Emergence of BCR–ABL1 Fusion in AML Post–FLT3 Inhibitor-Based Therapy: A Potentially Targetable Mechanism of Resistance – A Case Series

Ahmad S. Alotaibi; Musa Yilmaz; Sanam Loghavi; Courtney DiNardo; Gautam Borthakur; Tapan M. Kadia; Beenu Thakral; Naveen Pemmaraju; Ghayas C. Issa; Marina Konopleva; Nicholas J. Short; Keyur Patel; Guilin Tang; Farhad Ravandi; Naval Daver

doi:10.3389/fonc.2020.588876

Emergence of BCR–ABL1 Fusion in AML Post–FLT3 Inhibitor-Based Therapy: A Potentially Targetable Mechanism of Resistance – A Case Series

Ahmad S. Alotaibi, Musa Yilmaz, Sanam Loghavi, Courtney DiNardo, Gautam Borthakur, Tapan M. Kadia, Beenu Thakral, Naveen Pemmaraju, Ghayas C. Issa, Marina Konopleva, Nicholas J. Short, Keyur Patel, Guilin Tang, Farhad Ravandi, Naval Daver

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12 Scopus citations

Abstract

Despite the promising result with FLT3 inhibitors in AML, the emergence of resistance poses a significant challenge, leading to a shorter response duration and inferior survival. This is frequently driven by on-target or parallel prosurvival mutations. The emergence of BCR–ABL1 as a mechanism of possible clonal evolution in relapsed AML has rarely been reported. Here we report our experience with three patients who had emergent BCR–ABL1 fusion at relapse after FLT3 inhibitors–based therapies. The first patient was refractory to multiple lines of therapies, including FLT3 inhibitors–based therapy. Patients 2 and 3 showed some response to combined FLT3-inhibitor and BCR–ABL targeted therapy (gilteritinib and ponatinib). The availability of effective targeted therapies for BCR–ABL1 makes this an important aberration to proactively identify and possibly target at relapse post–FLT3-inhibitor therapies.

Original language	English (US)
Article number	588876
Journal	Frontiers in Oncology
Volume	10
DOIs	https://doi.org/10.3389/fonc.2020.588876
State	Published - Oct 20 2020

Keywords

AML
BCR-ABL
FLT3
FLT3 inhibitors
secondary mutations

ASJC Scopus subject areas

Oncology
Cancer Research

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10.3389/fonc.2020.588876

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Alotaibi, A. S., Yilmaz, M., Loghavi, S., DiNardo, C., Borthakur, G., Kadia, T. M., Thakral, B., Pemmaraju, N., Issa, G. C., Konopleva, M., Short, N. J., Patel, K., Tang, G., Ravandi, F., & Daver, N. (2020). Emergence of BCR–ABL1 Fusion in AML Post–FLT3 Inhibitor-Based Therapy: A Potentially Targetable Mechanism of Resistance – A Case Series. Frontiers in Oncology, 10, Article 588876. https://doi.org/10.3389/fonc.2020.588876

Alotaibi, AS, Yilmaz, M , Loghavi, S , DiNardo, C , Borthakur, G , Kadia, TM , Thakral, B , Pemmaraju, N , Issa, GC, Konopleva, M, Short, NJ , Patel, K , Tang, G , Ravandi, F & Daver, N 2020, 'Emergence of BCR–ABL1 Fusion in AML Post–FLT3 Inhibitor-Based Therapy: A Potentially Targetable Mechanism of Resistance – A Case Series', Frontiers in Oncology, vol. 10, 588876. https://doi.org/10.3389/fonc.2020.588876

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abstract = "Despite the promising result with FLT3 inhibitors in AML, the emergence of resistance poses a significant challenge, leading to a shorter response duration and inferior survival. This is frequently driven by on-target or parallel prosurvival mutations. The emergence of BCR–ABL1 as a mechanism of possible clonal evolution in relapsed AML has rarely been reported. Here we report our experience with three patients who had emergent BCR–ABL1 fusion at relapse after FLT3 inhibitors–based therapies. The first patient was refractory to multiple lines of therapies, including FLT3 inhibitors–based therapy. Patients 2 and 3 showed some response to combined FLT3-inhibitor and BCR–ABL targeted therapy (gilteritinib and ponatinib). The availability of effective targeted therapies for BCR–ABL1 makes this an important aberration to proactively identify and possibly target at relapse post–FLT3-inhibitor therapies.",

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author = "Alotaibi, {Ahmad S.} and Musa Yilmaz and Sanam Loghavi and Courtney DiNardo and Gautam Borthakur and Kadia, {Tapan M.} and Beenu Thakral and Naveen Pemmaraju and Issa, {Ghayas C.} and Marina Konopleva and Short, {Nicholas J.} and Keyur Patel and Guilin Tang and Farhad Ravandi and Naval Daver",

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AU - Kadia, Tapan M.

AU - Thakral, Beenu

AU - Pemmaraju, Naveen

AU - Issa, Ghayas C.

AU - Konopleva, Marina

AU - Short, Nicholas J.

AU - Patel, Keyur

AU - Tang, Guilin

AU - Ravandi, Farhad

AU - Daver, Naval

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N2 - Despite the promising result with FLT3 inhibitors in AML, the emergence of resistance poses a significant challenge, leading to a shorter response duration and inferior survival. This is frequently driven by on-target or parallel prosurvival mutations. The emergence of BCR–ABL1 as a mechanism of possible clonal evolution in relapsed AML has rarely been reported. Here we report our experience with three patients who had emergent BCR–ABL1 fusion at relapse after FLT3 inhibitors–based therapies. The first patient was refractory to multiple lines of therapies, including FLT3 inhibitors–based therapy. Patients 2 and 3 showed some response to combined FLT3-inhibitor and BCR–ABL targeted therapy (gilteritinib and ponatinib). The availability of effective targeted therapies for BCR–ABL1 makes this an important aberration to proactively identify and possibly target at relapse post–FLT3-inhibitor therapies.

AB - Despite the promising result with FLT3 inhibitors in AML, the emergence of resistance poses a significant challenge, leading to a shorter response duration and inferior survival. This is frequently driven by on-target or parallel prosurvival mutations. The emergence of BCR–ABL1 as a mechanism of possible clonal evolution in relapsed AML has rarely been reported. Here we report our experience with three patients who had emergent BCR–ABL1 fusion at relapse after FLT3 inhibitors–based therapies. The first patient was refractory to multiple lines of therapies, including FLT3 inhibitors–based therapy. Patients 2 and 3 showed some response to combined FLT3-inhibitor and BCR–ABL targeted therapy (gilteritinib and ponatinib). The availability of effective targeted therapies for BCR–ABL1 makes this an important aberration to proactively identify and possibly target at relapse post–FLT3-inhibitor therapies.

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Emergence of BCR–ABL1 Fusion in AML Post–FLT3 Inhibitor-Based Therapy: A Potentially Targetable Mechanism of Resistance – A Case Series

Abstract

Keywords

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