Identification of a New Subclass of ALK-negative ALCL Expressing Aberrant Levels of ERBB4 Transcripts

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2015 Oct 15

PMID 26463425

Citations 60

Authors

Irene Scarfo

Elisa Pellegrino

Elisabetta Mereu

Ivo Kwee

Luca Agnelli

Elisa Bergaggio

Giulia Garaffo

Nicoletta Vitale

Manuel Caputo

Rodolfo Machiorlatti

Paola Circosta

Francesco Abate

Antonella Barreca

Domenico Novero

Susan Mathew

Andrea Rinaldi

Enrico Tiacci

Sara Serra

Silvia Deaglio

Antonino Neri

Brunangelo Falini

Raul Rabadan

Francesco Bertoni

Giorgio Inghirami

Roberto Piva

Affiliations

Soon will be listed here.

Abstract

Anaplastic large-cell lymphoma (ALCL) is a clinical and biological heterogeneous disease that includes systemic anaplastic lymphoma kinase (ALK)-positive and ALK-negative entities. To discover biomarkers and/or genes involved in ALK-negative ALCL pathogenesis, we applied the cancer outlier profile analysis algorithm to a gene expression profiling data set including 249 cases of T-cell non-Hodgkin lymphoma and normal T cells. Ectopic coexpression of ERBB4 and COL29A1 genes was detected in 24% of ALK-negative ALCL patients. RNA sequencing and 5' RNA ligase-mediated rapid amplification of complementary DNA ends identified 2 novel ERBB4-truncated transcripts displaying intronic transcription start sites. By luciferase assays, we defined that the expression of ERBB4-aberrant transcripts is promoted by endogenous intronic long terminal repeats. ERBB4 expression was confirmed at the protein level by western blot analysis and immunohistochemistry. Lastly, we demonstrated that ERBB4-truncated forms show oncogenic potentials and that ERBB4 pharmacologic inhibition partially controls ALCL cell growth and disease progression in an ERBB4-positive patient-derived tumorgraft model. In conclusion, we identified a new subclass of ALK-negative ALCL characterized by aberrant expression of ERBB4-truncated transcripts carrying intronic 5' untranslated regions.

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