Zinc finger protein 384 ( <i>ZNF384</i> ) impact on childhood mixed phenotype acute leukemia and B-cell precursor acute lymphoblastic leukemia
Tuğçe Sudutan, Yücel Erbilgin, Özden Hatırnaz Ng, Serap Karaman, Zeynep Karakaş, Fulya KÜÇÜKCANKURT, Tiraje Çelkan, Çetin Timur, Nihal Özdemir, Sadan Hacısalihoglu, Sema Aylan Gelen, Müge Sayitoğlu
Abstract
B-cell precursor acute lymphoblastic leukemia (BCP-ALL) is a heterogeneous malignancy and consists of several genetic abnormalities. Some of these abnormalities are used in clinics for risk calculation and treatment decisions. Patients with ZNF384 rearrangements had a distinct expression profile regardless of their diagnosis, BCP-ALL or mixed phenotype acute leukemia (MPAL) and defined as a new subtype of ALL. In this study, we screened 42 MPAL and 91 BCP-ALL patients for the most common ZNF384 fusions; ZNF384::TCF3, ZNF384::EP300 and ZNF384::TAF15 by using PCR. We identified ZNF384 fusions in 9.5% of MPAL and 7.6% of BCP-ALL. A novel breakpoint was identified in ZNF384::TCF3 fusion in one BCP-ALL patient. T-myeloid MPAL patients showed significantly lower ZNF384 expression compared to lymphoid groups. Patients with ZNF384r had intermediate survival rates based on other subtypes. Prognostic and patient-specific treatment evaluation of ZNF384 fusions in both ALL and MPAL might help to improve risk characterization of patients.