CD30-positive peripheral T-cell lymphomas share molecular and phenotypic features
Bettina Bisig,
Aurélien de Reyniès,
Christophe Bonnet,
Pierre Sujobert,
David S. Rickman,
Teresa Marafioti,
Georges Delsol,
Laurence Lamant,
Philippe Gaulard,
Laurence de Leval
Affiliations
Bettina Bisig
University Institute of Pathology, Centre Hospitalier Universitaire Vaudois (CHUV), Lausanne, Switzerland;Department of Pathology, Centre Hospitalier Universitaire (CHU) Sart Tilman, Liège, Belgium;Laboratory of Experimental Pathology, GIGA–Research, University of Liège, Belgium
Aurélien de Reyniès
Programme Cartes d’Identité des Tumeurs (CIT), Ligue Nationale Contre le Cancer, Paris, France
Christophe Bonnet
Department of Hematology, CHU Sart Tilman, Liège, Belgium
Pierre Sujobert
Department of Pathology, Assistance Publique – Hôpitaux de Paris (AP–HP), Groupe Hospitalier Henri Mondor–Albert Chenevier, Créteil, France
David S. Rickman
Department of Pathology and Laboratory Medicine, Weill Cornell Medical College, New York, NY, USA
Teresa Marafioti
Department of Histopathology, University College Hospital, London, UK
Georges Delsol
Department of Pathology and INSERM U563, CHU Purpan, Toulouse, France
Laurence Lamant
Department of Pathology and INSERM U563, CHU Purpan, Toulouse, France
Philippe Gaulard
Department of Pathology, Assistance Publique – Hôpitaux de Paris (AP–HP), Groupe Hospitalier Henri Mondor–Albert Chenevier, Créteil, France;INSERM U955, Créteil, France;Université Paris-Est, Faculté de Médecine, Créteil, France
Laurence de Leval
University Institute of Pathology, Centre Hospitalier Universitaire Vaudois (CHUV), Lausanne, Switzerland;Department of Pathology, Centre Hospitalier Universitaire (CHU) Sart Tilman, Liège, Belgium;Laboratory of Experimental Pathology, GIGA–Research, University of Liège, Belgium
Peripheral T-cell lymphoma, not otherwise specified is a heterogeneous group of aggressive neoplasms with indistinct borders. By gene expression profiling we previously reported unsupervised clusters of peripheral T-cell lymphomas, not otherwise specified correlating with CD30 expression. In this work we extended the analysis of peripheral T-cell lymphoma molecular profiles to prototypical CD30+ peripheral T-cell lymphomas (anaplastic large cell lymphomas), and validated mRNA expression profiles at the protein level. Existing transcriptomic datasets from peripheral T-cell lymphomas, not otherwise specified and anaplastic large cell lymphomas were reanalyzed. Twenty-one markers were selected for immunohistochemical validation on 80 peripheral T-cell lymphoma samples (not otherwise specified, CD30+ and CD30−; anaplastic large cell lymphomas, ALK+ and ALK−), and differences between subgroups were assessed. Clinical follow-up was recorded. Compared to CD30− tumors, CD30+ peripheral T-cell lymphomas, not otherwise specified were significantly enriched in ALK− anaplastic large cell lymphoma-related genes. By immunohistochemistry, CD30+ peripheral T-cell lymphomas, not otherwise specified differed significantly from CD30− samples [down-regulated expression of T-cell receptor-associated proximal tyrosine kinases (Lck, Fyn, Itk) and of proteins involved in T-cell differentiation/activation (CD69, ICOS, CD52, NFATc2); upregulation of JunB and MUM1], while overlapping with anaplastic large cell lymphomas. CD30− peripheral T-cell lymphomas, not otherwise specified tended to have an inferior clinical outcome compared to the CD30+ subgroups. In conclusion, we show molecular and phenotypic features common to CD30+ peripheral T-cell lymphomas, and significant differences between CD30− and CD30+ peripheral T-cell lymphomas, not otherwise specified, suggesting that CD30 expression might delineate two biologically distinct subgroups.
