Literature DB >> 21860377

Mammary transplantation of stromal cells and carcinoma cells in C57BL/6J mice.

Nikki Cheng1, Diana L Lambert.   

Abstract

The influence of stromal cells, including fibroblasts on mammary tumor progression has been well documented through the use of mouse models, in particular through transplantation of stromal cells and epithelial cells in the mammary gland of mice. Current transplantation models often involve the use of immunocompromised mice due to the different genetic backgrounds of stromal cells and epithelial cells. Extracellular matrices are often used to embed the two different cell types for consistent cell-cell interactions, but involve the use of Matrigel or rat tail collagen, which are immunogenic substrates. The lack of functional T cells from immunocompromised mice prevents accurate assessment of stromal cells on mammary tumor progression in vivo, with important implications on drug development and efficacy. Moreover, immunocompromised mice are costly, hard to breed and require special care conditions. To overcome these obstacles, we have developed an approach to orthotopically transplant stromal cell and epithelial cells into mice from the same genetic background to induce consistent tumor formation. This system involves harvesting normal, carcinoma associated fibroblasts, PyVmT mammary carcinoma cells and collagen from donor C57BL/6J mice. The cells are then embedded in collagen and transplanted in the inguinal mammary glands of female C57BL/6J mice. Transplantation of PyVmT cells alone form palpable tumors 30-40 days post transplantation. Endpoint analysis at 60 days indicates that co-transplantation with fibroblasts enhances mammary tumor growth compared to PyVmT cells transplanted alone. While cells and matrix from C57BL/6J mice were used in these studies, the isolation of cells and matrix and transplantation approach may be applied towards mice from different genetic backgrounds demonstrating versatility. In summary, this system may be used to investigate molecular interactions between stromal cells and epithelial cells, and overcomes critical limitations in immunocompromised mouse models.

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Year:  2011        PMID: 21860377      PMCID: PMC3211117          DOI: 10.3791/2716

Source DB:  PubMed          Journal:  J Vis Exp        ISSN: 1940-087X            Impact factor:   1.355


  18 in total

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Authors:  Shira Bernard; Megan Myers; Wei Bin Fang; Brandon Zinda; Curtis Smart; Diana Lambert; An Zou; Fang Fan; Nikki Cheng
Journal:  J Mammary Gland Biol Neoplasia       Date:  2018-08-09       Impact factor: 2.673

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Authors:  Gage Brummer; Diana S Acevedo; Qingting Hu; Mike Portsche; Wei Bin Fang; Min Yao; Brandon Zinda; Megan Myers; Nehemiah Alvarez; Patrick Fields; Yan Hong; Fariba Behbod; Nikki Cheng
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Authors:  Min Yao; Wei Fang; Curtis Smart; Qingting Hu; Shixia Huang; Nehemiah Alvarez; Patrick Fields; Nikki Cheng
Journal:  Mol Cancer Res       Date:  2018-11-16       Impact factor: 5.852

4.  Ex vivo Live Imaging of Lung Metastasis and Their Microenvironment.

Authors:  Renske J E van den Bijgaart; Niwen Kong; Carrie Maynard; Vicki Plaks
Journal:  J Vis Exp       Date:  2016-02-03       Impact factor: 1.355

5.  Live imaging of drug responses in the tumor microenvironment in mouse models of breast cancer.

Authors:  Elizabeth S Nakasone; Hanne A Askautrud; Mikala Egeblad
Journal:  J Vis Exp       Date:  2013-03-24       Impact factor: 1.355

6.  TGF-β Negatively Regulates CXCL1 Chemokine Expression in Mammary Fibroblasts through Enhancement of Smad2/3 and Suppression of HGF/c-Met Signaling Mechanisms.

Authors:  Wei Bin Fang; Benford Mafuvadze; Min Yao; An Zou; Mike Portsche; Nikki Cheng
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7.  Targeted gene silencing of CCL2 inhibits triple negative breast cancer progression by blocking cancer stem cell renewal and M2 macrophage recruitment.

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  7 in total

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