Introduction
T-cell acute lymphoblastic leukemia (ALL), which is
an aggressive hematological malignancy occurring as a consequence
of malignant transformation of T-cell progenitors, accounts for
~25% of all adult cases of ALL (1,2). Although
CD1a, CD2, CD3 (membranous as well as cytoplasmic), CD4, CD5, CD7
and CD8 are all T-cell antigens, cytoplasmic CD3 is considered as
an indicator of T-cell lineage (2).
In addition to T-cell markers, myeloid-associated antigens CD33,
CD117 (2–4), CD34 (2,5) and CD56
(6,7)
have been found to be expressed by blasts in T-cell ALL. However,
concomitant expression of all these markers in the same patient has
not been previously reported.
We herein present a case of T-cell ALL exhibiting
aberrant expression of CD34, CD56, CD33 and CD117, in addition to
T-cell markers, which did not respond to induction treatment.
Case report
A 55-year-old woman was admitted to our hospital
with a sore throat unresponsive to medication for 1 month. On
physical examination, the tonsils and oropharynx were found to be
hyperemic, without any other remarkable findings. The laboratory
tests revealed a hemoglobin level of 9.1 g/dl, platelet count of
1.95×109/l, leukocyte count of 1.97×109/l and lactate dehydrogenase
level of 205 U/l. The peripheral blood smear examination revealed
blast cells. Bone marrow biopsy and aspiration were performed. The
bone marrow aspiration showed hand mirror-shaped blast cells
(Fig. 1). On conventional cytogenetic
study, there was no metaphase for assessment. On flow cytometric
analysis, the blast cells were found to be positive for cytoplasmic
CD3, CD2, CD5, CD7, CD34, CD56, CD33 and CD117, whereas they were
negative for myeloperoxidase, CD13, CD11b, CD15, CD19, CD79a, CD22
and CD10 (Fig. 2). The patient was
diagnosed with T-cell ALL according to the World Health
Organisation 2008 criteria (8), and
was administered cyclophosphamide, vincristine, adriamycin and
dexamethasone (hyper-CVAD 1A) therapy. After the first cycle of
treatment, bone marrow aspiration revealed 10% blast cells.
Therefore, methotrexate and cytarabine (hyper-CVAD 1B) treatment
was initiated. On the 18th day of therapy, the patient deteriorated
clinically and subsequently developed septic shock. The patient was
intubated and admitted to the intensive care unit; however, she
succumbed to the disease on day 20 of the hyper-CVAD 1B
treatment.
Discussion
Although T-cell ALL develops due to malignant
transformation of T-cell progenitors, aberrant myeloid marker
expression on blast cells, particularly of CD13, CD33 and rarely
CD117, has been previously described (2–4). In
myeloid antigen-expressing T-cell ALL patients, the frequency of
CD34 expression, a transmembrane glycoprotein that is expressed on
hematopoietic stem cells and early thymic T-cell precursors
(9), was also found to be increased
(5). There is an ongoing debate
regarding the clinical relevance of myeloid marker expression in
T-cell ALL and whether their expression is a predictor of poor
outcome (3–5,10,11). Furthermore, the effect of CD34
expression on clinical outcome in T-cell ALL is controversial
(9,10)
and remains to be elucidated.
Another surface antigen associated with poor
prognosis in T-cell ALL is the CD56 (also referred to as neural
cell adhesion molecule) surface antigen. CD56 is a marker for
natural killer (NK) cells, but is also expressed in neoplastic
myeloid, lymphoid, plasmacytoid dendritic and myeloma cells, as
well as in a minority of T cells (7).
Co-expression of myeloid markers together with CD34 and CD56 in
T-cell ALL is seen more frequently (6,7). To the
best of our knowledge, this is the first report of aberrant
co-expression of the NK cell marker CD56, the myeloid cell markers
CD117 and CD33 and the stem cell marker CD34 in a patient with
T-cell ALL. This appears to be associated with an unfavorable
outcome, despite the use of intensive chemotherapy.
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