Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature

Novel targeted therapies improve the survival of specific subgroups (defined by genetic variants) of patients with acute myeloid leukemia (AML), validating the paradigm of molecularly targeted therapy. However, identifying correlations between AML molecular attributes and effective therapies is chal...

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Autores principales: Tavor, Sigal, Shalit, Tali, Ilani, Noa Chapal, Moskovitz, Yoni, Livnat, Nir, Groner, Yoram, Barr, Haim, Minden, Mark D., Plotnikov, Alexander, Deininger, Michael W., Kaushansky, Nathali, Shlush, Liran I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Fondazione Ferrata Storti 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7726833/
https://www.ncbi.nlm.nih.gov/pubmed/33256378
http://dx.doi.org/10.3324/haematol.2019.240705
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author Tavor, Sigal
Shalit, Tali
Ilani, Noa Chapal
Moskovitz, Yoni
Livnat, Nir
Groner, Yoram
Barr, Haim
Minden, Mark D.
Plotnikov, Alexander
Deininger, Michael W.
Kaushansky, Nathali
Shlush, Liran I.
author_facet Tavor, Sigal
Shalit, Tali
Ilani, Noa Chapal
Moskovitz, Yoni
Livnat, Nir
Groner, Yoram
Barr, Haim
Minden, Mark D.
Plotnikov, Alexander
Deininger, Michael W.
Kaushansky, Nathali
Shlush, Liran I.
author_sort Tavor, Sigal
collection PubMed
description Novel targeted therapies improve the survival of specific subgroups (defined by genetic variants) of patients with acute myeloid leukemia (AML), validating the paradigm of molecularly targeted therapy. However, identifying correlations between AML molecular attributes and effective therapies is challenging. Recent advances in highthroughput, in vitro drug sensitivity screening applied to primary AML blasts were used to uncover such correlations; however, these methods cannot predict the response of leukemic stem cells. Our study aimed to predict in vitro response to targeted therapies, based on molecular markers, with subsequent validation in leukemic stem cells. We performed ex vivo screening of sensitivity to 46 drugs on 29 primary AML samples at diagnosis or relapse. Using unsupervised hierarchical clustering analysis we identified a group with sensitivity to several tyrosine kinase inhibitors, including the multi-tyrosine kinase inhibitor, dasatinib, and searched for correlations between the response to dasatinib, exome sequencing and gene expression in our dataset and in the Beat AML dataset. Unsupervised hierarchical clustering analysis of gene expression resulted in clustering of dasatinib responders and non-responders. In vitro response to dasatinib could be predicted based on gene expression (area under the curve=0.78). Furthermore, mutations in FLT3/ITD and PTPN11 were enriched in the dasatinib-sensitive samples as opposed to mutations in TP53 which were enriched in resistant samples. Based on these results, we selected FLT3/ITD AML samples and injected them into NSG-SGM3 mice. Our results demonstrate that in a subgroup of FLT3/ITD AML (4 out of 9) dasatinib significantly inhibited leukemic stem cell engraftment. In summary we show that dasatinib has an anti-leukemic effect both on bulk blasts and, more importantly, on leukemic stem cells from a subset of AML patients that can be identified based on mutational and expression profiles. Our data provide a rational basis for clinical trials of dasatinib in a molecularly selected subset of AML patients.
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spelling pubmed-77268332020-12-11 Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature Tavor, Sigal Shalit, Tali Ilani, Noa Chapal Moskovitz, Yoni Livnat, Nir Groner, Yoram Barr, Haim Minden, Mark D. Plotnikov, Alexander Deininger, Michael W. Kaushansky, Nathali Shlush, Liran I. Haematologica Article Novel targeted therapies improve the survival of specific subgroups (defined by genetic variants) of patients with acute myeloid leukemia (AML), validating the paradigm of molecularly targeted therapy. However, identifying correlations between AML molecular attributes and effective therapies is challenging. Recent advances in highthroughput, in vitro drug sensitivity screening applied to primary AML blasts were used to uncover such correlations; however, these methods cannot predict the response of leukemic stem cells. Our study aimed to predict in vitro response to targeted therapies, based on molecular markers, with subsequent validation in leukemic stem cells. We performed ex vivo screening of sensitivity to 46 drugs on 29 primary AML samples at diagnosis or relapse. Using unsupervised hierarchical clustering analysis we identified a group with sensitivity to several tyrosine kinase inhibitors, including the multi-tyrosine kinase inhibitor, dasatinib, and searched for correlations between the response to dasatinib, exome sequencing and gene expression in our dataset and in the Beat AML dataset. Unsupervised hierarchical clustering analysis of gene expression resulted in clustering of dasatinib responders and non-responders. In vitro response to dasatinib could be predicted based on gene expression (area under the curve=0.78). Furthermore, mutations in FLT3/ITD and PTPN11 were enriched in the dasatinib-sensitive samples as opposed to mutations in TP53 which were enriched in resistant samples. Based on these results, we selected FLT3/ITD AML samples and injected them into NSG-SGM3 mice. Our results demonstrate that in a subgroup of FLT3/ITD AML (4 out of 9) dasatinib significantly inhibited leukemic stem cell engraftment. In summary we show that dasatinib has an anti-leukemic effect both on bulk blasts and, more importantly, on leukemic stem cells from a subset of AML patients that can be identified based on mutational and expression profiles. Our data provide a rational basis for clinical trials of dasatinib in a molecularly selected subset of AML patients. Fondazione Ferrata Storti 2020-05-21 /pmc/articles/PMC7726833/ /pubmed/33256378 http://dx.doi.org/10.3324/haematol.2019.240705 Text en Copyright© 2020 Ferrata Storti Foundation http://creativecommons.org/licenses/by-nc/4.0/ This article is distributed under the terms of the Creative Commons Attribution Noncommercial License (by-nc 4.0) which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
spellingShingle Article
Tavor, Sigal
Shalit, Tali
Ilani, Noa Chapal
Moskovitz, Yoni
Livnat, Nir
Groner, Yoram
Barr, Haim
Minden, Mark D.
Plotnikov, Alexander
Deininger, Michael W.
Kaushansky, Nathali
Shlush, Liran I.
Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature
title Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature
title_full Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature
title_fullStr Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature
title_full_unstemmed Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature
title_short Dasatinib response in acute myeloid leukemia is correlated with FLT3/ITD, PTPN11 mutations and a unique gene expression signature
title_sort dasatinib response in acute myeloid leukemia is correlated with flt3/itd, ptpn11 mutations and a unique gene expression signature
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7726833/
https://www.ncbi.nlm.nih.gov/pubmed/33256378
http://dx.doi.org/10.3324/haematol.2019.240705
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