Tyrosine 842 in the activation loop is required for full transformation by the oncogenic mutant FLT3-ITD

Kazi, Julhash U.; Chougule, Rohit A.; Li, Tianfeng; Su, Xianwei; Moharram, Sausan A.; Rupar, Kaja; Marhäll, Alissa; Mohiuddin, Gazi; Sun, Jianmin; Zhao, Hui; Rönnstrand, Lars

Tyrosine 842 in the activation loop is required for full transformation by the oncogenic mutant FLT3-ITD

Mark

; Chougule, Rohit A. ^LU ; Li, Tianfeng ; Su, Xianwei ; Moharram, Sausan A. ^LU ; Rupar, Kaja ^LU ; Marhäll, Alissa ^LU ; Mohiuddin, Gazi ^LU ; Sun, Jianmin ^LU and Zhao, Hui , et al. (2017) In Cellular and Molecular Life Sciences 74(14). p.2679-2688

Abstract: The type III receptor tyrosine kinase FLT3 is frequently mutated in acute myeloid leukemia. Oncogenic FLT3 mutants display constitutive activity leading to aberrant cell proliferation and survival. Phosphorylation on several critical tyrosine residues is known to be essential for FLT3 signaling. Among these tyrosine residues, Y842 is located in the so-called activation loop. The position of this tyrosine residue is well conserved in all receptor tyrosine kinases. It has been reported that phosphorylation of the activation loop tyrosine is critical for catalytic activity for some but not all receptor tyrosine kinases. The role of Y842 residue in FLT3 signaling has not yet been studied. In this report, we show that Y842 is not important... (More); The type III receptor tyrosine kinase FLT3 is frequently mutated in acute myeloid leukemia. Oncogenic FLT3 mutants display constitutive activity leading to aberrant cell proliferation and survival. Phosphorylation on several critical tyrosine residues is known to be essential for FLT3 signaling. Among these tyrosine residues, Y842 is located in the so-called activation loop. The position of this tyrosine residue is well conserved in all receptor tyrosine kinases. It has been reported that phosphorylation of the activation loop tyrosine is critical for catalytic activity for some but not all receptor tyrosine kinases. The role of Y842 residue in FLT3 signaling has not yet been studied. In this report, we show that Y842 is not important for FLT3 activation or ubiquitination but plays a critical role in regulating signaling downstream of the receptor as well as controlling receptor stability. We found that mutation of Y842 in the FLT3-ITD oncogenic mutant background reduced cell viability and increased apoptosis. Furthermore, the introduction of the Y842 mutation in the FLT3-ITD background led to a dramatic reduction in in vitro colony forming capacity. Additionally, mice injected with cells expressing FLT3-ITD/Y842F displayed a significant delay in tumor formation, compared to FLT3-ITD expressing cells. Microarray analysis comparing gene expression regulated by FLT3-ITD versus FLT3-ITD/Y842F demonstrated that mutation of Y842 causes suppression of anti-apoptotic genes. Furthermore, we showed that cells expressing FLT3-ITD/Y842F display impaired activity of the RAS/ERK pathway due to reduced interaction between FLT3 and SHP2 leading to reduced SHP2 activation. Thus, we suggest that Y842 is critical for FLT3-mediated RAS/ERK signaling and cellular transformation.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/85268470-dea1-4ae2-9978-35cd6dbb37e0

author

Kazi, Julhash U. ^LU

; Chougule, Rohit A. ^LU ; Li, Tianfeng ; Su, Xianwei ; Moharram, Sausan A. ^LU ; Rupar, Kaja ^LU ; Marhäll, Alissa ^LU ; Mohiuddin, Gazi ^LU ; Sun, Jianmin ^LU and Zhao, Hui , et al. (More)

Kazi, Julhash U. ^LU

; Chougule, Rohit A. ^LU ; Li, Tianfeng ; Su, Xianwei ; Moharram, Sausan A. ^LU ; Rupar, Kaja ^LU ; Marhäll, Alissa ^LU ; Mohiuddin, Gazi ^LU ; Sun, Jianmin ^LU ; Zhao, Hui and Rönnstrand, Lars ^LU

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organization

publishing date

2017-03-07

type

Contribution to journal

publication status

published

subject

Cell and Molecular Biology

keywords

Activation loop, Acute myeloid leukemia, FLT3, FLT3-ITD, Microarray, SHP2, Survival, Transformation

in

Cellular and Molecular Life Sciences

volume

74

issue

14

pages

2679 - 2688

publisher

Birkhäuser Verlag

external identifiers

scopus:85014561805
pmid:28271164
wos:000403887100012

ISSN

1420-682X

DOI

10.1007/s00018-017-2494-0

language

English

LU publication?

yes

id

85268470-dea1-4ae2-9978-35cd6dbb37e0

date added to LUP

2017-03-14 12:08:07

date last changed

2024-01-28 14:16:04

@article{85268470-dea1-4ae2-9978-35cd6dbb37e0,
  abstract     = {{<p>The type III receptor tyrosine kinase FLT3 is frequently mutated in acute myeloid leukemia. Oncogenic FLT3 mutants display constitutive activity leading to aberrant cell proliferation and survival. Phosphorylation on several critical tyrosine residues is known to be essential for FLT3 signaling. Among these tyrosine residues, Y842 is located in the so-called activation loop. The position of this tyrosine residue is well conserved in all receptor tyrosine kinases. It has been reported that phosphorylation of the activation loop tyrosine is critical for catalytic activity for some but not all receptor tyrosine kinases. The role of Y842 residue in FLT3 signaling has not yet been studied. In this report, we show that Y842 is not important for FLT3 activation or ubiquitination but plays a critical role in regulating signaling downstream of the receptor as well as controlling receptor stability. We found that mutation of Y842 in the FLT3-ITD oncogenic mutant background reduced cell viability and increased apoptosis. Furthermore, the introduction of the Y842 mutation in the FLT3-ITD background led to a dramatic reduction in in vitro colony forming capacity. Additionally, mice injected with cells expressing FLT3-ITD/Y842F displayed a significant delay in tumor formation, compared to FLT3-ITD expressing cells. Microarray analysis comparing gene expression regulated by FLT3-ITD versus FLT3-ITD/Y842F demonstrated that mutation of Y842 causes suppression of anti-apoptotic genes. Furthermore, we showed that cells expressing FLT3-ITD/Y842F display impaired activity of the RAS/ERK pathway due to reduced interaction between FLT3 and SHP2 leading to reduced SHP2 activation. Thus, we suggest that Y842 is critical for FLT3-mediated RAS/ERK signaling and cellular transformation.</p>}},
  author       = {{Kazi, Julhash U. and Chougule, Rohit A. and Li, Tianfeng and Su, Xianwei and Moharram, Sausan A. and Rupar, Kaja and Marhäll, Alissa and Mohiuddin, Gazi and Sun, Jianmin and Zhao, Hui and Rönnstrand, Lars}},
  issn         = {{1420-682X}},
  keywords     = {{Activation loop; Acute myeloid leukemia; FLT3; FLT3-ITD; Microarray; SHP2; Survival; Transformation}},
  language     = {{eng}},
  month        = {{03}},
  number       = {{14}},
  pages        = {{2679--2688}},
  publisher    = {{Birkhäuser Verlag}},
  series       = {{Cellular and Molecular Life Sciences}},
  title        = {{Tyrosine 842 in the activation loop is required for full transformation by the oncogenic mutant FLT3-ITD}},
  url          = {{http://dx.doi.org/10.1007/s00018-017-2494-0}},
  doi          = {{10.1007/s00018-017-2494-0}},
  volume       = {{74}},
  year         = {{2017}},
}

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Tyrosine 842 in the activation loop is required for full transformation by the oncogenic mutant FLT3-ITD