Murine but Not Human Mesenchymal Stem Cells Generate Osteosarcoma-Like Lesions in the Lung

Aguilar, Susana; Nye, Emma; Chan, Jerry Kok Yen; Loebinger, Michael R.; Spencer‐Dene, Bradley; Fisk, Nick; Stamp, Gordon; Bonnet, Dominique; Janes, Sam M.

doi:10.1634/stemcells.2006-0762

Cited by 177 publications

(146 citation statements)

References 40 publications

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“…Similar to our data, the expression of EWS-FLI-1 was able to transform BM-mMSC [3] but unable to transform BM-hMSCs although it induced a gene expression profile resembling features of Ewing's Sarcomas [7]. Moreover, mMSCs but not hMSCs generated osteosarcoma-like lesions in the lung following systemic injection in mice [48]. These data confirm that mMSCs are much more susceptible to transformation and sarcoma development [49] than hMSCs, which seem to require additional cooperating mutations to constitute a useful cellular model for sarcomagenesis.…”

Section: Discussionsupporting

confidence: 89%

FUS-CHOP Fusion Protein Expression Coupled to p53 Deficiency Induces Liposarcoma in Mouse but Not in Human Adipose-Derived Mesenchymal Stem/Stromal Cells

et al. 2011

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Human sarcomas have been modeled in mice by expression of specific fusion genes in mesenchymal stem cells (MSCs). However, sarcoma models based on human MSCs are still missing. We attempted to develop a model of liposarcoma by expressing FUS (FUsed in Sarcoma; also termed TLS, Translocated in LipoSarcoma)-CHOP (C/ EBP HOmologous Protein; also termed DDIT3, DNA Damage-Inducible Transcript 3), a hallmark mixoid liposarcoma-associated fusion oncogene, in wild-type and p53-deficient mouse and human adipose-derived mesenchymal stem/stromal cells (ASCs). FUS-CHOP induced liposarcoma-like tumors when expressed in p53 2/2 but not in wild-type (wt) mouse ASCs (mASCs). In the absence of FUS-CHOP, p53 2/2 mASCs forms leiomyosarcoma, indicating that the expression of FUS-CHOP redirects the tumor genesis/phenotype. FUS-CHOP expression in wt mASCs does not initiate sarcomagenesis, indicating that p53 deficiency is required to induce FUS-CHOP-mediated liposarcoma in fat-derived mASCs. In a human setting, p53-deficient human ASCs (hASCs) displayed a higher in vitro growth rate and a more extended lifespan than wt hASCs. However, FUS-CHOP expression did not induce further changes in culture homeostasis nor initiated liposarcoma in either wt or p53-depleted hASCs. These results indicate that FUS-CHOP expression in a p53-deficient background is sufficient to initiate liposarcoma in mouse but not in hASCs, suggesting the need of additional cooperating mutations in hASCs. A microarray gene expression profiling has shed light into the potential deregulated pathways in liposarcoma formation from p53-deficient mASCs expressing FUS-CHOP, which might also function as potential cooperating mutations in the transformation process from hASCs. STEM CELLS 2011; 29:179-192 Disclosure of potential conflicts of interest is found at the end of this article.

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Section: Discussionsupporting

confidence: 89%

FUS-CHOP Fusion Protein Expression Coupled to p53 Deficiency Induces Liposarcoma in Mouse but Not in Human Adipose-Derived Mesenchymal Stem/Stromal Cells

et al. 2011

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“…The resulting MSC, when implanted into immunecompromised mice using hydroxyapatite/tricalcium phosphate as a carrier, as well as when injected into the tail vein led to sarcoma formation (Miura et al, 2006). Murine MSC also rapidly acquire chromosomal abnormalities in culture, and after infusion, these cells invaded lung parenchyma and formed tumor nodules with the characteristics of differentiated osteosarcomas (Aguilar et al, 2007). Compared to murine MSC, human MSC in long-term culture greatly differ in their behavior.…”

Section: Msc and Transformation Riskmentioning

confidence: 99%

Controversial issue: Is it safe to employ mesenchymal stem cells in cell-based therapies?

Lepperdinger

Brunauer

Jamnig

et al. 2008

Experimental Gerontology

113

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“…Furthermore, the immunosuppressive effects of human SPC are more potent, with effects seen at much lower SPC to responder ratios than required for similar murine SPC studies. (Di Nicola et al, 2002;Krampera et al, 2003) There are also cell dose limitations with intravenous administration of murine SPCs due to acute pulmonary embolism (Gao et al, 2001;Aguilar et al, 2007) related to their smaller pulmonary vascular bed. This limited our ability to administer even higher doses of SPCs to assess dose effects.…”

Section: A T Badillo Et Al ª 2008 the Authorsmentioning

confidence: 99%

Murine bone marrow derived stromal progenitor cells fail to prevent or treat acute graft‐versus‐host disease

Badillo¹,

Peranteau²,

Heaton

et al. 2008

Br J Haematol

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SummaryHuman and murine stromal progenitor cells (SPCs) can suppress alloresponse in vitro, suggesting that SPCs may have clinical application toward prevention or treatment of graft‐versus‐host disease (GVHD). However, th eresults of in vivo studies have been conflicting. This study utilized an established murine model of acute GVHD to assess the ability of bone marrow derived murine SPCs (mSPCs) to prevent or treat GVHD. GVHD was established by transplantation of B6 bone marrow and spleen cells into lethally irradiated (900 cGy) B6 × BALB/c F1 recipients. mSPCs were administered using various dose and timing protocols designed to either prevent or treat GVHD. After transplantation, mice were monitored daily for weight and survival. Differences in symptom severity were compared using a clinical GVHD scoring system. All GVHD control mice died of lethal GVHD. All groups treated with mSPCs for the prevention of GVHD went on to develop clinical GVHD with no alteration of the disease course or severity compared to controls. Administration of mSPC after the development of GVHD failed to improve the disease course. We conclude that in this model, the ability of SPCs to suppress alloresponse in vitro does not correlate with in vivo prevention or treatment of acute GVHD.

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Murine but Not Human Mesenchymal Stem Cells Generate Osteosarcoma-Like Lesions in the Lung

Cited by 177 publications

References 40 publications

FUS-CHOP Fusion Protein Expression Coupled to p53 Deficiency Induces Liposarcoma in Mouse but Not in Human Adipose-Derived Mesenchymal Stem/Stromal Cells

FUS-CHOP Fusion Protein Expression Coupled to p53 Deficiency Induces Liposarcoma in Mouse but Not in Human Adipose-Derived Mesenchymal Stem/Stromal Cells

Controversial issue: Is it safe to employ mesenchymal stem cells in cell-based therapies?

Murine bone marrow derived stromal progenitor cells fail to prevent or treat acute graft‐versus‐host disease

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