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Am J Clin Pathol. 1999
Apr;111(4):467-76.
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Acute lymphoblastic leukemia.
Survey of immunophenotype,
French-American-British classification,
frequency of myeloid antigen expression, and
karyotypic abnormalities in 210 pediatric
and adult cases.
Khalidi HS, Chang KL, Medeiros LJ,
Brynes RK, Slovak ML, Murata-Collins JL,
Arber DA.
Division of
Pathology, City of Hope National Medical
Center, Duarte, California 91010, USA.
Immunophenotypic studies
are essential to distinguish acute
lymphoblastic leukemia (ALL) from minimally
differentiated acute myeloid leukemia
(AMLM0) and to classify ALL into immunologic
subtypes. Frequently, immunophenotyping
identifies myeloid antigen expression in
ALL, causing a potential diagnostic problem.
To evaluate the immunophenotype of ALL, we
studied 210 cases of pediatric and adult ALL
by flow cytometry and compared the results
with the French-American-British (FAB)
Cooperative Group classification and the
karyotypic findings. Myeloid-associated
antigens were expressed in 78 (45.6%) of
precursor B-cell ALL cases. Pediatric
precursor B ALLs had a higher frequency of
myeloid antigen expression than did adult
cases. All mature B-cell ALL cases were
negative for TdT and myeloid antigens.
Myeloid antigen expression was less frequent
in T-cell ALL cases compared with precursor
B-cell ALL cases. Of the 192 cases submitted
for cytogenetic analysis, 147 were abnormal.
The most common chromosomal translocation
was the Philadelphia chromosome, which was
more likely to have L2 blast morphology and
a precursor B immunophenotype. Myeloid
antigen expression was present in 70.8% of
Ph-positive cases (P = .008). Chromosome
rearrangements involving 11q23 also showed
an increased frequency of myeloid antigen
expression. Chromosome translocations
involving regions of T-cell receptor genes
were present in 24% of T-cell ALL cases. A
high percentage of ALL cases, however, had
various other cytogenetic abnormalities,
many of which involved less well-studied
chromosomal regions.
PMID: 10191766 [PubMed -
indexed for MEDLINE]