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101. Update on treatment recommendations from the fourth international workshop on Waldenström's macroglobulinemia

Author

Dimopoulos, M.A. Gertz, M.A. Kastritis, E. Garcia-Sanz, R. Kimby, E.K. LeBlond, V. Fermand, J.-P. Merlini, G. Morel, P. Morra, E. Ocio, E.M. Owen, R. Ghobrial, I.M. Seymour, J. Kyle, R.A. Treon, S.P.

Subjects
hemic and lymphatic diseases
Abstract

Waldenström macroglobulinemia (WM) is a distinct B-cell lymphoproliferative disorder characterized by lymphoplasmacytic bone marrow infiltration along with an immunoglobulin M (lgM) monoclonal gammopathy. Patients with disease-related cytopenias, bulky adenopathy or organomegaly, symptomatic hyperviscosity, severe neuropathy, amyloidosis, cryoglobulinemia, cold agglutinin disease, or evidence of disease transformation should be considered for immediate therapy. Initiation of therapy should not be based on serum lgM levels alone, and asymptomatic patients should be observed. Individual patient considerations should be considered when deciding on a first-line agent including the presence of cytopenias, need for rapid disease control, age, and candidacy for autologous transplantation. Therapeutic outcomes should be evaluated using updated criteria. As part of the Fourth International Workshop on Waldenström's Macroglobulinemia, a consensus panel updated its recommendations on both first-line and salvage therapy in view of recently published and ongoing clinical trials. The panel considered encouraging results from recent studies of first-line combinations such as rituximab with nucleoside analogs with or without alkylating agents or with cyclophosphamide-based therapies (eg, cyclophosphamide, doxorubicin, vincristine, and prednisone or cyclophosphamide and dexamethasone) or the combination of rituximab with thalidomide. Such therapeutic approaches are likely to yield responses at least as good as, if not better than, monotherapy with any of the alkylating agents, nucleoside analogs, or rituximab. In the salvage setting, reuse of a first-line regimen or use of a different regimen should be considered along with bortezomib, alemtuzumab, autologous transplantation, and, in selected circumstances, allogeneic transplantation. Finally, the panel reaffirmed its encouragement of the active enrollment of patients with WM onto innovative clinical trials whenever possible. © 2008 by American Society of Clinical Oncology.

Published
2009

103. Update on treatment recommendations from the third international workshop on Waldenstrom's macroglobulinemia

Author

Treon, SP Gertz, MA Dimopoulos, M Anagnostopoulos, A Blade, J Garcia-Sanz, R Johnson, S Kimby, E LeBlond, V Fermand, JP others

Subjects
Health Sciences, Επιστήμες Υγείας
Abstract

Waldenstrom macroglobulinemia (WM) is a B-cell disorder characterized by the infiltration of lymphoplasmacytic cells into bone marrow and the presence of an IgM monoclonal gammopathy. As part of the Third International Workshop on WM, held October 7 to 10, 2004 in Paris, France, a consensus panel charged with providing treatment recommendations for WM updated its recommendations on both frontline and salvage therapies. The panel considered encouraging results from recent studies that addressed the use of extended-dose rituximab as well as other treatment options: therapy with either nucleoside analogs and alkylator agents, rituximab in combination with nucleoside analogs, nucleoside analogs plus alkylator agents, or combination chemotherapies, such as CHOP (cyclophosphamide, doxorubicin, vincristine, prednisone) or cyclophosphamide and dexamethasone. The panel determined that these were reasonable treatment options for WM patients and such therapeutic approaches were likely to yield results that are at least as good as if not better than the currently recommended use of single-agent alkylator, nucleoside analog, or standard-dose rituximab therapy. Such approaches were deemed to be reasonable treatment for WM patients in both the upfront and salvage settings, though randomized studies addressing the efficacy and toxicity of such novel approaches over previously established standard of care options are needed.

Published
2005

106. The prognostic value of multiparameter flow cytometry minimal residual disease assessment in relapsed multiple myeloma

Author

Paiva, B., primary, Chandia, M., additional, Puig, N., additional, Vidriales, M.-B., additional, Perez, J. J., additional, Lopez-Corral, L., additional, Ocio, E. M., additional, Garcia-Sanz, R., additional, Gutierrez, N. C., additional, Jimenez-Ubieto, A., additional, Lahuerta, J.-J., additional, Mateos, M.-V., additional, and San Miguel, J. F., additional

Published
2014
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109. Transcriptome analysis reveals molecular profiles associated with evolving steps of monoclonal gammopathies

Author

Lopez-Corral, L., primary, Corchete, L. A., additional, Sarasquete, M. E., additional, Mateos, M. V., additional, Garcia-Sanz, R., additional, Ferminan, E., additional, Lahuerta, J.-J., additional, Blade, J., additional, Oriol, A., additional, Teruel, A. I., additional, Martino, M. L., additional, Hernandez, J., additional, Hernandez-Rivas, J. M., additional, Burguillo, F. J., additional, San Miguel, J. F., additional, and Gutierrez, N. C., additional

Published
2014
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110. Bortezomib cumulative dose, efficacy, and tolerability with three different bortezomib-melphalan-prednisone regimens in previously untreated myeloma patients ineligible for high-dose therapy

Author

Mateos, M.-V., primary, Bringhen, S., additional, Richardson, P. G., additional, Lahuerta, J. J., additional, Larocca, A., additional, Oriol, A., additional, Boccadoro, M., additional, Garcia-Sanz, R., additional, Di Raimondo, F., additional, Esseltine, D.-L., additional, van de Velde, H., additional, Desai, A., additional, Londhe, A., additional, San Miguel, J. F., additional, and Palumbo, A., additional

Published
2014
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111. Design and standardization of PCR primers and protocols for detection of clonal immunoglobulin and T-cell receptor gene recombinations in suspect lymphoproliferations: Report of the BIOMED-2 Concerted Action BMH4-CT98-3936: Report of the BIOMED-2 Concerted Action BMH4-CT98-3936

Author

van Dongen, J.J.M., Langerak, A.W., Bruggemann, M., Evans, P.A.S., Hummel, M., Lavender, F.L., Delabesse, E., Davi, F., Schuuring, E., Garcia-Sanz, R., Van Krieken, J.H.J.M., Droese, J., Gonzalez, D., Bastard, C., White, H.E., Spaargaren, M., Gonzalez, M., Parreira, A., Smith, J.L., Morgan, G.J., Kneba, M., Macintyre, E.A., Damage and Repair in Cancer Development and Cancer Treatment (DARE), and Targeted Gynaecologic Oncology (TARGON)

Subjects
BCL2, POLYMERASE-CHAIN-REACTION, V-BETA REPERTOIRE, MINIMAL RESIDUAL DISEASE, clonality, FLOW-CYTOMETRIC ANALYSIS, TCRB, TCRD, TCRG, heteroduplex, PARAFFIN-EMBEDDED TISSUES, BCL1, ACUTE LYMPHOBLASTIC-LEUKEMIA, IGK, IGL, lymphoproliferative disorders, BIOMED-2, IGH, TIME QUANTITATIVE PCR, multiplex PCR, IN-SITU HYBRIDIZATION, t(14, 18), SOUTHERN BLOT ANALYSIS, PCR, immunoglobulin genes, t(11, 14), T-cell receptor genes, GeneScanning, HUMAN BONE-MARROW
Abstract

In a European BIOMED-2 collaborative study, multiplex PCR assays have successfully been developed and standardized for the detection of clonally rearranged immunoglobulin (Ig) and T-cell receptor (TCR) genes and the chromosome aberrations t(11; 14) and t(14; 18). This has resulted in 107 different primers in only 18 multiplex PCR tubes: three VH-JH, two DH-JH, two Ig kappa (IGK), one Ig lambda (IGL), three TCR beta (TCRB), two TCR gamma (TCRG), one TCR delta (TCRD), three BCL1-Ig heavy chain (IGH), and one BCL2-IGH. The PCR products of Ig/TCR genes can be analyzed for clonality assessment by heteroduplex analysis or GeneScanning. The detection rate of clonal rearrangements using the BIOMED-2 primer sets is unprecedentedly high. This is mainly based on the complementarity of the various BIOMED-2 tubes. In particular, combined application of IGH (VH-JH and DH-JH) and IGK tubes can detect virtually all clonal B-cell proliferations, even in B-cell malignancies with high levels of somatic mutations. The contribution of IGL gene rearrangements seems limited. Combined usage of the TCRB and TCRG tubes detects virtually all clonal T-cell populations, whereas the TCRD tube has added value in case of TCRgammadelta(+) T-cell proliferations. The BIOMED-2 multiplex tubes can now be used for diagnostic clonality studies as well as for the identification of PCR targets suitable for the detection of minimal residual disease

Published
2003

112. Primary therapy of Waldenström macroglobulinemia (WM) with weekly bortezomib, low-dose dexamethasone, and rituximab (BDR): Long-term results of a phase 2 study of the European Myeloma Network (EMN)

Author

Dimopoulos, M.A. (Meletios), Garcia-Sanz, R. (Ramon), Gavriatopoulou, M. (Maria), Morel, P., Kyrtsonis, M.-C. (Marie-Christine), Michalis, L.K. (Lampros), Kartasis, Z. (Zafiris), Leleu, X., Palladini, G. (Giovanni), Tedeschi, A. (Alessandra), Gika, D. (Dimitra), Merlini, G. (Giampaolo), Kastritis, E. (Efstathios), Sonneveld, P. (Pieter), Dimopoulos, M.A. (Meletios), Garcia-Sanz, R. (Ramon), Gavriatopoulou, M. (Maria), Morel, P., Kyrtsonis, M.-C. (Marie-Christine), Michalis, L.K. (Lampros), Kartasis, Z. (Zafiris), Leleu, X., Palladini, G. (Giovanni), Tedeschi, A. (Alessandra), Gika, D. (Dimitra), Merlini, G. (Giampaolo), Kastritis, E. (Efstathios), and Sonneveld, P. (Pieter)

Abstract

In this phase 2 multicenter trial, we evaluated the activity of bortezomib, dexamethasone, and rituximab (BDR) combination in previously untreated symptomatic patients with Waldenström macroglobulinemia (WM). To prevent immunoglobulin M (IgM) "flare," single agent bortezomib (1.3 mg/m 2 IV days 1, 4, 8, and 11;21-day cycle), was followed by weekly IV bortezomib (1.6 mg/m2 days 1, 8, 15, and 22) every 35 days for 4 additional cycles, followed by IV dexamethasone (40 mg) and IV rituximab (375 mg/m2) in cycles 2 and 5. Fifty-nine patients were treated; 45.5% and 40% were high and intermediate risk per the International Prognostic Scoring System for WM. On intent to treat, 85% responded (3% complete response, 7% very good partial response, 58% partial response [PR]).In 11% of patients, an increase of IgM ≥25% was observed after rituximab; no patient required plasmapheresis. After a minimum follow-up of 32 months, median progression-free survival was42months, 3-year durationof response for patients with≥PR was 70%, and 3-year survival was 81%. Peripheral neuropathy occurred in 46% (grade ≥3 in 7%); only 8% discontinued bortezomib due to neuropathy. BDR is rapidly acting, well tolerated, and nonmyelotoxic, inducing durable responses in previously untreated WM.

Published
2013
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113. EuroClonality/BIOMED-2 guidelines for interpretation and reporting of Ig/TCR clonality testing in suspected lymphoproliferations

Author

Langerak, A. W., Groenen, P. J. T. A., Brueggemann, M., Beldjord, K., Bellan, C., Bonello, L., Boone, E., Carter, G. I., Catherwood, M., Davi, F., Delfau-Larue, M-H, Diss, T., Evans, P. A. S., Gameiro, P., Garcia Sanz, R., Gonzalez, D., Grand, D., Håkansson, Å., Hummel, M., Liu, H., Lombardia, L., Macintyre, E. A., Milner, B. J., Montes-Moreno, S., Schuuring, E., Spaargaren, M., Hodges, E., van Dongen, J. J. M., Langerak, A. W., Groenen, P. J. T. A., Brueggemann, M., Beldjord, K., Bellan, C., Bonello, L., Boone, E., Carter, G. I., Catherwood, M., Davi, F., Delfau-Larue, M-H, Diss, T., Evans, P. A. S., Gameiro, P., Garcia Sanz, R., Gonzalez, D., Grand, D., Håkansson, Å., Hummel, M., Liu, H., Lombardia, L., Macintyre, E. A., Milner, B. J., Montes-Moreno, S., Schuuring, E., Spaargaren, M., Hodges, E., and van Dongen, J. J. M.

Abstract

PCR-based immunoglobulin (Ig)/T-cell receptor (TCR) clonality testing in suspected lymphoproliferations has largely been standardized and has consequently become technically feasible in a routine diagnostic setting. Standardization of the pre-analytical and post-analytical phases is now essential to prevent misinterpretation and incorrect conclusions derived from clonality data. As clonality testing is not a quantitative assay, but rather concerns recognition of molecular patterns, guidelines for reliable interpretation and reporting are mandatory. Here, the EuroClonality (BIOMED-2) consortium summarizes important pre- and post-analytical aspects of clonality testing, provides guidelines for interpretation of clonality testing results, and presents a uniform way to report the results of the Ig/TCR assays. Starting from an immunobiological concept, two levels to report Ig/TCR profiles are discerned: the technical description of individual (multiplex) PCR reactions and the overall molecular conclusion for B and T cells. Collectively, the EuroClonality (BIOMED-2) guidelines and consensus reporting system should help to improve the general performance level of clonality assessment and interpretation, which will directly impact on routine clinical management (standardized best-practice) in patients with suspected lymphoproliferations.

Published
2012
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114. Capillary electrophoresis single-strand conformation analysis (CE-SSCA) for clonality detection in lymphoproliferative disorders

Author

Gonzalez, D., Rombout, P., Sarasquete, M., Villarese, P., Wren, D., van Dongen, J.J., Garcia-Sanz, R., Macintyre, E.A., Langerak, A.W., Groenen, P.J.T.A., Gonzalez, D., Rombout, P., Sarasquete, M., Villarese, P., Wren, D., van Dongen, J.J., Garcia-Sanz, R., Macintyre, E.A., Langerak, A.W., and Groenen, P.J.T.A.

Abstract

Item does not contain fulltext

Published
2012

115. EuroClonality/BIOMED-2 guidelines for interpretation and reporting of Ig/TCR clonality testing in suspected lymphoproliferations

Author

Langerak, A.W., Groenen, P.J.T.A., Bruggemann, M., Beldjord, K., Bellan, C., Bonello, L., Boone, E., Carter, G.I., Catherwood, M., Davi, F., Delfau-Larue, M.H., Diss, T., Evans, P.A., Gameiro, P., Garcia Sanz, R., Gonzalez, D., Grand, D., Hakansson, A., Hummel, M., Liu, H., Lombardia, L., Macintyre, E.A., Milner, B.J., Montes-Moreno, S., Schuuring, E., Spaargaren, M., Hodges, E., van Dongen, J.J., Langerak, A.W., Groenen, P.J.T.A., Bruggemann, M., Beldjord, K., Bellan, C., Bonello, L., Boone, E., Carter, G.I., Catherwood, M., Davi, F., Delfau-Larue, M.H., Diss, T., Evans, P.A., Gameiro, P., Garcia Sanz, R., Gonzalez, D., Grand, D., Hakansson, A., Hummel, M., Liu, H., Lombardia, L., Macintyre, E.A., Milner, B.J., Montes-Moreno, S., Schuuring, E., Spaargaren, M., Hodges, E., and van Dongen, J.J.

Abstract

Item does not contain fulltext, PCR-based immunoglobulin (Ig)/T-cell receptor (TCR) clonality testing in suspected lymphoproliferations has largely been standardized and has consequently become technically feasible in a routine diagnostic setting. Standardization of the pre-analytical and post-analytical phases is now essential to prevent misinterpretation and incorrect conclusions derived from clonality data. As clonality testing is not a quantitative assay, but rather concerns recognition of molecular patterns, guidelines for reliable interpretation and reporting are mandatory. Here, the EuroClonality (BIOMED-2) consortium summarizes important pre- and post-analytical aspects of clonality testing, provides guidelines for interpretation of clonality testing results, and presents a uniform way to report the results of the Ig/TCR assays. Starting from an immunobiological concept, two levels to report Ig/TCR profiles are discerned: the technical description of individual (multiplex) PCR reactions and the overall molecular conclusion for B and T cells. Collectively, the EuroClonality (BIOMED-2) guidelines and consensus reporting system should help to improve the general performance level of clonality assessment and interpretation, which will directly impact on routine clinical management (standardized best-practice) in patients with suspected lymphoproliferations.

Published
2012

116. International Myeloma Working Group recommendations for global myeloma care

Author

Ludwig, H, primary, Miguel, J S, additional, Dimopoulos, M A, additional, Palumbo, A, additional, Garcia Sanz, R, additional, Powles, R, additional, Lentzsch, S, additional, Ming Chen, W, additional, Hou, J, additional, Jurczyszyn, A, additional, Romeril, K, additional, Hajek, R, additional, Terpos, E, additional, Shimizu, K, additional, Joshua, D, additional, Hungria, V, additional, Rodriguez Morales, A, additional, Ben-Yehuda, D, additional, Sondergeld, P, additional, Zamagni, E, additional, and Durie, B, additional

Published
2013
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117. Circulating clonotypic B cells in multiple myeloma and monoclonal gammopathy of undetermined significance

Author

Thiago, L. S., primary, Perez-Andres, M., additional, Balanzategui, A., additional, Sarasquete, M. E., additional, Paiva, B., additional, Jara-Acevedo, M., additional, Barcena, P., additional, Sanchez, M. L., additional, Almeida, J., additional, Gonzalez, M., additional, San Miguel, J. F., additional, Garcia-Sanz, R., additional, and Orfao, A., additional

Published
2013
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118. Intraclonal heterogeneity is a critical early event in the development of myeloma and precedes the development of clinical symptoms

Author

Walker, B A, primary, Wardell, C P, additional, Melchor, L, additional, Brioli, A, additional, Johnson, D C, additional, Kaiser, M F, additional, Mirabella, F, additional, Lopez-Corral, L, additional, Humphray, S, additional, Murray, L, additional, Ross, M, additional, Bentley, D, additional, Gutiérrez, N C, additional, Garcia-Sanz, R, additional, San Miguel, J, additional, Davies, F E, additional, Gonzalez, D, additional, and Morgan, G J, additional

Published
2013
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119. Powerful strategy for polymerase chain reaction-based clonality assessment in T-cell malignancies Report of the BIOMED-2 Concerted Action BHM4 CT98-3936.

Author

Bruggemann, M., White, H., Gaulard, P., Garcia-Sanz, R., Gameiro, P., Oeschger, S., Jasani, B., Ott, M., Delsol, G., Orfao, A., Tiemann, M., Herbst, H., Langerak, A.W., Spaargaren, M., Moreau, E.M.G., Groenen, P.J.T.A., Sambade, C., Foroni, L., Carter, G.I., Hummel, M., Bastard, C., Davi, F., Delfau-Larue, M.H., Kneba, M., Dongen, J.J.M. van, Beldjord, K., Molina, T.J., Bruggemann, M., White, H., Gaulard, P., Garcia-Sanz, R., Gameiro, P., Oeschger, S., Jasani, B., Ott, M., Delsol, G., Orfao, A., Tiemann, M., Herbst, H., Langerak, A.W., Spaargaren, M., Moreau, E.M.G., Groenen, P.J.T.A., Sambade, C., Foroni, L., Carter, G.I., Hummel, M., Bastard, C., Davi, F., Delfau-Larue, M.H., Kneba, M., Dongen, J.J.M. van, Beldjord, K., and Molina, T.J.

Abstract

Contains fulltext : 51510.pdf (publisher's version ) (Closed access), Polymerase chain reaction (PCR) assessment of clonal T-cell receptor (TCR) and immunoglobulin (Ig) gene rearrangements is an important diagnostic tool in mature T-cell neoplasms. However, lack of standardized primers and PCR protocols has hampered comparability of data in previous clonality studies. To obtain reference values for Ig/TCR rearrangement patterns, 19 European laboratories investigated 188 T-cell malignancies belonging to five World Health Organization-defined entities. The TCR/Ig spectrum of each sample was analyzed in duplicate in two different laboratories using the standardized BIOMED-2 PCR multiplex tubes accompanied by international pathology panel review. TCR clonality was detected in 99% (143/145) of all definite cases of T-cell prolymphocytic leukemia, T-cell large granular lymphocytic leukemia, peripheral T-cell lymphoma (unspecified) and angioimmunoblastic T-cell lymphoma (AILT), whereas nine of 43 anaplastic large cell lymphomas did not show clonal TCR rearrangements. Combined use of TCRB and TCRG genes revealed two or more clonal signals in 95% of all TCR clonal cases. Ig clonality was mostly restricted to AILT. Our study indicates that the BIOMED-2 multiplex PCR tubes provide a powerful strategy for clonality assessment in T-cell malignancies assisting the firm diagnosis of T-cell neoplasms. The detected TCR gene rearrangements can also be used as PCR targets for monitoring of minimal residual disease.

Published
2007

120. Restoration of microRNA-214 expression reduces growth of myeloma cells through positive regulation of P53 and inhibition of DNA replication

Author

Misiewicz-Krzeminska, I., primary, Sarasquete, M. E., additional, Quwaider, D., additional, Krzeminski, P., additional, Ticona, F. V., additional, Paino, T., additional, Delgado, M., additional, Aires, A., additional, Ocio, E. M., additional, Garcia-Sanz, R., additional, San Miguel, J. F., additional, and Gutierrez, N. C., additional

Published
2012
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121. EuroClonality/BIOMED-2 guidelines for interpretation and reporting of Ig/TCR clonality testing in suspected lymphoproliferations

Author

Langerak, A W, primary, Groenen, P J T A, additional, Brüggemann, M, additional, Beldjord, K, additional, Bellan, C, additional, Bonello, L, additional, Boone, E, additional, Carter, G I, additional, Catherwood, M, additional, Davi, F, additional, Delfau-Larue, M-H, additional, Diss, T, additional, Evans, P A S, additional, Gameiro, P, additional, Garcia Sanz, R, additional, Gonzalez, D, additional, Grand, D, additional, Håkansson, Å, additional, Hummel, M, additional, Liu, H, additional, Lombardia, L, additional, Macintyre, E A, additional, Milner, B J, additional, Montes-Moreno, S, additional, Schuuring, E, additional, Spaargaren, M, additional, Hodges, E, additional, and van Dongen, J J M, additional

Published
2012
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122. Genomic analysis of high-risk smoldering multiple myeloma

Author

Lopez-Corral, L., primary, Mateos, M. V., additional, Corchete, L. A., additional, Sarasquete, M. E., additional, de la Rubia, J., additional, de Arriba, F., additional, Lahuerta, J.-J., additional, Garcia-Sanz, R., additional, San Miguel, J. F., additional, and Gutierrez, N. C., additional

Published
2012
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123. Design and standardization of PCR primers and protocols for detection of clonal immunoglobulin and T-cell receptor gene recombinations in suspect lymphoproliferations: report of the BIOMED-2 Concerted Action BMH4-CT98-3936.

Author

Dongen, J.J.M. van, Langerak, A.W., Bruggemann, M., Evans, P., Hummel, M., Lavender, F.L., Delabesse, E., Davi, F., Schuuring, E., Garcia-Sanz, R., Krieken, J.H.J.M. van, Droese, J., Gonzalez, D., Bastard, C., White, H.E., Spaargaren, M.C., Gonzalez, M., Parreira, A., Smith, J.L., Morgan, G.J., Kneba, M., Macintyre, E.A., Dongen, J.J.M. van, Langerak, A.W., Bruggemann, M., Evans, P., Hummel, M., Lavender, F.L., Delabesse, E., Davi, F., Schuuring, E., Garcia-Sanz, R., Krieken, J.H.J.M. van, Droese, J., Gonzalez, D., Bastard, C., White, H.E., Spaargaren, M.C., Gonzalez, M., Parreira, A., Smith, J.L., Morgan, G.J., Kneba, M., and Macintyre, E.A.

Abstract

Contains fulltext : 142619.pdf (publisher's version ) (Closed access), In a European BIOMED-2 collaborative study, multiplex PCR assays have successfully been developed and standardized for the detection of clonally rearranged immunoglobulin (Ig) and T-cell receptor (TCR) genes and the chromosome aberrations t(11;14) and t(14;18). This has resulted in 107 different primers in only 18 multiplex PCR tubes: three VH-JH, two DH-JH, two Ig kappa (IGK), one Ig lambda (IGL), three TCR beta (TCRB), two TCR gamma (TCRG), one TCR delta (TCRD), three BCL1-Ig heavy chain (IGH), and one BCL2-IGH. The PCR products of Ig/TCR genes can be analyzed for clonality assessment by heteroduplex analysis or GeneScanning. The detection rate of clonal rearrangements using the BIOMED-2 primer sets is unprecedentedly high. This is mainly based on the complementarity of the various BIOMED-2 tubes. In particular, combined application of IGH (VH-JH and DH-JH) and IGK tubes can detect virtually all clonal B-cell proliferations, even in B-cell malignancies with high levels of somatic mutations. The contribution of IGL gene rearrangements seems limited. Combined usage of the TCRB and TCRG tubes detects virtually all clonal T-cell populations, whereas the TCRD tube has added value in case of TCRgammadelta(+) T-cell proliferations. The BIOMED-2 multiplex tubes can now be used for diagnostic clonality studies as well as for the identification of PCR targets suitable for the detection of minimal residual disease.

Published
2003

127. Upregulation of Dicer is more frequent in monoclonal gammopathies of undetermined significance than in multiple myeloma patients and is associated with longer survival in symptomatic myeloma patients

Author

Sarasquete, M. E., primary, Gutierrez, N. C., additional, Misiewicz-Krzeminska, I., additional, Paiva, B., additional, Chillon, M. C., additional, Alcoceba, M., additional, Garcia-Sanz, R., additional, Hernandez, J. M., additional, Gonzalez, M., additional, and San-Miguel, J. F., additional

Published
2010
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128. Long FLT3 internal tandem duplications and reduced PML-RAR expression at diagnosis characterize a high-risk subgroup of acute promyelocytic leukemia patients

Author

Chillon, M. C., primary, Santamaria, C., additional, Garcia-Sanz, R., additional, Balanzategui, A., additional, Maria Eugenia, S., additional, Alcoceba, M., additional, Marin, L., additional, Caballero, M. D., additional, Vidriales, M. B., additional, Ramos, F., additional, Bernal, T., additional, Diaz-Mediavilla, J., additional, de Coca, A. G., additional, Penarrubia, M. J., additional, Queizan, J. A., additional, Giraldo, P., additional, San Miguel, J. F., additional, and Gonzalez, M., additional

Published
2010
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130. The relevance of preferentially expressed antigen of melanoma (PRAME) as a marker of disease activity and prognosis in acute promyelocytic leukemia

Author

Santamaria, C., primary, Chillon, M. C., additional, Garcia-Sanz, R., additional, Balanzategui, A., additional, Sarasquete, M. E., additional, Alcoceba, M., additional, Ramos, F., additional, Bernal, T., additional, Queizan, J. A., additional, Penarrubia, M. J., additional, Giraldo, P., additional, San Miguel, J. F., additional, and Gonzalez, M., additional

Published
2008
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131. Bortezomib plus melphalan and prednisone in elderly untreated patients with multiple myeloma: updated time-to-events results and prognostic factors for time to progression

Author

Mateos, M.-V., primary, Hernandez, J. M., additional, Hernandez, M. T., additional, Gutierrez, N. C., additional, Palomera, L., additional, Fuertes, M., additional, Garcia-Sanchez, P., additional, Lahuerta, J. J., additional, de la Rubia, J., additional, Terol, M.-J., additional, Sureda, A., additional, Bargay, J., additional, Ribas, P., additional, Alegre, A., additional, de Arriba, F., additional, Oriol, A., additional, Carrera, D., additional, Garcia-Larana, J., additional, Garcia-Sanz, R., additional, Blade, J., additional, Prosper, F., additional, Mateo, G., additional, Esseltine, D.-L., additional, van de Velde, H., additional, and San Miguel, J. F., additional

Published
2008
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132. Presence of DRB1*01 Allele in Multiple Myeloma Patients Is Associated with Indolent Disease.

Author

Alcoceba, M., primary, Marin, L., primary, Balanzategui, A., primary, Sarasquete, M.E., primary, Martin-Jimenez, P., primary, Chillon, M.C., primary, Vargas, M., primary, Corral, R., primary, Perez, E., primary, Fernandez-Calvo, J., primary, Martinez, A., primary, Hernandez, J.M., primary, Blade, Joan, primary, Lahuerta, J.J., primary, Garcia-Sanz, R., primary, Gonzalez, M., primary, and Miguel, J.F. San, primary

Published
2007
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133. Clinical Efficacy of Bortezomib Based Therapy in Plasma Cell Leukemias.

Author

Alegre, Adrian, primary, Aguado, B., additional, Lahuerta, J.J., additional, Cervero, C., additional, Oriol, A., additional, Abella, A., additional, Carrion, R., additional, Renat, R., additional, Hernandez-Rivas, J.A., additional, de la Rubia, J., additional, Mateos, M.V., additional, Garcia-Sanz, R., additional, Rodriguez-Notario, R., additional, Navas, B., additional, Fernandez-Rañada, J.M., additional, and Miguel, J.F. San, additional

Published
2007
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136. Powerful strategy for polymerase chain reaction-based clonality assessment in T-cell malignancies Report of the BIOMED-2 Concerted Action BHM4 CT98-3936

Author

Brüggemann, M, primary, White, H, additional, Gaulard, P, additional, Garcia-Sanz, R, additional, Gameiro, P, additional, Oeschger, S, additional, Jasani, B, additional, Ott, M, additional, Delsol, G, additional, Orfao, A, additional, Tiemann, M, additional, Herbst, H, additional, Langerak, A W, additional, Spaargaren, M, additional, Moreau, E, additional, Groenen, P J T A, additional, Sambade, C, additional, Foroni, L, additional, Carter, G I, additional, Hummel, M, additional, Bastard, C, additional, Davi, F, additional, Delfau-Larue, M-H, additional, Kneba, M, additional, van Dongen, J J M, additional, Beldjord, K, additional, and Molina, T J, additional

Published
2006
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137. 6q deletion in Waldenström macroglobulinemia is associated with features of adverse prognosis

Author

Ocio, E. M., primary, Schop, R. F. J., additional, Gonzalez, B., additional, Van Wier, S. A., additional, Hernandez‐Rivas, J. M., additional, Gutierrez, N. C., additional, Garcia‐Sanz, R., additional, Moro, M. J., additional, Aguilera, C., additional, Hernandez, J., additional, Xu, R., additional, Greipp, P. R., additional, Dispenzieri, A., additional, Jalal, S. M., additional, Lacy, M. Q., additional, Gonzalez‐Paz, N., additional, Gertz, M. A., additional, San Miguel, J. F., additional, and Fonseca, R., additional

Published
2006
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138. High-Dose Therapy/Stem Cell Support (HDT), Including Tandem Transplant, for Primary Refractory Multiple Myeloma (MM): Results from the Spanish Myeloma Group (PETHEMA/GEM) in 49 Patients.

Author

Rosinol, L., primary, Garcia-Sanz, R., additional, Lahuerta, J. J., additional, Hernandez-Garcia, M., additional, Sureda, A., additional, de la Rubia, J., additional, Ribera, J. M., additional, Hernandez-Ruiz, B., additional, Carreras, D., additional, Navarro, I., additional, Garcia-Ruiz, J. C., additional, Gardella, S., additional, Garcia-Larana, J., additional, Diaz-Mediavilla, J., additional, San Miguel, J. F., additional, and Blade, J., additional

Published
2005
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142. Report of Consensus Panel 4 from the 11thInternational Workshop on Waldenstrom's Macroglobulinemia on Diagnostic and Response Criteria

Author

Treon, SP, Tedeschi, A, San-Miguel, J, Garcia-Sanz, R, Anderson, KC, Kimby, E, Minnema, MC, Benevolo, G, Qiu, L, Yi, S, Terpos, E, Tam, CS, Castillo, JJ, Morel, P, Dimopoulos, M, and Owen, RG

Abstract

Consensus Panel 4 (CP4) of the 11thInternational Workshop on Waldenstrom's Macroglobulinemia (IWWM-11) was tasked with reviewing the current criteria for diagnosis and response assessment. Since the initial consensus reports of the 2ndInternational Workshop, there have been updates in the understanding of the mutational landscape of IgM related diseases, including the discovery and prevalence of MYD88 and CXCR4 mutations; an improved recognition of disease related morbidities attributed to monoclonal IgM and tumor infiltration; and a better understanding of response assessment based on multiple, prospective trials that have evaluated diverse agents in WM. The key recommendations from IWWM-11 CP4 included: i) re-affirmation of IWWM-2 consensus panel recommendations that arbitrary values for laboratory parameters such as minimal IgM level or BM infiltration should not be used to distinguish WM from IgM MGUS; ii) delineation of IgM MGUS into two subclasses including a subtype characterized by clonal plasma cells and MYD88 wild-type, and the other by presence of monotypic or monoclonal B cells which may carry the MYD88 mutation; and iii) recognition of “simplified” response assessments that use serum IgM only for determining partial and very good partial responses (simplified IWWM-6/new IWWM-11 response criteria). Guidance on response determination for suspected IgM flare and IgM rebound related to treatment, as well as extramedullary disease assessment was also updated and included in this report.

Published
2023
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143. Report of Consensus Panel 3 from the 11thInternational Workshop on Waldenström's Macroglobulinemia: Recommendations for Molecular Diagnosis in Waldenström's Macroglobulinemia

Author

Garcia-Sanz, R, Varettoni, M, Jiménez, C, Ferrero, S, Poulain, S, San-Miguel, JF, Guerrera, ML, Drandi, D, Bagratuni, T, McMaster, M, Roccaro, AM, Roos-Weil, D, Leiba, M, Li, Y, Qiu, L, Hou, J, De Larrea, C Fernandez, Castillo, JJ, Dimopoulos, M, Owen, RG, Treon, SP, and Hunter, ZR

Abstract

Apart from the MYD88L265Pmutation, extensive information exists on the molecular mechanisms in Waldenström's Macroglobulinemia and its potential utility in the diagnosis and treatment tailoring. However, no consensus recommendations are yet available. Consensus Panel 3 (CP3) of the 11thInternational Workshop on Waldenström's Macroglobulinemia (IWWM-11) was tasked with reviewing the current molecular necessities and best way to access the minimum data required for a correct diagnosis and monitoring. Key recommendations from IWWM-11 CP3 included: 1) molecular studies are warranted for patients in whom therapy is going to be started; such studies should also be done in those whose bone marrow (BM) material is sampled based on clinical issues; 2) molecular studies considered essential for these situations are those that clarify the status of 6q and 17p chromosomes, and MYD88, CXCR4, and TP53genes. These tests in other situations, and/or other tests, are considered optional; 3) independently of the use of more sensitive and/or specific techniques, the minimum requirements are Allele Specific Polymerase Chain Reaction for MYD88L265Pand CXCR4S338Xusing whole BM, and Fluorescence in situ hybridization for 6q and 17p and sequencing for CXCR4and TP53using CD19+ enriched BM; 4) these requirements refer to all patients; therefore, sample should be sent to specialized centers.

Published
2023
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144. Report of Consensus Panel 7 from the 11thInternational Workshop on Waldenström Macroglobulinemia on Priorities for Novel Clinical Trials.

Author

Tam, CS, Kapoor, P, Castillo, JJ, Buske, C, Ansell, SM, Branagan, AR, Kimby, E, Li, Y, Palomba, ML, Qiu, L, Shadman, M, Abeykoon, JP, Sarosiek, S, Vos, JMI, Yi, S, Stephens, D, Roos-Weil, D, Roccaro, AM, Morel, P, Munshi, NC, Anderson, KC, San-Miguel, J, Garcia-Sanz, R, Dimopoulos, MA, Treon, SP, and Kersten, MJ.

Abstract

Recent advances in the understanding of Waldenström macroglobulinemia (WM) biology have impacted the development of effective novel agents and improved our knowledge of how the genomic background of WM may influence selection of therapy. Consensus Panel 7 (CP7) of the 11thInternational Workshop on WM was convened to examine the current generation of completed and ongoing clinical trials involving novel agents, consider updated data on WM genomics, and make recommendations on the design and prioritization of future clinical trials. CP7 considers limited duration and novel-novel agent combinations to be the priority for the next generation of clinical trials. Evaluation of MYD88, CXCR4and TP53at baseline in the context of clinical trials is crucial. The common chemoimmunotherapy backbones, bendamustine-rituximab (BR) and dexamethasone, rituximab and cyclophosphamide (DRC), may be considered standard-of-care for the frontline comparative studies. Key unanswered questions include the definition of frailty in WM; the importance of attaining a very good partial response or better (≥VGPR), within stipulated time frame, in determining survival outcomes; and the optimal treatment of WM populations with special needs

Published
2023
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146. Incomplete DJH rearrangements of the IgH gene are frequent in multiple myeloma patients: immunobiological characteristics and clinical implications.

Author

Gonzalez, D, Balanzategui, A, Garcia-Sanz, R, Gutierrez, N, Seabra, C, van Dongen, J J M, Gonzalez, M, and San Miguel, J F

Subjects
B cell lymphoma, MULTIPLE myeloma, CELL proliferation, LYMPHOBLASTIC leukemia, LYMPHOPROLIFERATIVE disorders
Abstract

DH-JH rearrangements of the Ig heavy-chain gene (IGH) occur early during B-cell development. Consequently, they are detected in precursor-B-cell acute lymphoblastic leukemias both at diagnosis and relapse. Incomplete DJH rearrangements have also been occasionally reported in mature B-cell lymphoproliferative disorders, but their frequency and immunobiological characteristics have not been studied in detail. We have investigated the frequency and characteristics of incomplete DJH as well as complete VDJH rearrangements in a series of 84 untreated multiple myeloma (MM) patients. The overall detection rate of clonality by amplifying VDJH and DJH rearrangements using family-specific primers was 94%. Interestingly, we found a high frequency (60%) of DJH rearrangements in this group. As expected from an immunological point of view, the vast majority of DJH rearrangements (88%) were unmutated. To the best of our knowledge, this is the first systematic study describing the incidence of incomplete DJH rearrangements in a series of unselected MM patients. These results strongly support the use of DJH rearrangements as PCR targets for clonality studies and, particularly, for quantification of minimal residual disease by real-time quantitative PCR using consensus JH probes in MM patients. The finding of hypermutation in a small proportion of incomplete DJH rearrangements (six out of 50) suggests important biological implications concerning the process of somatic hypermutation. Moreover, our data offer a new insight in the regulatory development model of IGH rearrangements. [ABSTRACT FROM AUTHOR]

Published
2003

147. Incomplete DJH rearrangements as a novel tumor target for minimal residual disease quantitation in multiple myeloma using real-time PCR.

Author

Gonzalez, D, Gonzalez, M, Alonso, M E, Lopez-Perez, R, Balanzategui, A, Chillon, M C, Silva, M, Garcia-Sanz, R, and San Miguel, J F

Subjects
IMMUNOGLOBULINS, MULTIPLE myeloma
Abstract

The hypervariable regions of immunoglobulin heavy-chain (IgH) rearrangements provide a specific tumor marker in multiple myeloma (MM). Recently, real-time PCR assays have been developed in order to quantify the number of tumor cells after treatment. However, these strategies are hampered by the presence of somatic hypermutation (SH) in VDJH rearrangements from multiple myeloma (MM) patients, which causes mismatches between primers and/or probes and the target, leading to a nonaccurate quantification of tumor cells. Our group has recently described a 60% incidence of incomplete DJH rearrangements in MM patients, with no or very low rates of SH. In this study, we compare the efficiency of a real-time PCR approach for the analysis of both complete and incomplete IgH rearrangements in eight MM patients using only three JH consensus probes. We were able to design an allele-specific oligonucleotide for both the complete and incomplete rearrangement in all patients. DJH rearrangements fulfilled the criteria of effectiveness for real-time PCR in all samples (ie no unspecific amplification, detection of less than 10 tumor cells within 10[SUP5] polyclonal background and correlation coefficients of standard curves higher than 0.98). By contrast, only three out of eight VDJH rearrangements fulfilled these criteria. Further analyses showed that the remaining five VDJH rearrangements carried three or more somatic mutations in the probe and primer sites, leading to a dramatic decrease in the melting temperature. These results support the use of incomplete DJH rearrangements instead of complete somatically mutated VDJH rearrangements for investigation of minimal residual disease in multiple myeloma. [ABSTRACT FROM AUTHOR]

Published
2003

148. Patterns of BCR/ABL gene rearrangements by interphase fluorescence in situ hybridization (FISH) in BCR/ABL+ leukemias: incidence and underlying genetic abnormalities.

Author

Primo, D, Tabernero, M D, Rasillo, A, Sayagues, J M, Espinosa, A B, Chillon, M C, Garcia-Sanz, R, Gutierrez, N, Giralt, M, Hagemeijer, A, San Miguel, J F, and Orfao, A

Subjects
FLUORESCENCE in situ hybridization, MYELOID leukemia
Abstract

Interphase fluorescence in situ hybridization (iFISH) is increasingly used for the identification of BCR/ABL gene rearrangements in chronic myeloid leukemia (CML) and acute lymphoblastic leukemia (ALL). In the present study, we have explored the incidence of both typical and atypical iFISH patterns of BCR/ABL gene rearrangements in a series of 168 consecutive BCR/ABL[SUP+] patients - 135 CML, 31 precursor B-ALL and two acute myeloblastic leukemia (AML) cases -- and established their underlying genetic alterations through further molecular and chromosome analyses. Two different FISH probes (Vysis Inc., Downers Grove, IL, USA) were used: the LSI BCR/ABL dual color extra signal (ES) and the dual color dual fusion BCR/ABL probe (D-FISH). Our results show that most BCR/ABL[SUP+] patients (83%, including 88% of all CML, 61% of ALL and one of two AML) displayed typical iFISH patterns of either Major (M) BCR/ABL (87% of CML, 13% of ALL and one of the two AML) or minor (m) BCR/ABL gene rearrangements (1% of all CML and 48% of ALL cases) with the two probes. Further molecular and cytogenetic studies confirmed the presence of such typical rearrangements in all except one of these ALL cases who had coexistence of an MBCR/ABL and an mBCR/ ABL gene rearrangement together with monosomy 9. In the remaining 29 cases (17%), up to five different atypical iFISH patterns were detected with the ES probe. Atypical iFISH patterns were most frequently due to additional numerical changes -- most often supernumerary Philadelphia (Ph) chromosome (7%) but also gain or loss of chromosome 9 (1%) or 22 (1%). Deletion of 9q sequences proximal to the breakpoint were also frequently observed with the ES probe (8%). Application of the D-FISH probe showed that in most of these latter cases (5%) deletion of 22q sequences distal to the breakpoint also occurred. The remaining cases with atypical iFISH had cryptic insertion of BCR in 9q34 (1%). Exact interpretation of each iFISH pattern was supported... [ABSTRACT FROM AUTHOR]

Published
2003
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149. The combination of thalidomide, cyclophosphamide and dexamethasone (ThaCyDex) is feasible and can be an option for relapsed/refratory multiple myeloma.

Author

Garcia-Sanz, R. and Gonzalez-Fraile, M.I.

Subjects
*THALIDOMIDE, *TERATOGENIC agents
Abstract

Introduction: Thalidomide has recently proven to be a useful drug for treatment of refractory and relapsed multiple myeloma patients, up to 35% of whom achieve remission. However, little is known about the potential additive or synergistic effect upon its association with other drugs with proven efficacy in MM. Material and methods: The present pilot study was designed to evaluate the toxicity and response rate of the association of thalidomide, cyclophosphamide and dexamethasone (ThaCyDex) in 22 refractory or relapsed MM patients. The protocol scheduled the administration of thalidomide at escalating doses (200 to 800 mg/day), daily oral cyclophosphamide (CTX) (50 mg/day) and pulsed dexamethasone (40 mg/day, four days every three weeks). Results: Adverse effects were moderate (grade ≥2) with only two patients in whom treatment was withdrawn due to neuropathy and severe somnolence. Infections were recorded in six patients, four requiring hospitalization for intravenous antibiotic therapy. No cases of thrombocytopenia grade ≥2 were noted. Other side effects included grade ≥2 constipation (29%), somnolence (35%) or dizziness (12%). In addition, one case of meralgia paresthetica and one with a deep venous thrombosis were noted. Two cases displayed hyperglycemia and myopathy attributed to dexamethasone, which was solved upon changing to prednisone. With a median follow-up of 12 months, 17 patients were evaluable for response; 13 (77%) responded to the therapy, including nine cases (53%) with a > 50% M-component reduction (two of them with a complete remission). Only two responders have already progressed, with a projected event free survival of 51% at 12 months. Seven patients have died due to disease progression (n = 5), sudden death (n = 1) and infection (n = 1). Conclusion: This study shows that ThaCyDex is a feasible and promising therapeutic approach for patients with relapsed/refractory MM. [ABSTRACT FROM AUTHOR]

Published
2002
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