Beyond NPM-anaplastic lymphoma kinase driven lymphomagenesis

Tabbò, Fabrizio; Ponzoni, Maurilio; Rabadan, Raul; Bertoni, Francesco; cell Lymphoma Study Group, Giorgio Inghirami European T.; Sabrina, Aliberti; Antonella, Barreca; Luca, Besson; Ramona, Crescenzo; Di Giacomo Filomena,; Marcello, Gaudiano; Giorgio, Inghirami; Indira, Landra; Elena, Lasorsa; Rodolfo, Machiorlatti; Elisabetta, Mereu; Katia, Messana; Domenico, Novero; Elisa, Pellegrino; Achille, Pich; Roberto, Piva; Irene, Scarfo; Elisa, Spaccarotella; Fabrizio, Tabbo; Maria, Todaro; Ivana, Ubezzi; Susanna, Urigu; Francesco, Vittone; Francesco, Abage; Elisa, Ficarra; Andrea, Acquaviva; Maurilio, Ponzoni; Carmelo, Stella; Agostinelli, Claudio; Piccaluga, PIER PAOLO; Pileri, Stefano; Brunangelo, Falini; Enrico, Tiacci; Francesco, Bertoni; Michela, Boi; Ivo, Kwee

doi:10.1097/MOH.0b013e3283623c07

PURPOSE OF REVIEW: Anaplastic large cell lymphomas (ALCLs) are rare entities whose somatic genetic lesions have been identified only in a subset of patients. Thus, an integrated and massive discovery programme is required to define their tumourigenic alterations and to design more successful tailored therapies. RECENT FINDINGS: The discovery of anaplastic lymphoma kinase (ALK) fusions has provided the basis for the characterization of distinct subsets among ALCL patients. Although the oncogenic addiction of ALK signalling is proven, the tumorigenic contribution of coactivating lesions is still missing. As ALK- and ALK+ share common signatures, it is plausible that analogous mechanisms of transformation may be operating in both subsets, as confirmed by the dysregulated activation of c-MYC, RAS and NFκB, and the loss of Blimp-1 and p53/p63 axis. Nonetheless, recurrent genetic alterations for ALK- ALCL or refractory leukaemic ALK+ ALCL are lacking. Moreover, although conventional chemotherapies (anthracycline-based) are most successful, that is in ALK+ ALCL patients, the implementation of ALK inhibitors or of anti-CD30 based treatments provides innovative solutions, particularly in paediatric ALK+ ALCL and in chemorefractory/relapsed patients. SUMMARY: The complete portrayal of the landscape of genetic alterations in ALCL will dictate the development of innovative chemotherapeutic and targeted therapies that will fit most with the molecular and clinical profiling of individual patients.

Beyond NPM-anaplastic lymphoma kinase driven lymphomagenesis / Fabrizio Tabbò,Maurilio Ponzoni,Raul Rabadan,Francesco Bertoni,Giorgio Inghirami European T-cell Lymphoma Study Group; Aliberti Sabrina; Barreca Antonella; Besson Luca; Crescenzo Ramona; Di Giacomo Filomena; Gaudiano Marcello; Inghirami Giorgio; Landra Indira; Lasorsa Elena; Machiorlatti Rodolfo; Mereu Elisabetta; Messana Katia; Novero Domenico; Pellegrino Elisa; Pich Achille; Piva Roberto; Scarfo Irene; Spaccarotella Elisa; Tabbo Fabrizio; Todaro Maria; Ubezzi Ivana; Urigu Susanna; Vittone Francesco; Abage Francesco; Ficarra Elisa; Acquaviva Andrea; Ponzoni Maurilio; Stella Carmelo; Agostinelli Claudio; Piccaluga Pier Paolo; Pileri Stefano; Falini Brunangelo; Tiacci Enrico; Bertoni Francesco; Boi Michela; Kwee Ivo. - In: CURRENT OPINION IN HEMATOLOGY. - ISSN 1065-6251. - STAMPA. - 20:(2013), pp. 374-381. [10.1097/MOH.0b013e3283623c07]