Literature DB >> 22016821

AMD3100-mediated production of interleukin-1 from mesenchymal stem cells is key to chemosensitivity of breast cancer cells.

Steven J Greco, Shyam A Patel, Margarette Bryan, Lillian F Pliner, Debabrata Banerjee, Pranela Rameshwar.   

Abstract

Breast cancer cells (BCCs) can remain quiescent for a long period, before detection and during remission. Mesenchymal stem cells (MSCs) exert both protective and growth support of BCCs. Intercellular interactions between MSCs and BCCs partly occur through membrane-bound CXCL12 (SDF-1α) and its receptor, CXCR4. MSCs can protect BCCs by suppressing immune cytotoxicity and concomitant induction of regulatory T-cells. This study investigated how the cellular interactions between MSCs and BCCs can be targeted to sensitize the BCCs to chemotherapy. Knockdown of CXCR4 and CXCL12 indicated that these molecules are involved in reduced proliferation of MDA-MB-231 and T47D BCCs. We therefore treated co-cultures of MSCs and BCCs with the CXCR4 antagonist, AMD3100, and showed that this treatment led to cycling of BCCs with increased sensitivity to carboplatin, although the effectiveness of carboplatin required the presence of AMD3100. Cytokine array analyses and transwell cultures indicated that AMD3100 caused an increase in BCC proliferation by inducing the production of IL-1α and IL-1β in MSCs after uncoupling from BCCs. The findings with cell lines were validated with primary BCCs from the blood of patients, and in nude BALB/ c mice. MDA-MB-231 was injected in the dorsal flank of mice. The tumors were treated with IL-1 receptor antagonist, AMD3100 and/ or carboplatin. The results verified a critical role for IL-1 in transitioning MSCs from protective to supportive with respect to BCC growth. The clinical significance of these studies was further highlighted in preliminary studies that detected circulating MSCs in obese, but not non-obese patients. Since obese breast cancer patients show poor outcome, these findings underscore that importance of MSCs in consideration for future development of efficient therapy.

Entities:  

Keywords:  AMD3100; CXCR4; breast cancer; interleukin-1; mesenchymal stem cells

Year:  2011        PMID: 22016821      PMCID: PMC3195931     

Source DB:  PubMed          Journal:  Am J Cancer Res        ISSN: 2156-6976            Impact factor:   6.166


  44 in total

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Review 2.  Circulating and disseminated tumor cells.

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4.  Gap junction-mediated import of microRNA from bone marrow stromal cells can elicit cell cycle quiescence in breast cancer cells.

Authors:  Philip K Lim; Sarah A Bliss; Shyam A Patel; Marcelo Taborga; Meneka A Dave; Larissa A Gregory; Steven J Greco; Margarette Bryan; Prem S Patel; Pranela Rameshwar
Journal:  Cancer Res       Date:  2011-02-22       Impact factor: 12.701

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  20 in total

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2.  Steroid-Mediated Decrease in Blood Mesenchymal Stem Cells in Liver Transplant could Impact Long-Term Recovery.

Authors:  Nykia D Walker; Yasmine Mourad; Katherine Liu; Michael Buxhoeveden; Catherine Schoenberg; Jean D Eloy; Dorian J Wilson; Lloyd G Brown; Andrei Botea; Faraz Chaudhry; Steven J Greco; Nicholas M Ponzio; Nikolaos Pyrsopoulos; Baburao Koneru; Yuriy Gubenko; Pranela Rameshwar
Journal:  Stem Cell Rev Rep       Date:  2017-10       Impact factor: 5.739

3.  Treg/Th17 polarization by distinct subsets of breast cancer cells is dictated by the interaction with mesenchymal stem cells.

Authors:  Shyam A Patel; Meneka A Dave; Sarah A Bliss; Agata B Giec-Ujda; Margarette Bryan; Lillian F Pliner; Pranela Rameshwar
Journal:  J Cancer Stem Cell Res       Date:  2014-05-29

4.  Exosomes in the Healthy and Malignant Bone Marrow Microenvironment.

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6.  Sodium Tungstate for Promoting Mesenchymal Stem Cell Chondrogenesis.

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Review 8.  The mesenchymal tumor microenvironment: a drug-resistant niche.

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Review 9.  Chemokines orchestrate tumor cells and the microenvironment to achieve metastatic heterogeneity.

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Journal:  Cancer Metastasis Rev       Date:  2021-05-06       Impact factor: 9.264

10.  MiR-139 Modulates Cancer Stem Cell Function of Human Breast Cancer through Targeting CXCR4.

Authors:  Chun-Wen Cheng; Wen-Ling Liao; Po-Ming Chen; Jyh-Cherng Yu; Hui-Ping Shiau; Yi-Hsien Hsieh; Huei-Jane Lee; Yu-Chun Cheng; Pei-Ei Wu; Chen-Yang Shen
Journal:  Cancers (Basel)       Date:  2021-05-25       Impact factor: 6.639

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