z, Yan, XJ, Plevova, K, Sandberg, Yorick, Vojdeman, FJ, Tzenou, T, Chu, CC, Veronese, S, Mansouri, L, Smedby, KE, Giudicelli, V, Nguyen-Khac, F, Panagiotidis, P, Juliusson, G, Anagnostopoulos, A, Lefranc, MP, Trentin, L, Catherwood, M, Montillo, M, Niemann, CU, Langerak, Ton, Pospisilova, S, Stavroyianni, N, Chiorazzi, N, Oscier, D, Jelinek, DF, Shanafelt, T, Darzentas, N, Belessi, C, Davi, F, Ghia, P, Rosenquist, R, and Stamatopoulos, K

Published
2018

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