An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature

BRAF protein is a serine/threonine kinase with 766 amino acids. Approximately 15% of human cancers harbor BRAF mutations as well as other BRAF anomalies (amplifications, fusions). Somatic mutations mainly occur in the catalytic kinase domain (CR3), and the predominant mutation is p.V600E which is th...

Descripción completa

Detalles Bibliográficos
Autores principales: Ghorbani-Aghbolaghi, Amir, Lechpammer, Mirna, Ali, Saba F., Ku, Nam K., Dwyre, Denis M., Rashidi, Hooman H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: São Paulo, SP: Universidade de São Paulo, Hospital Universitário 2017
Materias:
Article / Clinical Case Report
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5634429/
https://www.ncbi.nlm.nih.gov/pubmed/29043205
http://dx.doi.org/10.4322/acr.2017.032
_version_ 1783270088804139008
author Ghorbani-Aghbolaghi, Amir
Lechpammer, Mirna
Ali, Saba F.
Ku, Nam K.
Dwyre, Denis M.
Rashidi, Hooman H.
author_facet Ghorbani-Aghbolaghi, Amir
Lechpammer, Mirna
Ali, Saba F.
Ku, Nam K.
Dwyre, Denis M.
Rashidi, Hooman H.
author_sort Ghorbani-Aghbolaghi, Amir
collection PubMed
description BRAF protein is a serine/threonine kinase with 766 amino acids. Approximately 15% of human cancers harbor BRAF mutations as well as other BRAF anomalies (amplifications, fusions). Somatic mutations mainly occur in the catalytic kinase domain (CR3), and the predominant mutation is p.V600E which is the substitution of glutamic acid (E) for valine (V) as result of a mutation at codon 600 of the kinase domain. To our knowledge, the vast majority of the cancers have non-germline BRAF mutations. Here we describe a case of a 60-year-old female with a history of hairy cell leukemia (HCL) who presented with aphasia and forgetfulness. A follow-up Brain CT scan showed three distinct brain lesions which were found to be diagnostic of melanoma (confirmed by immunohistochemistry) with no evidence of a concurrent brain involvement by a B-cell neoplasm. Molecular studies confirmed the same BRAF p.V600E mutation in both malignancies (hairy cell leukemia and melanoma). Thereafter the patient was started on BRAF inhibitor treatment and is now symptom-free after one year of follow up. Having two concurrent malignancies with a shared BRAF mutation is extremely rare and makes this an excellent example of a genomic marker-driven treatment in two histologically and immunophenotypically distinct tumors.
format Online
Article
Text
id pubmed-5634429
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher São Paulo, SP: Universidade de São Paulo, Hospital Universitário
record_format MEDLINE/PubMed
spelling pubmed-56344292017-10-17 An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature Ghorbani-Aghbolaghi, Amir Lechpammer, Mirna Ali, Saba F. Ku, Nam K. Dwyre, Denis M. Rashidi, Hooman H. Autops Case Rep Article / Clinical Case Report BRAF protein is a serine/threonine kinase with 766 amino acids. Approximately 15% of human cancers harbor BRAF mutations as well as other BRAF anomalies (amplifications, fusions). Somatic mutations mainly occur in the catalytic kinase domain (CR3), and the predominant mutation is p.V600E which is the substitution of glutamic acid (E) for valine (V) as result of a mutation at codon 600 of the kinase domain. To our knowledge, the vast majority of the cancers have non-germline BRAF mutations. Here we describe a case of a 60-year-old female with a history of hairy cell leukemia (HCL) who presented with aphasia and forgetfulness. A follow-up Brain CT scan showed three distinct brain lesions which were found to be diagnostic of melanoma (confirmed by immunohistochemistry) with no evidence of a concurrent brain involvement by a B-cell neoplasm. Molecular studies confirmed the same BRAF p.V600E mutation in both malignancies (hairy cell leukemia and melanoma). Thereafter the patient was started on BRAF inhibitor treatment and is now symptom-free after one year of follow up. Having two concurrent malignancies with a shared BRAF mutation is extremely rare and makes this an excellent example of a genomic marker-driven treatment in two histologically and immunophenotypically distinct tumors. São Paulo, SP: Universidade de São Paulo, Hospital Universitário 2017-09-30 /pmc/articles/PMC5634429/ /pubmed/29043205 http://dx.doi.org/10.4322/acr.2017.032 Text en Autopsy and Case Reports. ISSN 2236-1960. Copyright © 2017. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium provided the article is properly cited.
spellingShingle Article / Clinical Case Report
Ghorbani-Aghbolaghi, Amir
Lechpammer, Mirna
Ali, Saba F.
Ku, Nam K.
Dwyre, Denis M.
Rashidi, Hooman H.
An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature
title An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature
title_full An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature
title_fullStr An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature
title_full_unstemmed An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature
title_short An extremely rare case of concurrent BRAF V600E mutation driven hairy cell leukemia and melanoma: case report and review of literature
title_sort extremely rare case of concurrent braf v600e mutation driven hairy cell leukemia and melanoma: case report and review of literature
topic Article / Clinical Case Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5634429/
https://www.ncbi.nlm.nih.gov/pubmed/29043205
http://dx.doi.org/10.4322/acr.2017.032
work_keys_str_mv AT ghorbaniaghbolaghiamir anextremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT lechpammermirna anextremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT alisabaf anextremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT kunamk anextremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT dwyredenism anextremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT rashidihoomanh anextremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT ghorbaniaghbolaghiamir extremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT lechpammermirna extremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT alisabaf extremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT kunamk extremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT dwyredenism extremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature
AT rashidihoomanh extremelyrarecaseofconcurrentbrafv600emutationdrivenhairycellleukemiaandmelanomacasereportandreviewofliterature

Ejemplares similares