Inhibitory effects of midostaurin and avapritinib on myeloid progenitors derived from patients with KIT D816V positive advanced systemic mastocytosis
Inhibitory effects of midostaurin and avapritinib on myeloid progenitors derived from patients with KIT D816V positive advanced systemic mastocytosis
Advanced systemic mastocytosis (advSM) is characterized by the presence of an acquired KIT D816V mutation in >90% of patients. In the majority of patients, KIT D816V is not only detected in mast cells but also in other hematopoietic lineages. We sought to investigate the effects of the KIT-inhibitors midostaurin and avapritinib on single-cell-derived myeloid progenitor cells using granulocyte-macrophage colony-forming-units of patients with KIT D816V positive advSM. Colonies obtained prior to treatment were incubated in vitro with midostaurin (n = 10) or avapritinib (n = 11) and showed a marked reduction (≥50%) of KIT D816V positive colonies in 3/10 (30%) and 7/11 (64%) patient samples, respectively. Three of those 7 (43%) avapritinib responders were resistant to midostaurin in both, in vitro and in vivo. Colonies from four patients with high-risk molecular profile and aggressive clinical course were resistant to both drugs. The in vitro activity of midostaurin strongly correlated with clinical and molecular responses, e.g., relative reduction of KIT D816V allele burden and the proportion of KIT D816V positive colonies obtained after six months midostaurin-treatment in vivo. We conclude that the colony inhibition assay provides useful information for prediction of responses on midostaurin and that avapritinib has a superior in vitro activity compared to midostaurin.
1105-1205
Lübke, Johannes
aa66da00-2473-47f4-913c-f4601623ac0c
Naumann, Nicole
43566136-d964-415e-be36-45aeb4f88965
Kluger, Sebastian
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Schwaab, Juliana
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Metzgeroth, Georgia
611ec46d-9a11-4e24-ae0f-5ac19dfd0237
Evans, Erica
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Gardino, Alexandra K.
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Lengauer, Christoph
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Hofmann, Wolf-karsten
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Fabarius, Alice
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Cross, Nicholas C. P.
f87650da-b908-4a34-b31b-d62c5f186fe4
Reiter, Andreas
ffa23e84-4a13-4cb5-aaf0-3fafe25dbede
Jawhar, Mohamad
a608a215-173b-47bd-89eb-a8de2fe595aa
1 May 2019
Lübke, Johannes
aa66da00-2473-47f4-913c-f4601623ac0c
Naumann, Nicole
43566136-d964-415e-be36-45aeb4f88965
Kluger, Sebastian
8042b644-b591-4dc5-99c1-cc8f092e55a1
Schwaab, Juliana
d63ed545-a6fc-4815-ab86-f901e55c2a2f
Metzgeroth, Georgia
611ec46d-9a11-4e24-ae0f-5ac19dfd0237
Evans, Erica
029ad8d9-38dd-4427-8943-e17158efe0c5
Gardino, Alexandra K.
0bdee45c-c055-4e9b-bc17-f15fd2c9c611
Lengauer, Christoph
86ec4999-df1b-4c92-9e98-73c58953e9f3
Hofmann, Wolf-karsten
ab66838b-bf8c-4352-a0f0-3c8aafed2570
Fabarius, Alice
5c31b1e0-c6da-49b8-843a-5b0ca736e5a2
Cross, Nicholas C. P.
f87650da-b908-4a34-b31b-d62c5f186fe4
Reiter, Andreas
ffa23e84-4a13-4cb5-aaf0-3fafe25dbede
Jawhar, Mohamad
a608a215-173b-47bd-89eb-a8de2fe595aa
Lübke, Johannes, Naumann, Nicole, Kluger, Sebastian, Schwaab, Juliana, Metzgeroth, Georgia, Evans, Erica, Gardino, Alexandra K., Lengauer, Christoph, Hofmann, Wolf-karsten, Fabarius, Alice, Cross, Nicholas C. P., Reiter, Andreas and Jawhar, Mohamad
(2019)
Inhibitory effects of midostaurin and avapritinib on myeloid progenitors derived from patients with KIT D816V positive advanced systemic mastocytosis.
Leukemia, 33 (5), .
(doi:10.1038/s41375-019-0450-8).
Abstract
Advanced systemic mastocytosis (advSM) is characterized by the presence of an acquired KIT D816V mutation in >90% of patients. In the majority of patients, KIT D816V is not only detected in mast cells but also in other hematopoietic lineages. We sought to investigate the effects of the KIT-inhibitors midostaurin and avapritinib on single-cell-derived myeloid progenitor cells using granulocyte-macrophage colony-forming-units of patients with KIT D816V positive advSM. Colonies obtained prior to treatment were incubated in vitro with midostaurin (n = 10) or avapritinib (n = 11) and showed a marked reduction (≥50%) of KIT D816V positive colonies in 3/10 (30%) and 7/11 (64%) patient samples, respectively. Three of those 7 (43%) avapritinib responders were resistant to midostaurin in both, in vitro and in vivo. Colonies from four patients with high-risk molecular profile and aggressive clinical course were resistant to both drugs. The in vitro activity of midostaurin strongly correlated with clinical and molecular responses, e.g., relative reduction of KIT D816V allele burden and the proportion of KIT D816V positive colonies obtained after six months midostaurin-treatment in vivo. We conclude that the colony inhibition assay provides useful information for prediction of responses on midostaurin and that avapritinib has a superior in vitro activity compared to midostaurin.
Text
Jawhar et al
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Accepted/In Press date: 8 March 2019
e-pub ahead of print date: 25 March 2019
Published date: 1 May 2019
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Local EPrints ID: 429763
URI: http://eprints.soton.ac.uk/id/eprint/429763
ISSN: 0887-6924
PURE UUID: 2bd1a979-67b0-43f7-8693-0825822f13ef
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Date deposited: 05 Apr 2019 16:30
Last modified: 16 Mar 2024 03:24
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Contributors
Author:
Johannes Lübke
Author:
Nicole Naumann
Author:
Sebastian Kluger
Author:
Juliana Schwaab
Author:
Georgia Metzgeroth
Author:
Erica Evans
Author:
Alexandra K. Gardino
Author:
Christoph Lengauer
Author:
Wolf-karsten Hofmann
Author:
Alice Fabarius
Author:
Andreas Reiter
Author:
Mohamad Jawhar
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