Published online 19 May 2009
(Haematologica 2009, 10.3324/haematol.2008.000299)
Copyright © 2009 by Ferrata Storti Foundation
Miroslav Djokic1,* ,
Elisabet Björklund1 ,
Elisabeth Blennow2 ,
Joanna Mazur3 ,
Stefan Söderhäll4 ,
Anna Porwit1
(Haematologica 2009, 10.3324/haematol.2008.000299)
Copyright © 2009 by Ferrata Storti Foundation
Brief Reports |
Overexpression of CD123 correlates with the hyperdiploid genotype in acute lymphoblastic leukemia
1 Department of Pathology, Karolinska University Hospital, Stockholm
2 Department of Molecular Medicine, Karolinska Institute, Stockholm
3 Department of Child and Adolescent Health, Institute of Mother and Child, Warsaw, Poland
4 Children’s Cancer Research Unit at Astrid Lindgren Children’s Hospital, Karolinska University Hospital, Stockholm, Sweden
Correspondence: Miroslav Djokic, Department of Pathology, University of Pittsburgh Medical Center, 200 Lothrop Street, G316, Pittsburgh, PA, 15090, USA. E-mail:djokicm{at}upmc.edu
ABSTRACT
We evaluated CD123 expression in 95 pediatric and 24 adult ALL patients and compared the results with the CD123 expression in normal B-cell precursors. Early B-cell precursors were negative while intermediate precursors and mature B cells showed weak CD123 expression. Leukemic blasts in 31% of precursor-B ALL samples exhibited strong expression of CD123, 61% had moderate CD123 expression and 8% were negative; 81.5% of ALL with hyperdiploid karyotype (
52 chromosomes) showed strong CD123 overexpression. In contrast, cases with ETV6/RUNX1 rearrangement had weak CD123 expression. Our study suggests that overexpression of CD123 is an aberrant phenotype present in a subset of precursor-B ALL with hyperdiploid genotype, and represents an additional marker of good prognosis in pediatric precursor-B ALL. Moreover, aberrant CD123 expression in ALL is a good marker for monitoring of minimal residual disease.
Key words: overexpression, CD123, hyperdiploid genotype.