Acute Myeloid Leukemia: Novel Therapy, excluding Transplantation
Oral and Poster Abstracts
616. Acute Myeloid Leukemia: Novel Therapy, excluding Transplantation: Poster I
Hall A, Level 2
(Orange County Convention Center)
Giulia Daniele1*, Clelia Tiziana Storlazzi1*, Cristina Papayannidis, MD, PhD2, Ilaria Iacobucci, PhD3*, Angelo Lonoce1*, Margherita Perricone4*, Mariana Lomiento5*, Fabiana Mammoli5*, Elena Marasco6*, Vilma Mantovani6*, Hilmar Quentmeier, PhD7*, Giorgia Simonetti, PhD8*, Antonella Padella8*, Vincenzo Franza9*, Hans G. Drexler, MD, PhD7, Jie Ding, PhD7*, Orazio Palumbo10*, Massimo Carella10*, Niroshan Nadarajah, M.Sc.11*, Renč Massimiliano Marsano1*, Antonio Palazzo1*, Emanuela Ottaviani8*, Carmen Baldazzi, PhD8*, Nicoletta Testoni8*, Sergio Ferrari, MD, PhD5* and Giovanni Martinelli, MD, PhD2
1Department of Biology, University of Bari, Bari, Italy
2Bologna University School of Medicine, Bologna, Italy
3"Serągnoli" Institute of Hematology, University of Bologna, Bologna, Italy
4Institute of Hematology, Bologna, Italy
5Department of Life Science, University of Modena and Reggio Emilia, Modena, Italy
6Center for Applied Biomedical Research (CRBA), Bologna, Italy
7DSMZ, Braunschweig, Germany
8University of Bologna, Bologna, Italy
9Institute of Hematology "Seragnoli", University of Bologna, Bologna, Italy
10Medical Genetics Unit, IRCCS, San Giovanni Rotondo, Italy
11MLL Munich Leukemia Laboratory, Munich, Germany
We describe a new AML entity, occurring in 30% of de novo acute myeloid leukemia, due to structural and epigenetic deregulation of the
UNCX homeobox (HB) gene. By molecular approaches, we identified a M5 AML patient with a t(7;10)(p22;p14) translocation as the sole cytogenetic anomaly and showing ectopic expression of
UNCX (7p22.3), which encode for a transcription factor involved in somitogenesis and neurogenesis. Since
UNCX was never reported in association with cancer but only with common myeloid cell proliferation and regulation of cell differentiation, we decided to investigate its contribution to leukemogenesis. We observed
UNCX ectopic expression in 32.3% (20/62) and in 8% (6/75) of acute myeloid leukemia (AML) patients and cell lines, respectively. Notably, retroviral-mediated
UNCX transfer in CD34+ HSCs induced a slow-down in their proliferation and differentiation and transduced cells showed a lower growth rate but a higher percentage of CD34+ stem cells in liquid culture than controls. Additionally,
UNCX infected cells displayed a decrease of
MAP2K1 proliferation marker but increase of
KLF4, HOXA10, and
CCNA1, associated with impaired differentiation and pluripotency. Similarly,
UNCX-positive patients revealed alteration of gene pathways involved in proliferation, cell cycle control and hematopoiesis. Since HB genes encode for transcription factors showing a crucial role in normal hematopoiesis and in leukemogenesis, we focused our attention on the role of altered
UNCX expression level. Of note, its murine ortholog, (
Uncx) was previously described as embedded within a low-methylated regions (≤ 10%) called “canyon” and dysregulated in murine hematopoietic stem cells (HSCs) as a consequence of altered methylation at canyons edges (borders) due to
Dnmt3a inactivation. In our hands,
UNCX activation was accompanied by methylation changes at both its canyon borders, clearly indicating an epigenetic regulation of this gene, although not induced by
DNMT3A mutations.
Clinical parameters and correlation with response to therapy will be presented.
Taken together, our results indicate that more than 30% of de novo AML have a novel entity with a putative leukemogenic role of UNCX, whose activation may be ascribed to epigenetic regulators.
Acknowledgments: MG, CP, GS, and AP(2) and this work was supported by ELN, AIL, AIRC, progetto Regione-Università 2010-12 (L. Bolondi), Fondazione del Monte di Bologna e Ravenna, FP7 NGS-PTL project. CTS, GD and AL are supported by Associazione Italiana Ricerca sul Cancro (AIRC) funding.
Disclosures: Nadarajah: MLL Munich Leukemia Laboratory:
Employment
. Martinelli: MSD:
Consultancy
; Novartis:
Consultancy
,
Speakers Bureau
; Ariad:
Consultancy
; BMS:
Consultancy
,
Speakers Bureau
; Pfizer:
Consultancy
; AMGEN:
Consultancy
; ROCHE:
Consultancy
.
*signifies non-member of ASH