High‐risk cytogenetic abnormalities in multiple myeloma: PETHEMA‐GEM experience
Veronica González‐Calle,
Paula Rodriguez‐Otero,
Maria J. Calasanz,
Manuela Guijarro,
Joaquin Martínez‐López,
Laura Rosiñol,
Miguel T. Hernández,
Ana I. Teruel,
Mercedes Gironella,
Albert Oriol,
Javier de laRubia,
Ana P. González‐Rodríguez,
Joan Bargay,
Felipe deArriba,
Luis Palomera,
Marta‐Sonia González‐Pérez,
Anna Sureda,
Enrique Ocio,
Juan J. Lahuerta,
Joan Bladé,
Jesus F. San Miguel,
Maria V. Mateos,
Norma C. Gutiérrez
Affiliations
Veronica González‐Calle
Department of Hematology, Hospital Universitario de Salamanca, Instituto de Investigacion Biomedica de Salamanca (IBSAL), Centro de Investigación del Cancer (IBMCC‐USAL, CSIC) CIBERONC Salamanca Spain
Paula Rodriguez‐Otero
Department of Hematology, Cancer Center Clinica Universidad de Navarra, CCUN, Centro de Investigacion Medica Aplicadas (Cima); Instituto de Investigación Sanitaria de Navarra (IDISNA) CIBERONC Pamplona Spain
Maria J. Calasanz
Department of Hematology, Cancer Center Clinica Universidad de Navarra, CCUN, Centro de Investigacion Medica Aplicadas (Cima); Instituto de Investigación Sanitaria de Navarra (IDISNA) CIBERONC Pamplona Spain
Manuela Guijarro
Department of Hematology, Hospital Universitario 12 de Octubre, I + 12, CNIO Complutense University, CIBERONC Madrid Spain
Joaquin Martínez‐López
Department of Hematology, Hospital Universitario 12 de Octubre, I + 12, CNIO Complutense University, CIBERONC Madrid Spain
Laura Rosiñol
Department of Hematology, Hospital Clínic IDIBAPS Barcelona Spain
Miguel T. Hernández
Department of Hematology Hospital Universitario de Canarias Tenerife Spain
Ana I. Teruel
Department of Hematology Hospital Clínico de Valencia Valencia Spain
Mercedes Gironella
Department of Hematology Hospital Vall d'Hebron Barcelona Spain
Albert Oriol
Department of Hematology, Institut Català d'Oncologia i Institut Josep Carreras Hospital Germans Trias i Pujol Badalona Spain
Javier de laRubia
Department of Hematology, Hospital Universitario y Politécnico La Fe CIBERONC Valencia Spain
Ana P. González‐Rodríguez
Department of Hematology Hospital Universitario Central De Asturias Oviedo Spain
Joan Bargay
Department of Hematology Hospital Son Llatzer Palma de Mallorca Spain
Felipe deArriba
Department of Hematology, Hospital Morales Meseguer, IMIB‐Pascual Parrilla Universidad de Murcia Murcia Spain
Luis Palomera
Department of Hematology Hospital Clinico Universitario Lozano Blesa Zaragoza Spain
Marta‐Sonia González‐Pérez
Department of Hematology, University Hospital of Santiago de Compostela Servizo Galego de Saúde (SERGAS) Santiago de Compostela Spain
Anna Sureda
Department of Hematology Institut Català D'Oncologia L'Hospitalet Badalona Spain
Enrique Ocio
Department of Hematology Hospital Universitario Marques de Valdecilla Santander Spain
Juan J. Lahuerta
Department of Hematology, Hospital Universitario 12 de Octubre, I + 12, CNIO Complutense University, CIBERONC Madrid Spain
Joan Bladé
Department of Hematology, Hospital Clínic IDIBAPS Barcelona Spain
Jesus F. San Miguel
Department of Hematology, Cancer Center Clinica Universidad de Navarra, CCUN, Centro de Investigacion Medica Aplicadas (Cima); Instituto de Investigación Sanitaria de Navarra (IDISNA) CIBERONC Pamplona Spain
Maria V. Mateos
Department of Hematology, Hospital Universitario de Salamanca, Instituto de Investigacion Biomedica de Salamanca (IBSAL), Centro de Investigación del Cancer (IBMCC‐USAL, CSIC) CIBERONC Salamanca Spain
Norma C. Gutiérrez
Department of Hematology, Hospital Universitario de Salamanca, Instituto de Investigacion Biomedica de Salamanca (IBSAL), Centro de Investigación del Cancer (IBMCC‐USAL, CSIC) CIBERONC Salamanca Spain
Abstract This study examines the impact of cytogenetic abnormalities and their co‐segregation on the prognosis of newly diagnosed multiple myeloma patients. The analysis included 1304 patients from four different GEM‐PETHEMA clinical trials. Genetic alterations, such as t(4;14), t(14;16), del(17p), +1q, and del(1p), were investigated using FISH on CD38 purified plasma cells. The frequency of genetic alterations detected were as follows: del(17p) in 8%, t(4;14) in 12%, t(14;16) in 3%, +1q in 43%, and del(1p) in 8%. The median follow‐up was 61 months, and the median progression‐free survival (PFS) and overall survival (OS) were 44 months and not reached, respectively. Consistent with previous reports, the presence of t(4;14) was associated with shorter PFS and OS. In our series, the presence of t(14;16) did not impact survival, maybe due to limitations in sample size. Del(17p) was linked to poor prognosis using a cut‐off level of ≥20% positive cells, without any impact of higher cut‐off in prognosis, except for patients with clonal fraction ≥80% who had a dismal outcome. Cosegregation of cytogenetic abnormalities patients worsened the prognosis in t(4;14) patients but not in patients with del(17p), which retained its adverse prognosis even as a solitary abnormality. Gain(1q) was associated with significantly shorter PFS and OS, while del(1p) affected PFS but not OS. Nevertheless, when co‐segregation was eliminated, the detrimental effect of +1q or del(1p) was no longer observed. In conclusion, this study confirms the prognostic significance of high‐risk cytogenetic abnormalities in MM and highlights the importance of considering co‐occurrence for accurate prognosis assessment.
