An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia

BACKGROUND: Myelodysplastic syndrome (MDS) is rare in the pediatric age group and it may be associated with inheritable bone marrow failure (BMF) such as Fanconi anemia (FA). FA is a rare multi-system genetic disorder, characterized by congenital malformations and progressive BMF. Patients with FA u...

Descripción completa

Detalles Bibliográficos
Autores principales: Lovatel, Viviane Lamim, de Souza, Daiane Corrêa, Alvarenga, Tatiana Fonseca, Capela de Matos, Roberto R., Diniz, Claudia, Schramm, Marcia Trindade, Llerena Júnior, Juan Clinton, Silva, Maria Luiza Macedo, Abdelhay, Eliana, de Souza Fernandez, Teresa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2018
Materias:
Case Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6042331/
https://www.ncbi.nlm.nih.gov/pubmed/30008805
http://dx.doi.org/10.1186/s13039-018-0389-x
_version_ 1783339129305563136
author Lovatel, Viviane Lamim
de Souza, Daiane Corrêa
Alvarenga, Tatiana Fonseca
Capela de Matos, Roberto R.
Diniz, Claudia
Schramm, Marcia Trindade
Llerena Júnior, Juan Clinton
Silva, Maria Luiza Macedo
Abdelhay, Eliana
de Souza Fernandez, Teresa
author_facet Lovatel, Viviane Lamim
de Souza, Daiane Corrêa
Alvarenga, Tatiana Fonseca
Capela de Matos, Roberto R.
Diniz, Claudia
Schramm, Marcia Trindade
Llerena Júnior, Juan Clinton
Silva, Maria Luiza Macedo
Abdelhay, Eliana
de Souza Fernandez, Teresa
author_sort Lovatel, Viviane Lamim
collection PubMed
description BACKGROUND: Myelodysplastic syndrome (MDS) is rare in the pediatric age group and it may be associated with inheritable bone marrow failure (BMF) such as Fanconi anemia (FA). FA is a rare multi-system genetic disorder, characterized by congenital malformations and progressive BMF. Patients with FA usually present chromosomal aberrations when evolving to MDS or acute myeloid leukemia (AML). Thus, the cytogenetic studies in the bone marrow (BM) of these patients have an important role in the therapeutic decision, mainly in the indication for hematopoietic stem cell transplantation (HSCT). The most frequent chromosomal alterations in the BM of FA patients are gains of the chromosomal regions 1q and 3q, and partial or complete loss of chromosome 7. However, the significance and the predictive value of such clonal alterations, with respect to malignant progress, are not fully understood and data from molecular cytogenetic studies are very limited. CASE PRESENTATION: A five-year-old boy presented recurrent infections and persistent anemia. The BM biopsy revealed hypocellularity. G-banding was performed on BM cells and showed a normal karyotype. The physical examination showed to be characteristic of FA, being the diagnosis confirmed by DEB test. Five years later, even with supportive treatment, the patient presented severe hypocellularity and BM evolution revealing megakaryocyte dysplasia, intense dyserythropoiesis, and 11% myeloblasts. G-banded analysis showed an abnormal karyotype involving a der(9)t(9;11)(p24;q?22). The FISH analysis showed the monoallelic loss of ATM and KMT2A genes. At this moment the diagnosis was MDS, refractory anemia with excess of blasts (RAEB). Allogeneic HSCT was indicated early in the diagnosis, but no donor was found. Decitabine treatment was initiated and well tolerated, although progression to AML occurred 3 months later. Chemotherapy induction was initiated, but there was no response. The patient died due to disease progression and infection complications. CONCLUSIONS: Molecular cytogenetic analysis showed a yet unreported der(9)t(9;11)(p24;q?22),der(11)t(9;11)(p24;q?22) during the evolution from FA to MDS/AML. The FISH technique was important allowing the identification at the molecular level of the monoallelic deletion involving the KMT2A and ATM genes. Our results suggest that this chromosomal alteration conferred a poor prognosis, being associated with a rapid leukemic transformation and a poor treatment response.
format Online
Article
Text
id pubmed-6042331
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-60423312018-07-13 An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia Lovatel, Viviane Lamim de Souza, Daiane Corrêa Alvarenga, Tatiana Fonseca Capela de Matos, Roberto R. Diniz, Claudia Schramm, Marcia Trindade Llerena Júnior, Juan Clinton Silva, Maria Luiza Macedo Abdelhay, Eliana de Souza Fernandez, Teresa Mol Cytogenet Case Report BACKGROUND: Myelodysplastic syndrome (MDS) is rare in the pediatric age group and it may be associated with inheritable bone marrow failure (BMF) such as Fanconi anemia (FA). FA is a rare multi-system genetic disorder, characterized by congenital malformations and progressive BMF. Patients with FA usually present chromosomal aberrations when evolving to MDS or acute myeloid leukemia (AML). Thus, the cytogenetic studies in the bone marrow (BM) of these patients have an important role in the therapeutic decision, mainly in the indication for hematopoietic stem cell transplantation (HSCT). The most frequent chromosomal alterations in the BM of FA patients are gains of the chromosomal regions 1q and 3q, and partial or complete loss of chromosome 7. However, the significance and the predictive value of such clonal alterations, with respect to malignant progress, are not fully understood and data from molecular cytogenetic studies are very limited. CASE PRESENTATION: A five-year-old boy presented recurrent infections and persistent anemia. The BM biopsy revealed hypocellularity. G-banding was performed on BM cells and showed a normal karyotype. The physical examination showed to be characteristic of FA, being the diagnosis confirmed by DEB test. Five years later, even with supportive treatment, the patient presented severe hypocellularity and BM evolution revealing megakaryocyte dysplasia, intense dyserythropoiesis, and 11% myeloblasts. G-banded analysis showed an abnormal karyotype involving a der(9)t(9;11)(p24;q?22). The FISH analysis showed the monoallelic loss of ATM and KMT2A genes. At this moment the diagnosis was MDS, refractory anemia with excess of blasts (RAEB). Allogeneic HSCT was indicated early in the diagnosis, but no donor was found. Decitabine treatment was initiated and well tolerated, although progression to AML occurred 3 months later. Chemotherapy induction was initiated, but there was no response. The patient died due to disease progression and infection complications. CONCLUSIONS: Molecular cytogenetic analysis showed a yet unreported der(9)t(9;11)(p24;q?22),der(11)t(9;11)(p24;q?22) during the evolution from FA to MDS/AML. The FISH technique was important allowing the identification at the molecular level of the monoallelic deletion involving the KMT2A and ATM genes. Our results suggest that this chromosomal alteration conferred a poor prognosis, being associated with a rapid leukemic transformation and a poor treatment response. BioMed Central 2018-07-11 /pmc/articles/PMC6042331/ /pubmed/30008805 http://dx.doi.org/10.1186/s13039-018-0389-x Text en © The Author(s). 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Case Report
Lovatel, Viviane Lamim
de Souza, Daiane Corrêa
Alvarenga, Tatiana Fonseca
Capela de Matos, Roberto R.
Diniz, Claudia
Schramm, Marcia Trindade
Llerena Júnior, Juan Clinton
Silva, Maria Luiza Macedo
Abdelhay, Eliana
de Souza Fernandez, Teresa
An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia
title An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia
title_full An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia
title_fullStr An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia
title_full_unstemmed An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia
title_short An uncommon t(9;11)(p24;q22) with monoallelic loss of ATM and KMT2A genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from Fanconi anemia
title_sort uncommon t(9;11)(p24;q22) with monoallelic loss of atm and kmt2a genes in a child with myelodysplastic syndrome/acute myeloid leukemia who evolved from fanconi anemia
topic Case Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6042331/
https://www.ncbi.nlm.nih.gov/pubmed/30008805
http://dx.doi.org/10.1186/s13039-018-0389-x
work_keys_str_mv AT lovatelvivianelamim anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT desouzadaianecorrea anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT alvarengatatianafonseca anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT capeladematosrobertor anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT dinizclaudia anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT schrammmarciatrindade anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT llerenajuniorjuanclinton anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT silvamarialuizamacedo anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT abdelhayeliana anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT desouzafernandezteresa anuncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT lovatelvivianelamim uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT desouzadaianecorrea uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT alvarengatatianafonseca uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT capeladematosrobertor uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT dinizclaudia uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT schrammmarciatrindade uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT llerenajuniorjuanclinton uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT silvamarialuizamacedo uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT abdelhayeliana uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia
AT desouzafernandezteresa uncommont911p24q22withmonoalleliclossofatmandkmt2agenesinachildwithmyelodysplasticsyndromeacutemyeloidleukemiawhoevolvedfromfanconianemia

Ejemplares similares