Translocation t(X;20)(q13;q13.3) as a secondary chromosome abnormality in a patient with 5q-: a case report

Carlos Augusto Figueiredo Correia, Juliana Lino Rodrigues de Matos, Cristina Alonso Ratis, Silvia Helena A Figueira, Renata Kiyomi Kishimoto, Elvira D Rodrigues Pereira Velloso Affiliation

Laboratorio de Tecnicas Especiais- Citogenetica do Hospital Israelita Albert Einstein, Sao Paulo, Brazil (CAFC, CAR, SHAF, RKK, EDRPV); Hospital das Clinicas da Universidade Federal de Minas Gerais, Minas Gerais, Brazil (CAFC); Hemomed, Sao Paulo, Brazil (JLRdM)

Previous history

Preleukaemia

+ Low risk myelodysplastic syndrome (refractory anemia) diagnosed 32 months before (December, 2009).

Malignant disease

Inborn condition

Clinics case report

Age

76 yrs

Sex

Liver

Spleen

Lymph nodes

Cns involv

Blood data

Wbc

2.7

8.5

Platelets

146

Blasts

Bone marrow

5 Global normocellularity, with erythroid and megakaryocytic hyperplasia and megakaryocytic dysplasia (no-lobated megakaryocytes suggestive of 5q- Syndrome), less than 5% of myeloblasts and 23% of ring sideroblasts.

Cyto path

Cytology

Myelodysplastic Syndrome - Refractory anemia with ring sideroblasts (FAB classification).

Precise diagnosis

Myelodysplastic Syndrome - Refractory citopenia with multilineage dysplasia and ringed sideroblasts (WHO classification).

Survival data

Date diagnosis

08-2012

Treatment

Erythropoietin

Complete remission

Treatment relat death

Relapse

Status

Date last follow

09-2012

Survival

1 month from the cytogenetic abnormality detection, 30 months from the MDS diagnosis.

Karyotype

Sample

Bone marrow

Culture time

24 and 48 hours without stimulating agents

Banding

GTG

Results

46,XX,del(5)(q13q31)[1]/46,X,t(X;20)(q13;q13.3),del(5(q13q31))[11]/46,XX[8]

Karyotype relapse

not done

Images

Partial G-banded karyotypes showing the del(5)(q13q31) and the t(X;20)(q13;q13.3)

Comments section

Comments

The band Xq13 is frequently involved in rearrangements seen in hematological malignancy. The structural rearrangement idic(X)(q13) is associate with the myelodysplastic syndrome with ringed sideroblasts and this region is difficult for mapping because is rich in complex repeats with subregional inversions and high concentration of LINE repeats (boosters of X-inactivation). The chromosome 20q interstitial deletions are well established nonrandom abnormalities in myeloid disorders, particularly in polycythemia vera and myelodysplasia. Very few cases of translocations involving chromosome 20 have been reported in hematological malignancy. The band 20q13 is rich in cancer genes and translocation involving this region has been reported in cases of acute myeloid leukemia. One study shows that breakpoints of X chromosomes associated with myelodysplasia were located in a region of 450 kb next to the gene XIST (Xq13). Another study demonstrated that a critical event in myelodysplasia is loss of tumor suppressor genes present on the long arm of chromosome 20. This suppression can occur when a potential cryptic deletion is associated with a translocation. This phenomenon generates a second mechanism causing inactivation of the X chromosome and derivative 20 resulting loss of function of tumor suppressor genes. Seven cases of t(X;20)(q13;q13) were described in literature; all affecting women over the age of 57 with myeloid disorders. We report the detection, by conventional cytogenetic methods, the t(X;20)(q13;q13.3) in one female patient with myelodysplastic syndrome subtype Refractory citopenia with multilineage dysplasia and ringed sideroblasts (classification WHO). Although this translocation was described as a primary clonal chromosome abnormality, in this case the t(X;20) seems to be a secondary chromosome abnormality following a deletion 5q.

Bibliography

Pubmed ID	Last Year	Title	Authors
7053756	1982	Three patients with structurally abnormal X chromosomes, each with Xq13 breakpoints and a history of idiopathic acquired sideroblastic anemia.	Dewald GW et al
2790752	1989	Twenty-six patients with hematologic disorders and X chromosome abnormalities. Frequent idic(X)(q13) chromosomes and Xq13 anomalies associated with pathologic ringed sideroblasts.	Dewald GW et al
8241509	1993	Molecular genetics of myeloid leukemia: identification of the commonly deleted segment of chromosome 20.	Roulston D et al
7627929	1995	Characterization by chromosome painting of balanced and unbalanced X chromosome translocations in myelodysplastic syndromes.	Michaux L et al
10756090	2000	Characterization of a highly complex region in Xq13 and mapping of three isodicentric breakpoints associated with preleukemia.	McDonell N et al
15771910	2005	Translocation (X;20) involving the inactive X chromosome in a patient with myeloproliferative disorder.	O'Reilly J et al
15676151	2005	Translocation (X;20)(q13;q13.3): a nonrandom abnormality in four patients with myeloid disorders.	Reddy KS et al

Citation

Carlos Augusto Figueiredo Correia, Juliana Lino Rodrigues de Matos, Cristina Alonso Ratis, Silvia Helena A Figueira, Renata Kiyomi Kishimoto, Elvira D Rodrigues Pereira Velloso

Translocation t(X;20)(q13;q13.3) as a secondary chromosome abnormality in a patient with 5q-: a case report

Atlas Genet Cytogenet Oncol Haematol. 2013-01-01

Online version: http://atlasgeneticsoncology.org/case-report/208864/translocation-t(x;20)(q13;q13-3)-as-a-secondary-chromosome-abnormality-in-a-patient-with-5q-a-case-report