t(17;21)(q11.2;q22) as a sole aberration in acute myelomonocytic leukemia

Helena Podgornik, Peter Cernelc Affiliation

University medical center Ljubljana, Department of Haematology, Zaloska 7, 1000 Ljubljana, Slovenia

Previous history

Preleukaemia

Malignant disease

Inborn condition

Clinics case report

Age

87 yrs

Sex

Liver

Spleen

Lymph nodes

Cns involv

Blood data

Wbc

30,6

Platelets

Blasts

Bone marrow

28 of blasts) (Hypercellular; 28% of blasts; 20% of monocytic lineage, dispoiesis in megakariocytic lineage and diserithropoiesis

Cyto path

Cytology

Acute myelomonocytic leukemia

Immunophenotype

CD4-/CD11c+/CD13+/CD14+/CD15+/CD33+/CD34+↓/CD45+/ CD64+/CD65+/MPO+↓

Rearranged ig tcr

Pathology

Not done

Electron microscopy

Not done

Precise diagnosis

Acute myelomonocytic leukemia

Survival data

Date diagnosis

04-2011

Treatment

Symptomatic (antibiotics)

Complete remission

Treatment relat death

Relapse

Status

Date last follow

04-2011

Survival

Karyotype

Sample

Bone marrow

Culture time

Banding

GTG

Results

46,XY,t(17;21)(q11.2;q22)[19]/46,XY[1]

Mol cytogenet technics

FISH; LSI RUNX1/RUNX1T1, LSI MLL (Abbott); WC 17, 21 (Kreatech)

Mol cytogenet results

nuc ish(RUNX1T1x2,RUNX1x3)[130/200]; ish t(17;21)(WCP17+,WCP21+;WCP17+,WCP21+)

Other molec studies

Technics

PCR

Results

FLT3-ITD - negative; NPM1 mutation - negative.

Images

Figure 1. Partial Karyograme with a balanced translocation t(17;21)(q11.2;q22).

Figure 2. GTG banded metaphase chromosomes.

Figure 3. FISH on previously GTG banded chromosomes (Fig. 2). WC 17 (aqua) and WC 21 (red) (Kreatech).

Figure 4. Metaphase FISH by LSI AML1(RUNX1)/ETO(RUNX1T1) DNA probe (Abbott) with split signal for RUNX1 (green). On GTG banded metaphase normal 21 with the strong RUNX1 signal and both derivatives with split RUNX1 signals are indicated.

Comments section

Comments

We report the first case of t(17;21)(q11.2;q22) as the sole anomaly in AML. This rare recurrent abnormality has been linked to treatment related leukemia or MDS although it has been also found in de novo leukemia (Roulston et al., 1998; Nadal et al., 2008). Our patient had no previous history of cancer or preleukemia. Cytomorphology of bone marrow cells was, however consistent with dysplastic changes typical for s-AML. FISH analysis with probe specific for RUNX1 has been done in two previous cases with t(17;21)(q11.2;q22). While in one patient RUNX1 has been lost (Nadal et al., 2008) our result corresponds to the case of Roulston et al. (Roulston et al., 1998) where signals from RUNX1 were split by the translocation. Due to his age and poor physical condition our patient was not treated by intensive chemotherapy and he died within a month from diagnosis.

Article Bibliography

Pubmed ID	Last Year	Title	Authors

Citation

Helena Podgornik, Peter Cernelc

t(17;21)(q11.2;q22) as a sole aberration in acute myelomonocytic leukemia

Atlas Genet Cytogenet Oncol Haematol. 2012-02-01

Online version: http://atlasgeneticsoncology.org/case-report/208861/js/css/favicon/favicon-32x32.png