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The MYC/Max/MxD network is a target of mutated FLT3 signaling in hematopoietic stem cells in FLT3-ITD-induced myeloproliferative disease

Basit, Farhan ; Andersson, Maria and Hultquist, Anne LU (2018) In Stem Cells International 2018.
Abstract


Acute myeloid leukemia (AML) has poor prognosis due to various mutations, e.g., in the FLT3 gene. Therefore, it is important to identify pathways regulated by the activated Flt3 receptor for the discovery of new therapeutic targets. The Myc network of oncogenes and tumor suppressor genes is involved in mechanisms regulating proliferation and survival of cells, including that of the hematopoietic system. In this study, we evaluated the expression of the Myc oncogenes and Mxd antagonists in hematopoietic stem cell and myeloid progenitor populations in the Flt3-ITD-knockin myeloproliferative mouse model. Our data shows that the expression of Myc network genes is changed in... (More)


Acute myeloid leukemia (AML) has poor prognosis due to various mutations, e.g., in the FLT3 gene. Therefore, it is important to identify pathways regulated by the activated Flt3 receptor for the discovery of new therapeutic targets. The Myc network of oncogenes and tumor suppressor genes is involved in mechanisms regulating proliferation and survival of cells, including that of the hematopoietic system. In this study, we evaluated the expression of the Myc oncogenes and Mxd antagonists in hematopoietic stem cell and myeloid progenitor populations in the Flt3-ITD-knockin myeloproliferative mouse model. Our data shows that the expression of Myc network genes is changed in Flt3-ITD mice compared with the wild type. Mycn is increased in multipotent progenitors and in the pre-GM compartment of myeloid progenitors in the ITD mice while the expression of several genes in the tumor suppressor Mxd family, including Mxd1, Mxd2, and Mxd4, is concomitantly downregulated, as well as the expression of the Mxd-related gene Mnt and the transcriptional activator Miz-1. LSKCD150
+
CD48

hematopoietic long-term stem cells are decreased in the Flt3-ITD cells while multipotent progenitors are increased. Of note, PKC412-mediated inhibition of Flt3-ITD signaling results in downregulation of cMyc and upregulation of the Myc antagonists Mxd1, Mxd2, and Mxd4. Our data provides new mechanistic insights into downstream alterations upon aberrant Flt3 signaling and rationale for combination therapies for tyrosine kinase inhibitors with Myc antagonists in treating AML.

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publishing date
type
Contribution to journal
publication status
published
subject
in
Stem Cells International
volume
2018
article number
3286949
publisher
Hindawi Limited
external identifiers
  • scopus:85062864249
  • pmid:30420889
ISSN
1687-966X
DOI
10.1155/2018/3286949
language
English
LU publication?
yes
id
91a14550-aeaa-467c-966c-9e0a66dd2b6d
date added to LUP
2019-04-01 10:17:38
date last changed
2024-06-11 07:40:50
@article{91a14550-aeaa-467c-966c-9e0a66dd2b6d,
  abstract     = {{<p><br>
                                                         Acute myeloid leukemia (AML) has poor prognosis due to various mutations, e.g., in the FLT3 gene. Therefore, it is important to identify pathways regulated by the activated Flt3 receptor for the discovery of new therapeutic targets. The Myc network of oncogenes and tumor suppressor genes is involved in mechanisms regulating proliferation and survival of cells, including that of the hematopoietic system. In this study, we evaluated the expression of the Myc oncogenes and Mxd antagonists in hematopoietic stem cell and myeloid progenitor populations in the Flt3-ITD-knockin myeloproliferative mouse model. Our data shows that the expression of Myc network genes is changed in Flt3-ITD mice compared with the wild type. Mycn is increased in multipotent progenitors and in the pre-GM compartment of myeloid progenitors in the ITD mice while the expression of several genes in the tumor suppressor Mxd family, including Mxd1, Mxd2, and Mxd4, is concomitantly downregulated, as well as the expression of the Mxd-related gene Mnt and the transcriptional activator Miz-1. LSKCD150                             <br>
                            <sup>+</sup><br>
                                                         CD48                             <br>
                            <sup>−</sup><br>
                                                          hematopoietic long-term stem cells are decreased in the Flt3-ITD cells while multipotent progenitors are increased. Of note, PKC412-mediated inhibition of Flt3-ITD signaling results in downregulation of cMyc and upregulation of the Myc antagonists Mxd1, Mxd2, and Mxd4. Our data provides new mechanistic insights into downstream alterations upon aberrant Flt3 signaling and rationale for combination therapies for tyrosine kinase inhibitors with Myc antagonists in treating AML.                         <br>
                        </p>}},
  author       = {{Basit, Farhan and Andersson, Maria and Hultquist, Anne}},
  issn         = {{1687-966X}},
  language     = {{eng}},
  month        = {{10}},
  publisher    = {{Hindawi Limited}},
  series       = {{Stem Cells International}},
  title        = {{The MYC/Max/MxD network is a target of mutated FLT3 signaling in hematopoietic stem cells in FLT3-ITD-induced myeloproliferative disease}},
  url          = {{http://dx.doi.org/10.1155/2018/3286949}},
  doi          = {{10.1155/2018/3286949}},
  volume       = {{2018}},
  year         = {{2018}},
}