Myeloproliferative disease induced by TEL-PDGFRB displays dynamic range sensitivity to Stat5 gene dosage

doi:10.1182/blood-2006-07-036335

. 2007 May 1;109(9):3906-14.

doi: 10.1182/blood-2006-07-036335. Epub 2007 Jan 11.

Myeloproliferative disease induced by TEL-PDGFRB displays dynamic range sensitivity to Stat5 gene dosage

Jennifer A Cain¹, Zhifu Xiang, Julie O'Neal, Friederike Kreisel, AnnaLynn Colson, Hui Luo, Lothar Hennighausen, Michael H Tomasson

Affiliations

PMID: 17218386
PMCID: PMC1874559
DOI: 10.1182/blood-2006-07-036335

Myeloproliferative disease induced by TEL-PDGFRB displays dynamic range sensitivity to Stat5 gene dosage

Jennifer A Cain et al. Blood. 2007.

. 2007 May 1;109(9):3906-14.

doi: 10.1182/blood-2006-07-036335. Epub 2007 Jan 11.

Authors

Jennifer A Cain¹, Zhifu Xiang, Julie O'Neal, Friederike Kreisel, AnnaLynn Colson, Hui Luo, Lothar Hennighausen, Michael H Tomasson

Affiliation

¹ Department of Internal Medicine, Division of Oncology, Washington University Siteman Cancer Center, 550 S. Euclid Avenue, St. Louis, MO 63110, USA.

PMID: 17218386
PMCID: PMC1874559
DOI: 10.1182/blood-2006-07-036335

Abstract

Expression of the constitutively activated TEL/PDGFbetaR fusion protein is associated with the t(5;12)(q33;p13) chromosomal translocation found in a subset of patients with chronic myelomonocytic leukemia. TEL/PDGFbetaR activates multiple signal transduction pathways in cell-culture systems, and expression of the TEL-PDGFRB fusion gene induces myeloproliferative disease (MPD) in mice. We used gene-_targeted mice to characterize the contribution of signal transducer and activator of transcription (Stat) and Src family genes to TEL-PDGFRB-mediated transformation in methylcellulose colony and murine bone marrow transduction/transplantation assays. Fetal liver hematopoietic stem and progenitor cells harboring _targeted deletion of both Stat5a and Stat5b (Stat5ab(null/null)) genes were refractory to transformation by TEL-PDGFRB in methylcellulose colony assays. Notably, these cell populations were maintained in Stat5ab(null/null) fetal livers and succumbed to transformation by c-Myc. Surprisingly, _targeted disruption of either Stat5a or Stat5b alone also impaired TEL-PDGFRB-mediated transformation. Survival of TPiGFP-->Stat5a(-/-) and TPiGFP-->Stat5a(+/-) mice was significantly prolonged, demonstrating significant sensitivity of TEL-PDGFRB-induced MPD to the dosage of Stat5a. TEL-PDGFRB-mediated MPD was incompletely penetrant in TPiGFP-->Stat5b(-/-) mice. In contrast, Src family kinases Lyn, Hck, and Fgr and the Stat family member Stat1 were dispensable for TEL-PDGFRB disease. Together, these data demonstrate that Stat5a and Stat5b are dose-limiting mediators of TEL-PDGFRB-induced myeloproliferation.

PubMed Disclaimer

Figures

**Figure 1**
*Stat5* is required in primary murine hematopoietic cells for *TEL-PDGFRB*–mediated growth. (A) Cytokine-independent colony formation of 14.5-dpc fetal liver cells expressing either *TEL-PDGFRB* or *c-Myc*. Data shown are the mean percentage of colonies formed by *Stat5ab^null/null* and *Stat5ab*^+/null cells relative to *Stat5ab*^+/+ cells for a given experimental condition. Error bars represent standard deviation. *TPNeo* induced formation of 195 ± 18 *Stat5ab*^+/+, 194 ± 19 *Stat5ab*^+/null, and 3 ± 1 *Stat5ab^null/null* G418-resistant colonies per 10⁵ transduced fetal liver cells. Positive control *c-Myc* induced formation of 159 ± 8 colonies per 10⁵ *Stat5ab^null/null* fetal liver cells plated and 184 ± 31 colonies in *Stat5ab*^+/+ cells. Cells transduced with negative control MSCV-*Neo* did not form colonies in the absence of cytokines (data not shown). Transduction efficiency of *Stat5ab*^+/+ and *Stat5ab^null/null* fetal liver cells with MSCV-*Myc* was 14% and 12% for 2 independent experiments. For *TPNeo* and MSCV-*Neo*, transduction efficiency of *Stat5ab*^+/+ cells averaged 25% ± 15% and *Stat5ab^null/null* cells averaged 45% ± 16% for 7 independent transductions of each genotype. (B) *TEL-PDGFRB* induced cytokine independent colony formation in *Stat5a*^+/+ (469 ± 26 colonies per 10⁵ transduced cells), *Stat5a*^+/− (266 ± 40), and *Stat5a*^−/− (163 ± 16) whole bone marrow cells. Data shown are the mean percentage of colonies formed by *Stat5a*^−/− and *Stat5a*^+/− cells relative to *Stat5a*^+/+ cells for a given experimental condition. Error bars represent standard deviation. Transduction efficiency of *Stat5a*^−/− cells averaged 98% ± 17% and 93% ± 18% for *Stat5a*^+/+ bone marrow cells in 3 independent transductions. (C) *TEL-PDGFRB* induced cytokine-independent colony formation in *Stat5b*^+/+ (602 ± 39 colonies per 10⁵ transduced cells), *Stat5b*^+/− (135 ± 25), and *Stat5b*^−/− (27 ± 11) whole bone marrow cells. Data shown are the mean percentage of colonies formed by *Stat5b*^−/− and *Stat5b*^+/− cells relative to *Stat5b*^+/+ cells for a given experimental condition. Error bars represent standard deviation. Transduction efficiency of *Stat5b*^−/− cells was 99% and 81% for *Stat5b*^+/+ bone marrow cells. (*TPNeo* indicates *TEL-PDGFRB*-PGK *Neo*; MSCV-*Myc*, MSCV-*c-Myc* ires GFP; and ND, not done.)

**Figure 2**
**Hematopoietic stem and progenitor-cell populations are preserved in fetal livers of *Stat5ab^null/null* mice**. (A) Flow cytometric analysis of *Stat5ab^null/null*, *Stat5ab*^+/null, and *Stat5ab*^+/+ 14.5-dpc fetal livers for early hematopoietic cells. Top panel shows Kit and Sca-1 expression of lineage-negative fetal liver cells. Bottom panel shows CMP (FcγR^loCD34⁺), MEP (FcγR^loCD34⁻), and GMP (FcγR^hiCD34⁺) populations, with percentage of Kit⁺Lin⁻Sca⁻ falling into each progenitor population as indicated. (B) Proportion of cells that is identified as either KLS (black), progenitors (CMPs, MEPs, or GMPs, diagonal stripes), or lineage-committed (gray) hematopoietic cells within *Stat5ab*^+/+, *Stat5ab*^+/null, and *Stat5ab^null/null* 14.5-dpc fetal livers as determined by flow cytometric detection of cell-surface markers. (C) Cytokine-dependent colony formation of vector-transduced 14.5-dpc fetal liver cells when cells were plated in the presence of SCF, IL3, IL6, and EPO. Data shown are the mean percentage of colonies formed by *Stat5ab^null/null* and *Stat5ab*^+/null cells relative to *Stat5ab*^+/+ cells. Error bars represent standard deviation. Vector control *Stat5ab*^+/+ cells generated 688 ± 18 G418-resistant colonies per 10⁵ transduced fetal liver cells, while *Stat5ab*^+/null and *Stat5ab^null/null* cells formed 535 ± 12 and 355 ± 10 colonies. *TPNeo*-transduced *Stat5ab*^+/+, *Stat5ab*^+/null, and *Stat5ab^null/null* cells formed 337 ± 33, 559 ± 43, and 321 ± 30 G418 colonies, respectively. Transduction efficiency of *Stat5ab*^+/+ cells averaged 25% ± 15% and *Stat5ab^null/null* cells averaged 45% ± 16% for 7 independent transductions of each genotype. (KLS indicates Kit⁺Sca⁺Lin⁻; CMP, common myeloid progenitor; MEP, megakaryocyte-erythrocyte progenitor; and GMP, granulocyte-monocyte progenitor.)

**Figure 3**
*Stat5a* gene dosage mediates the latency of *TEL-PDGFRB*–induced myeloproliferation. (A) Kaplan-Meier plot shows survival of recipient mice when *TEL-PDGFRB* is expressed in bone marrow cells harboring homozygous or heterozygous inactivation of *Stat5a. TP*iGFP→*Stat5a*^+/+ mice (circles) developed severe MPD (spleen weight median, 790 ± 90 mg; range, 620-910 mg; n = 6). TPiGFP→*Stat5a*^+/− mice (▵) developed moderate or severe MPD (spleen weight median, 770 ± 300 mg; range, 350-1120 mg; n = 7). TPiGFP→*Stat5a*^−/− mice (squares) developed moderate MPD with splenomegaly (spleen weight, 710 ± 550 mg; range, 350-2070 mg; n = 8) and leukocytosis. Black shapes indicate death due to severe (fatal) MPD marked by leukocytosis and splenomegaly (WBC, > 50 × 10⁹/L [50 000/μL] and spleen weight, > 450 mg) at time of death due to disease. Shaded shapes represent moderate MPD (WBC, > 15 × 10⁹/L [15 000/μL] and/or spleen weight, > 450 mg) at time of death due to disease. Open shapes indicate animal found dead. (B) Median peripheral blood cell count at time of death due to disease. Error bars represent standard deviation. *TEL-PDGFRB* induced severe leukocytosis in TPiGFP→*Stat5a*^+/+ mice (359 ± 225 × 10⁹/L [359 000 ± 225 000/μL]; range, 60-737 × 10⁹/L [60 000-737 000/μL]; n = 6) and moderate leukocytosis in TPiGFP→*Stat5a*^+/− mice (28 ± 15 × 10⁹/L [28 000 ± 15 000/μL]; range, 12-131 × 10⁹/L [12 000-131 000/μL]; n = 7) as well as TPiGFP→*Stat5a*^−/− mice (29 ± 27 × 10⁹/L [29 000 ± 27 000/μL];range, 10-94 × 10⁹/L [10 000-94 000/μL]; n = 8). (C) Three mice from each cohort were analyzed 28 days after transplantation. Median of peripheral blood counts is shown. Error bars represent standard deviation. Peripheral blood counts of *GFP*→*Stat5a*^−/− control mice are also shown. (TPiGFP indicates *TEL-PDGFRB* ires *eGFP*; MPD, myeloproliferative disease; and WBC, peripheral white blood cell count.)

**Figure 4**
**Severity and penetrance of *TEL-PDGFRB*–induced myeloproliferation are reduced in the absence of Stat5b**. (A) Kaplan-Meier plot shows survival of recipient mice when *TEL-PDGFRB* is expressed in bone marrow cells harboring _targeted deletion of *Stat5b* (TPiGFP→*Stat5b*^−/−, squares) or wild-type control bone marrow cells (TPiGFP→*Stat5b*^+/+, ○). TPiGFP→*Stat5b*^+/+ mice developed severe MPD (spleen weight median, 890 ± 274 mg; range, 670-1460 mg [n = 6]; WBC median, 139 ± 87 × 10⁹/L [139 000 ± 87 000/μL]; range, 13-237 × 10⁹/L [13 000-237 000/μL] [n = 6]; median survival ± standard error, 33 ± 2.9 days). Severe MPD was detected in 5 of 7 TPiGFP→*Stat5b*^−/− mice at time of death due to disease (spleen weight median, 1220 ± 401 mg; range, 420-1440 mg [n = 7]; WBC median, 103 ±151 × 10⁹/L [103 000 ± 151 000/μL]; range, 6-446 × 10⁹/L [6000-446 000/μL] [n = 7]; median survival ± standard error, 57 ± 60.2 days). Experiment was performed twice, once in the original outbred strain with wild-type littermate control and again with the _targeted *Stat5b* allele backcrossed to balb/c resulting in similar disease latency and severity. Black shapes indicate death due to severe MPD marked by leukocytosis and splenomegaly (WBC, > 50 × 10⁹/L [50 000/μL] and spleen weight, > 450 mg) at time of death due to disease. Shaded shapes represent moderate MPD (WBC, > 15 × 10⁹/L [15 000/μL] and/or spleen weight, > 450 mg) at time of death due to disease. Open shapes indicate animal found dead. GFP was detected in bone marrow, spleen, and peripheral blood of TPiGFP→*Stat5b*^−/− (37% ± 4% [n = 7]; 50% ± 15% [n = 7]; and 58% ± 32% [n = 7], respectively) and TPiGFP→*Stat5b*^+/+ (44% [n = 1]; 50% ± 15% [n = 3]; and 58% ± 32% [n = 3], respectively) recipient mice (data not shown). (B) Flow cytometric detection of mature myeloid (Gr-1⁺Mac-1⁺) cells in the spleens of both TPiGFP→*Stat5b*^+/+ and TPiGFP→*Stat5b*^−/− mice 33 days after transplantation. (C) Microscopic images of representative mice at time of death (*GFP*→*Stat5b*^+/+, 151 days after transplantation; TPiGFP→*Stat5b*^+/+, 29 days after transplantation; and TPiGFP→*Stat5b*^−/−, 29 days after transplantation). Panels show Wright-Giemsa–stained smears of peripheral blood (Ci-iii; 100×), and H&E–stained histologic sections of spleen (Civ-vi; 20×) and liver (Cvii-ix; 40×). These illustrate a normal morphology of peripheral blood, spleen, and liver in the *GFP*→*Stat5b*^+/+ group, whereas both TPiGFP→*Stat5b*^+/+ and TPiGFP→*Stat5b*^−/− show marked leukocytosis of maturing neutrophils in the peripheral blood, pronounced red pulp expansion by myeloid hyperplasia composed of predominantly maturing forms in the spleen, and sinusoidal and perivascular infiltrates of maturing granulocytic cells in the liver. Arrows indicate clusters of maturing myeloid cells in the liver. (TPiGFP indicates *TEL-PDGFRB* ires *eGFP*; MPD, myeloproliferative disease; WBC, peripheral white blood cell count; PB, peripheral blood; Sp, spleen; and Li, liver.)

**Figure 5**
***TEL-PDGFRB*–mediated myeloproliferative disease does not require Src family members *Lyn*, *Hck*, and *Fgr.***(A) Retroviral constructs encode *TEL-PDGFRB* followed by an internal ribosomal entry site to allow expression of a second cDNA, either *GFP* or *c-Src*. (B) Kaplan-Meier plot of recipient mouse survival when *TEL-PDGFRB* is coexpressed with either GFP (□) or *c-Src* (○) in Hck-, Lyn-, and Fgr-deficient cells. The 4 TPiGFP→*Lyn*^−/−*Hck*^−/−*Fgr*^−/− mice had varying degrees of disease severity (spleen weight, 445 ± 273 mg; range, 270-590 mg; median WBC, 38 ± 66 × 10⁹/L [38 000 ± 66 000/μL]; range, 14-156 × 10⁹/L [14 000-156 000/μL]). MPD was detected in 3 of 3 TPiSrc→ *Lyn*^−/−*Hck*^−/−*Fgr*^−/− mice analyzed for disease severity at time of death (spleen weight median, 590 ± 190 mg; range, 480-850 mg; median WBC, 86 ±839 × 10⁹/L [86 000 ± 839 000/μL]; range, 14-1502 × 10⁹/L [14 000-1 502 000 000/μL]). Black shapes indicate death due to severe MPD marked by leukocytosis and splenomegaly (WBC, > 50 × 10⁹/L [50 000/μL] and spleen weight, > 450 mg) at time of death due to disease. Shaded shapes represent moderate MPD (WBC, > 15 × 10⁹/L [15 000/μL] and/or spleen weight, > 450 mg) at time of death due to disease. Open shapes indicate animal found dead. (ires indicates internal ribosomal entry site; GFP, green fluorescent protein; LTR, long terminal repeat; PNT, pointed domain; TK, tyrosine kinase; MPD, myeloproliferative disease; and WBC, peripheral white blood cell count.)

See this image and copyright information in PMC

Cited by

Myeloid/Lymphoid Neoplasms with ETV6::PDGFRB Fusion Gene: A Rare Case of Poor Response to Imatinib and Possible Transformation Mechanisms from Myeloid Neoplasms of Bone Marrow to T-Cell Lymphoblastic Lymphoma Invasion in Lymph Nodes.
Gou Y, Tang Y, Liu S, Cheng S, Deng X, Wen Q, Feng Y, Peng X, Wang P, Zhang X. Gou Y, et al. J Inflamm Res. 2023 Nov 11;16:5163-5170. doi: 10.2147/JIR.S427995. eCollection 2023. J Inflamm Res. 2023. PMID: 38026242 Free PMC article.
Stat5 is critical for the development and maintenance of myeloproliferative neoplasm initiated by Nf1 deficiency.
Sachs Z, Been RA, DeCoursin KJ, Nguyen HT, Mohd Hassan NA, Noble-Orcutt KE, Eckfeldt CE, Pomeroy EJ, Diaz-Flores E, Geurts JL, Diers MD, Hasz DE, Morgan KJ, MacMillan ML, Shannon KM, Largaespada DA, Wiesner SM. Sachs Z, et al. Haematologica. 2016 Oct;101(10):1190-1199. doi: 10.3324/haematol.2015.136002. Epub 2016 Jul 14. Haematologica. 2016. PMID: 27418650 Free PMC article.
Effective _targeting of STAT5-mediated survival in myeloproliferative neoplasms using ABT-737 combined with rapamycin.
Li G, Miskimen KL, Wang Z, Xie XY, Tse W, Gouilleux F, Moriggl R, Bunting KD. Li G, et al. Leukemia. 2010 Aug;24(8):1397-405. doi: 10.1038/leu.2010.131. Epub 2010 Jun 10. Leukemia. 2010. PMID: 20535152 Free PMC article.
STAT5 requires the N-domain to maintain hematopoietic stem cell repopulating function and appropriate lymphoid-myeloid lineage output.
Li G, Wang Z, Zhang Y, Kang Z, Haviernikova E, Cui Y, Hennighausen L, Moriggl R, Wang D, Tse W, Bunting KD. Li G, et al. Exp Hematol. 2007 Nov;35(11):1684-94. doi: 10.1016/j.exphem.2007.08.026. Exp Hematol. 2007. PMID: 17976521 Free PMC article.
Constitutive activation of oncogenic PDGFRα-mutant proteins occurring in GIST patients induces receptor mislocalisation and alters PDGFRα signalling characteristics.
Bahlawane C, Eulenfeld R, Wiesinger MY, Wang J, Muller A, Girod A, Nazarov PV, Felsch K, Vallar L, Sauter T, Satagopam VP, Haan S. Bahlawane C, et al. Cell Commun Signal. 2015 Mar 31;13:21. doi: 10.1186/s12964-015-0096-8. Cell Commun Signal. 2015. PMID: 25880691 Free PMC article.

See all "Cited by" articles

References

1. Golub TR, Barker GF, Lovett M, Gilliland DG. Fusion of PDGF receptor beta to a novel ets-like gene, tel, in chronic myelomonocytic leukemia with t(5;12) chromosomal translocation. Cell. 1994;77:307–316. - PubMed
1. Carroll M, Tomasson MH, Barker GF, Golub TR, Gilliland DG. The TEL/platelet-derived growth factor beta receptor (PDGF beta R) fusion in chronic myelomonocytic leukemia is a transforming protein that self-associates and activates PDGF beta R kinase-dependent signaling pathways. Proc Natl Acad Sci U S A. 1996;93:14845–14850. - PMC - PubMed
1. Jousset C, Carron C, Boureux A, et al. A domain of TEL conserved in a subset of ETS proteins defines a specific oligomerization interface essential to the mitogenic properties of the TEL-PDGFR beta oncoprotein. EMBO J. 1997;16:69–82. - PMC - PubMed
1. Tran HH, Kim CA, Faham S, Siddall MC, Bowie JU. Native interface of the SAM domain polymer of TEL. BMC Struct Biol. 2002;2:5. - PMC - PubMed
1. Bourgeade MF, Defachelles AS, Cayre YE. Myc is essential for transformation by TEL/platelet-derived growth factor receptor beta (PDGFRbeta). Blood. 1998;91:3333–3339. - PubMed

Publication types

Actions
Actions

MeSH terms

Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions

Substances

Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions

Grants and funding

LinkOut - more resources

Full Text Sources
Medical
- MedlinePlus Health Information
Molecular Biology Databases
- Mouse Genome Informatics (MGI)
Research Materials
- NCI CPTC Antibody Characterization Program
Miscellaneous
- NCI CPTAC Assay Portal

[1] Golub TR, Barker GF, Lovett M, Gilliland DG. Fusion of PDGF receptor beta to a novel ets-like gene, tel, in chronic myelomonocytic leukemia with t(5;12) chromosomal translocation. Cell. 1994;77:307–316. - PubMed

[2] Golub TR, Barker GF, Lovett M, Gilliland DG. Fusion of PDGF receptor beta to a novel ets-like gene, tel, in chronic myelomonocytic leukemia with t(5;12) chromosomal translocation. Cell. 1994;77:307–316. - PubMed

[3] Carroll M, Tomasson MH, Barker GF, Golub TR, Gilliland DG. The TEL/platelet-derived growth factor beta receptor (PDGF beta R) fusion in chronic myelomonocytic leukemia is a transforming protein that self-associates and activates PDGF beta R kinase-dependent signaling pathways. Proc Natl Acad Sci U S A. 1996;93:14845–14850. - PMC - PubMed

[4] Carroll M, Tomasson MH, Barker GF, Golub TR, Gilliland DG. The TEL/platelet-derived growth factor beta receptor (PDGF beta R) fusion in chronic myelomonocytic leukemia is a transforming protein that self-associates and activates PDGF beta R kinase-dependent signaling pathways. Proc Natl Acad Sci U S A. 1996;93:14845–14850. - PMC - PubMed

[5] Jousset C, Carron C, Boureux A, et al. A domain of TEL conserved in a subset of ETS proteins defines a specific oligomerization interface essential to the mitogenic properties of the TEL-PDGFR beta oncoprotein. EMBO J. 1997;16:69–82. - PMC - PubMed

[6] Jousset C, Carron C, Boureux A, et al. A domain of TEL conserved in a subset of ETS proteins defines a specific oligomerization interface essential to the mitogenic properties of the TEL-PDGFR beta oncoprotein. EMBO J. 1997;16:69–82. - PMC - PubMed

[7] Tran HH, Kim CA, Faham S, Siddall MC, Bowie JU. Native interface of the SAM domain polymer of TEL. BMC Struct Biol. 2002;2:5. - PMC - PubMed

[8] Tran HH, Kim CA, Faham S, Siddall MC, Bowie JU. Native interface of the SAM domain polymer of TEL. BMC Struct Biol. 2002;2:5. - PMC - PubMed

[9] Bourgeade MF, Defachelles AS, Cayre YE. Myc is essential for transformation by TEL/platelet-derived growth factor receptor beta (PDGFRbeta). Blood. 1998;91:3333–3339. - PubMed

[10] Bourgeade MF, Defachelles AS, Cayre YE. Myc is essential for transformation by TEL/platelet-derived growth factor receptor beta (PDGFRbeta). Blood. 1998;91:3333–3339. - PubMed

Save citation to file

Email citation

Add to Collections

Add to My Bibliography

Your saved search

Create a file for external citation management software

Your RSS Feed

Myeloproliferative disease induced by TEL-PDGFRB displays dynamic range sensitivity to Stat5 gene dosage

Affiliation

Myeloproliferative disease induced by TEL-PDGFRB displays dynamic range sensitivity to Stat5 gene dosage

Authors

Affiliation

Abstract

Figures

Similar articles

Cited by

References

Publication types

MeSH terms

Substances

Grants and funding

LinkOut - more resources

Full Text Sources

Medical

Molecular Biology Databases

Research Materials

Miscellaneous

Abstract

Figures

Similar articles

Cited by

References

Publication types

MeSH terms

Substances

Related information

Grants and funding

LinkOut - more resources

Full Text Sources

Medical

Molecular Biology Databases

Research Materials

Miscellaneous