ICL-induced miR139-3p and miR199a-3p have opposite roles in hematopoietic cell expansion and leukemic transformation

Mir Farshid Alemdehy; Jurgen R. Haanstra; Hans W. J. de Looper; Paulina M. H. van Strien; Judith Verhagen-Oldenampsen; Yvette Caljouw; Mathijs A. Sanders; Remco Hoogenboezem; Arnoud H. de Ru; George M. C. Janssen; Stephanie E. Smetsers; Marc B. Bierings; Peter A. van Veelen; Marieke von Lindern; Ivo P. Touw; Stefan J. Erkeland

doi:https://doi.org/10.1182/blood-2014-11-612507

ICL-induced miR139-3p and miR199a-3p have opposite roles in hematopoietic cell expansion and leukemic transformation

Mir Farshid Alemdehy, Jurgen R. Haanstra, Hans W. J. de Looper, Paulina M. H. van Strien, Judith Verhagen-Oldenampsen, Yvette Caljouw, Mathijs A. Sanders, Remco Hoogenboezem, Arnoud H. de Ru, George M. C. Janssen, Stephanie E. Smetsers, Marc B. Bierings, Peter A. van Veelen, Marieke von Lindern, Ivo P. Touw, Stefan J. Erkeland

Landsteiner Laboratory (AMC)

Research output: Contribution to journal › Article › Academic › peer-review

41 Citations (Scopus)

Abstract

Interstrand crosslinks (ICLs) are toxic DNA lesions that cause severe genomic damage during replication, especially in Fanconi anemia pathway-deficient cells. This results in progressive bone marrow failure and predisposes to acute myeloid leukemia (AML). The molecular mechanisms responsible for these defects are largely unknown. Using Ercc1-deficient mice, we show that Trp53 is responsible for ICL-induced bone marrow failure and that loss of Trp53 is leukemogenic in this model. In addition, Ercc1-deficient myeloid progenitors gain elevated levels of miR-139-3p and miR-199a-3p with age. These microRNAs exert opposite effects on hematopoiesis. Ectopic expression of miR-139-3p strongly inhibited proliferation of myeloid progenitors, whereas inhibition of miR-139-3p activity restored defective proliferation of Ercc1-deficient progenitors. Conversely, the inhibition of miR-199a-3p functions aggravated the myeloid proliferation defect in the Ercc1-deficient model, whereas its enforced expression enhanced proliferation of progenitors. Importantly, miR-199a-3p caused AML in a pre-leukemic mouse model, supporting its role as an onco-microRNA. Target genes include HuR for miR-139-3p and Prdx6, Runx1, and Suz12 for miR-199a-3p. The latter genes have previously been implicated as tumor suppressors in de novo and secondary AML. These findings show that, in addition to TRP53-controlled mechanisms, miR-139-3p and miR-199a-3p are involved in the defective hematopoietic function of ICL-repair deficient myeloid progenitors

Original language	English
Pages (from-to)	3937-3948
Journal	Blood
Volume	125
Issue number	25
DOIs	https://doi.org/10.1182/blood-2014-11-612507
Publication status	Published - 2015

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https://doi.org/10.1182/blood-2014-11-612507

Cite this

Alemdehy, M. F., Haanstra, J. R., de Looper, H. W. J., van Strien, P. M. H., Verhagen-Oldenampsen, J., Caljouw, Y., Sanders, M. A., Hoogenboezem, R., de Ru, A. H., Janssen, G. M. C., Smetsers, S. E., Bierings, M. B., van Veelen, P. A., von Lindern, M., Touw, I. P., & Erkeland, S. J. (2015). ICL-induced miR139-3p and miR199a-3p have opposite roles in hematopoietic cell expansion and leukemic transformation. Blood, 125(25), 3937-3948. https://doi.org/10.1182/blood-2014-11-612507

@article{a3fb5c71372547babe221bc67010d259,

title = "ICL-induced miR139-3p and miR199a-3p have opposite roles in hematopoietic cell expansion and leukemic transformation",

abstract = "Interstrand crosslinks (ICLs) are toxic DNA lesions that cause severe genomic damage during replication, especially in Fanconi anemia pathway-deficient cells. This results in progressive bone marrow failure and predisposes to acute myeloid leukemia (AML). The molecular mechanisms responsible for these defects are largely unknown. Using Ercc1-deficient mice, we show that Trp53 is responsible for ICL-induced bone marrow failure and that loss of Trp53 is leukemogenic in this model. In addition, Ercc1-deficient myeloid progenitors gain elevated levels of miR-139-3p and miR-199a-3p with age. These microRNAs exert opposite effects on hematopoiesis. Ectopic expression of miR-139-3p strongly inhibited proliferation of myeloid progenitors, whereas inhibition of miR-139-3p activity restored defective proliferation of Ercc1-deficient progenitors. Conversely, the inhibition of miR-199a-3p functions aggravated the myeloid proliferation defect in the Ercc1-deficient model, whereas its enforced expression enhanced proliferation of progenitors. Importantly, miR-199a-3p caused AML in a pre-leukemic mouse model, supporting its role as an onco-microRNA. Target genes include HuR for miR-139-3p and Prdx6, Runx1, and Suz12 for miR-199a-3p. The latter genes have previously been implicated as tumor suppressors in de novo and secondary AML. These findings show that, in addition to TRP53-controlled mechanisms, miR-139-3p and miR-199a-3p are involved in the defective hematopoietic function of ICL-repair deficient myeloid progenitors",

author = "Alemdehy, {Mir Farshid} and Haanstra, {Jurgen R.} and {de Looper}, {Hans W. J.} and {van Strien}, {Paulina M. H.} and Judith Verhagen-Oldenampsen and Yvette Caljouw and Sanders, {Mathijs A.} and Remco Hoogenboezem and {de Ru}, {Arnoud H.} and Janssen, {George M. C.} and Smetsers, {Stephanie E.} and Bierings, {Marc B.} and {van Veelen}, {Peter A.} and {von Lindern}, Marieke and Touw, {Ivo P.} and Erkeland, {Stefan J.}",

year = "2015",

doi = "https://doi.org/10.1182/blood-2014-11-612507",

language = "English",

volume = "125",

pages = "3937--3948",

journal = "Blood",

issn = "0006-4971",

publisher = "American Society of Hematology",

number = "25",

}

Alemdehy, MF, Haanstra, JR, de Looper, HWJ, van Strien, PMH, Verhagen-Oldenampsen, J, Caljouw, Y, Sanders, MA, Hoogenboezem, R, de Ru, AH, Janssen, GMC, Smetsers, SE, Bierings, MB, van Veelen, PA, von Lindern, M, Touw, IP & Erkeland, SJ 2015, 'ICL-induced miR139-3p and miR199a-3p have opposite roles in hematopoietic cell expansion and leukemic transformation', Blood, vol. 125, no. 25, pp. 3937-3948. https://doi.org/10.1182/blood-2014-11-612507

TY - JOUR

T1 - ICL-induced miR139-3p and miR199a-3p have opposite roles in hematopoietic cell expansion and leukemic transformation

AU - Alemdehy, Mir Farshid

AU - Haanstra, Jurgen R.

AU - de Looper, Hans W. J.

AU - van Strien, Paulina M. H.

AU - Verhagen-Oldenampsen, Judith

AU - Caljouw, Yvette

AU - Sanders, Mathijs A.

AU - Hoogenboezem, Remco

AU - de Ru, Arnoud H.

AU - Janssen, George M. C.

AU - Smetsers, Stephanie E.

AU - Bierings, Marc B.

AU - van Veelen, Peter A.

AU - von Lindern, Marieke

AU - Touw, Ivo P.

AU - Erkeland, Stefan J.

PY - 2015

Y1 - 2015

N2 - Interstrand crosslinks (ICLs) are toxic DNA lesions that cause severe genomic damage during replication, especially in Fanconi anemia pathway-deficient cells. This results in progressive bone marrow failure and predisposes to acute myeloid leukemia (AML). The molecular mechanisms responsible for these defects are largely unknown. Using Ercc1-deficient mice, we show that Trp53 is responsible for ICL-induced bone marrow failure and that loss of Trp53 is leukemogenic in this model. In addition, Ercc1-deficient myeloid progenitors gain elevated levels of miR-139-3p and miR-199a-3p with age. These microRNAs exert opposite effects on hematopoiesis. Ectopic expression of miR-139-3p strongly inhibited proliferation of myeloid progenitors, whereas inhibition of miR-139-3p activity restored defective proliferation of Ercc1-deficient progenitors. Conversely, the inhibition of miR-199a-3p functions aggravated the myeloid proliferation defect in the Ercc1-deficient model, whereas its enforced expression enhanced proliferation of progenitors. Importantly, miR-199a-3p caused AML in a pre-leukemic mouse model, supporting its role as an onco-microRNA. Target genes include HuR for miR-139-3p and Prdx6, Runx1, and Suz12 for miR-199a-3p. The latter genes have previously been implicated as tumor suppressors in de novo and secondary AML. These findings show that, in addition to TRP53-controlled mechanisms, miR-139-3p and miR-199a-3p are involved in the defective hematopoietic function of ICL-repair deficient myeloid progenitors

AB - Interstrand crosslinks (ICLs) are toxic DNA lesions that cause severe genomic damage during replication, especially in Fanconi anemia pathway-deficient cells. This results in progressive bone marrow failure and predisposes to acute myeloid leukemia (AML). The molecular mechanisms responsible for these defects are largely unknown. Using Ercc1-deficient mice, we show that Trp53 is responsible for ICL-induced bone marrow failure and that loss of Trp53 is leukemogenic in this model. In addition, Ercc1-deficient myeloid progenitors gain elevated levels of miR-139-3p and miR-199a-3p with age. These microRNAs exert opposite effects on hematopoiesis. Ectopic expression of miR-139-3p strongly inhibited proliferation of myeloid progenitors, whereas inhibition of miR-139-3p activity restored defective proliferation of Ercc1-deficient progenitors. Conversely, the inhibition of miR-199a-3p functions aggravated the myeloid proliferation defect in the Ercc1-deficient model, whereas its enforced expression enhanced proliferation of progenitors. Importantly, miR-199a-3p caused AML in a pre-leukemic mouse model, supporting its role as an onco-microRNA. Target genes include HuR for miR-139-3p and Prdx6, Runx1, and Suz12 for miR-199a-3p. The latter genes have previously been implicated as tumor suppressors in de novo and secondary AML. These findings show that, in addition to TRP53-controlled mechanisms, miR-139-3p and miR-199a-3p are involved in the defective hematopoietic function of ICL-repair deficient myeloid progenitors

U2 - https://doi.org/10.1182/blood-2014-11-612507

DO - https://doi.org/10.1182/blood-2014-11-612507

M3 - Article

C2 - 25778535

SN - 0006-4971

VL - 125

SP - 3937

EP - 3948

JO - Blood

JF - Blood

IS - 25

ER -