Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation

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Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation Publisher Pubmed

Bahrambeigi V^{1, 2} ; Ahmadi N¹ ; Salehi R² ; Javanmard SH^{1, 3}

Source: Immunological Investigations Published:2015

Abstract

Adipose-derived mesenchymal stem cells (ADSCs) are attractive tools for cancer gene therapy due to their intrinsic tropism to the tumor environment. Interleukin-2 (IL2) is recognized as a key regulatory molecule, which enhances the activity and growth of the immune effector cell function. High-Dose IL2 Therapy is an option for treatment of malignant melanoma but has frequent, often serious and sometimes life-threatening side effects. Here we investigated the effect of genetically modified ADSCs (GM-ADSCs) expressing IL2 in immunocompetent mouse models of subcutaneous and lung metastatic melanoma. Prior to in vivo studies, we demonstrated that IL2 produced by GM-ADSCs may act as a growth factor for melanoma cells due to the increased viability and reduced apoptosis of melanoma cells after in vitro treatment. Subcutaneous co-injection of IL2-expressing ADSCs with melanoma cells significantly enhanced the melanoma tumor growth. Furthermore, histological analysis of subcutaneous tumors for IL2 and Melan-A (a melanocytic differentiation marker) confirmed that most of cells in melanoma/IL2-ADSC co-injected tumors are melanoma cells, not IL2-ADSCs. In pulmonary metastases model, melanoma cells were injected intravenously and 10 days later mice were treated by systematical injection of GM-ADSCs. Intravenously injected IL2-ADSCs engrafted into melanoma lung tumors but were unable to reduce melanoma lung metastases. Besides, administered IL2-ADSCs significantly reduced systemic CD4+ cells and did not impact the total survival of lung metastases melanoma bearing mice. In conclusion, this study showed that IL2-producing ADSCs can favor B16F10 melanoma cell proliferation. Therefore, therapies utilizing IL2 have to be taken into careful consideration. © 2015 Informa Healthcare USA, Inc. All rights reserved: reproduction in whole or part not permitted.

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Style	Citing Format
MLA	Bahrambeigi V, et al.. "Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation." Immunological Investigations, vol. 44, no. 3, 2015, pp. 216-236.
APA	Bahrambeigi V, Ahmadi N, Salehi R, Javanmard SH (2015). Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation. Immunological Investigations, 44(3), 216-236.
Chicago	Bahrambeigi V, Ahmadi N, Salehi R, Javanmard SH. "Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation." Immunological Investigations 44, no. 3 (2015): 216-236.
Harvard	Bahrambeigi V et al. (2015) 'Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation', Immunological Investigations, 44(3), pp. 216-236.
Vancouver	Bahrambeigi V, Ahmadi N, Salehi R, Javanmard SH. Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation. Immunological Investigations. 2015;44(3):216-236.
BibTex	@article{ author = {Bahrambeigi V and Ahmadi N and Salehi R and Javanmard SH}, title = {Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation}, journal = {Immunological Investigations}, volume = {44}, number = {3}, pages = {216-236}, year = {2015} }
RIS	TY - JOUR AU - Bahrambeigi V AU - Ahmadi N AU - Salehi R AU - Javanmard SH TI - Genetically Modified Murine Adipose-Derived Mesenchymal Stem Cells Producing Interleukin-2 Favor B16f10 Melanoma Cell Proliferation JO - Immunological Investigations VL - 44 IS - 3 SP - 216 EP - 236 PY - 2015 ER -

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