• BCR::ABL1 M244V confers clinical resistance to asciminib; M244V and other kinase N-lobe mutations confer resistance to asciminib in vitro.

  • Mutations in the BCR::ABL1 kinase domain may impair the durability of response to combinations of asciminib and ATP-competitive TKIs.

Subjects:
Brief Reports, Clinical Trials and Observations, Myeloid Neoplasia
Abstract

Secondary kinase domain mutations in BCR::ABL1 represent the most common cause of resistance to tyrosine kinase inhibitor (TKI) therapy in patients with chronic myeloid leukemia. The first 5 approved BCR::ABL1 TKIs target the adenosine triphosphate (ATP)–binding pocket. Mutations confer resistance to these ATP-competitive TKIs and those approved for other malignancies by decreasing TKI affinity and/or increasing ATP affinity. Asciminib, the first highly active allosteric TKI approved for any malignancy, targets an allosteric regulatory pocket in the BCR::ABL1 kinase C-lobe. As a non–ATP-competitive inhibitor, the activity of asciminib is predicted to be impervious to increases in ATP affinity. Here, we report several known mutations that confer resistance to ATP-competitive TKIs in the BCR::ABL1 kinase N-lobe that are distant from the asciminib binding pocket yet unexpectedly confer in vitro resistance to asciminib. Among these is BCR::ABL1 M244V, which confers clinical resistance even to escalated asciminib doses. We demonstrate that BCR::ABL1 M244V does not impair asciminib binding, thereby invoking a novel mechanism of resistance. Molecular dynamic simulations of the M244V substitution implicate stabilization of an active kinase conformation through impact on the α-C helix as a mechanism of resistance. These N-lobe mutations may compromise the clinical activity of ongoing combination studies of asciminib with ATP-competitive TKIs.

Subjects:
Brief Reports, Clinical Trials and Observations, Myeloid Neoplasia
1.
Hochhaus
A
,
Larson
RA
,
Guilhot
F
, et al.
Long-term outcomes of imatinib treatment for chronic myeloid leukemia
.
N Engl J Med
.
2017
;
376
(
10
):
917
-
927
.
Google Scholar
Crossref
Search ADS
 
2.
Pan
Y
,
Mader
MM
.
Principles of kinase allosteric inhibition and pocket validation
.
J Med Chem
.
2022
;
65
(
7
):
5288
-
5299
.
Google Scholar
Crossref
Search ADS
 
3.
Hughes
TP
,
Mauro
MJ
,
Cortes
JE
, et al.
Asciminib in chronic myeloid leukemia after ABL kinase inhibitor failure
.
N Engl J Med
.
2019
;
381
(
24
):
2315
-
2326
.
Google Scholar
Crossref
Search ADS
 
4.
Rea
D
,
Mauro
MJ
,
Boquimpani
C
, et al.
A phase 3, open-label, randomized study of asciminib, a STAMP inhibitor, vs bosutinib in CML after 2 or more prior TKIs
.
Blood
.
2021
;
138
(
21
):
2031
-
2041
.
Google Scholar
Crossref
Search ADS
PubMed
 
5.
Hantschel
O
,
Nagar
B
,
Guettler
S
, et al.
A myristoyl/phosphotyrosine switch regulates c-Abl
.
Cell
.
2003
;
112
(
6
):
845
-
857
.
Google Scholar
Crossref
Search ADS
PubMed
 
6.
Nagar
B
,
Hantschel
O
,
Young
MA
, et al.
Structural basis for the autoinhibition of c-Abl tyrosine kinase
.
Cell
.
2003
;
112
(
6
):
859
-
871
.
Google Scholar
Crossref
Search ADS
PubMed
 
7.
Wylie
AA
,
Schoepfer
J
,
Jahnke
W
, et al.
The allosteric inhibitor ABL001 enables dual targeting of BCR-ABL1
.
Nature
.
2017
;
543
(
7647
):
733
-
737
.
Google Scholar
Crossref
Search ADS
PubMed
 
8.
Shah
NP
,
Nicoll
JM
,
Nagar
B
, et al.
Multiple BCR-ABL kinase domain mutations confer polyclonal resistance to the tyrosine kinase inhibitor imatinib (STI571) in chronic phase and blast crisis chronic myeloid leukemia
.
Cancer Cell
.
2002
;
2
(
2
):
117
-
125
.
Google Scholar
Crossref
Search ADS
PubMed
 
9.
Smith
CC
,
Wang
Q
,
Chin
CS
, et al.
Validation of ITD mutations in FLT3 as a therapeutic target in human acute myeloid leukaemia
.
Nature
.
2012
;
485
(
7397
):
260
-
263
.
Google Scholar
Crossref
Search ADS
PubMed
 
10.
Branford
S
,
Rudzki
Z
,
Walsh
S
, et al.
High frequency of point mutations clustered within the adenosine triphosphate-binding region of BCR/ABL in patients with chronic myeloid leukemia or Ph-positive acute lymphoblastic leukemia who develop imatinib (STI571) resistance
.
Blood
.
2002
;
99
(
9
):
3472
-
3475
.
Google Scholar
Crossref
Search ADS
PubMed
 
11.
Kobayashi
S
,
Boggon
TJ
,
Dayaram
T
, et al.
EGFR mutation and resistance of non-small-cell lung cancer to gefitinib
.
N Engl J Med
.
2005
;
352
(
8
):
786
-
792
.
Google Scholar
Crossref
Search ADS
 
12.
Lyczek
A
,
Berger
BT
,
Rangwala
AM
, et al.
Mutation in Abl kinase with altered drug-binding kinetics indicates a novel mechanism of imatinib resistance
.
Proc Natl Acad Sci U S A
.
2021
;
118
(
46
):
e2111451118
.
Google Scholar
Crossref
Search ADS
PubMed
 
13.
Yun
CH
,
Mengwasser
KE
,
Toms
AV
, et al.
The T790M mutation in EGFR kinase causes drug resistance by increasing the affinity for ATP
.
Proc Natl Acad Sci U S A
.
2008
;
105
(
6
):
2070
-
2075
.
Google Scholar
Crossref
Search ADS
PubMed
 
14.
Braun
TP
,
Eide
CA
,
Druker
BJ
.
Response and resistance to BCR-ABL1-targeted therapies
.
Cancer Cell
.
2020
;
37
(
4
):
530
-
542
.
Google Scholar
Crossref
Search ADS
PubMed
 
15.
Eide
CA
,
Zabriskie
MS
,
Savage Stevens
SL
, et al.
Combining the allosteric inhibitor asciminib with ponatinib suppresses emergence of and restores efficacy against highly resistant BCR-ABL1 mutants
.
Cancer Cell
.
2019
;
36
(
4
):
431
-
443.e5
.
Google Scholar
Crossref
Search ADS
PubMed
 
16.
Lamontanara
AJ
,
Georgeon
S
,
Tria
G
,
Svergun
DI
,
Hantschel
O
.
The SH2 domain of Abl kinases regulates kinase autophosphorylation by controlling activation loop accessibility
.
Nat Commun
.
2014
;
5
:
5470
.
Google Scholar
Crossref
Search ADS
PubMed
 
17.
Lorenz
S
,
Deng
P
,
Hantschel
O
,
Superti-Furga
G
,
Kuriyan
J
.
Crystal structure of an SH2-kinase construct of c-Abl and effect of the SH2 domain on kinase activity
.
Biochem J
.
2015
;
468
(
2
):
283
-
291
.
Google Scholar
Crossref
Search ADS
PubMed
 
18.
Martinez Molina
D
,
Jafari
R
,
Ignatushchenko
M
, et al.
Monitoring drug target engagement in cells and tissues using the cellular thermal shift assay
.
Science
.
2013
;
341
(
6141
):
84
-
87
.
Google Scholar
Crossref
Search ADS
PubMed
 
19.
Hantschel
O
,
Superti-Furga
G
.
Regulation of the c-Abl and Bcr-Abl tyrosine kinases
.
Nat Rev Mol Cell Biol
.
2004
;
5
(
1
):
33
-
44
.
Google Scholar
Crossref
Search ADS
PubMed
 
20.
Khorashad
JS
,
de Lavallade
H
,
Apperley
JF
, et al.
Finding of kinase domain mutations in patients with chronic phase chronic myeloid leukemia responding to imatinib may identify those at high risk of disease progression
.
J Clin Oncol
.
2008
;
26
(
29
):
4806
-
4813
.
Google Scholar
Crossref
Search ADS
 
21.
Qin
Y
,
Chen
S
,
Jiang
B
, et al.
Characteristics of BCR-ABL kinase domain point mutations in Chinese imatinib-resistant chronic myeloid leukemia patients
.
Ann Hematol
.
2011
;
90
(
1
):
47
-
52
.
Google Scholar
Crossref
Search ADS
PubMed
 
22.
Branford
S
,
Melo
JV
,
Hughes
TP
.
Selecting optimal second-line tyrosine kinase inhibitor therapy for chronic myeloid leukemia patients after imatinib failure: does the BCR-ABL mutation status really matter?
.
Blood
.
2009
;
114
(
27
):
5426
-
5435
.
Google Scholar
Crossref
Search ADS
PubMed
 
23.
Kim
C
,
Ludewig
H
,
Hadzipasic
A
,
Kutter
S
,
Nguyen
V
,
Kern
D
.
A biophysical framework for double-drugging kinases
.
Proc Natl Acad Sci U S A
.
2023
;
120
(
34
):
e2304611120
.
Google Scholar
Crossref
Search ADS
PubMed
 
© 2024 American Society of Hematology. Published by Elsevier Inc. All rights are reserved, including those for text and data mining, AI training, and similar technologies.
2024
You do not currently have access to this content.
Sign in via your Institution