A New Approach to Cancer Therapy: The Tumor Microenvironment as Target

Schwendener, Reto A.; Mete, Sibel

doi:10.2174/9781608057986113010003

Cited by 2 publications

(3 citation statements)

References 402 publications

(448 reference statements)

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“…This is expected due to the high percentage of monoclonal cells present within BM from which the constructs were originally derived and the relatively simple type I collagen hydrogels in which they were seeded. These high myeloma constructs indicated the importance of the in vivo tumor microniche for the in vitro study of long-lived plasma cells because without these essential components or additional factors introduced, plasma cells are unable to survive for 5 days in vitro (Cassese et al, 2003; Arce et al, 2004; Cretu & Brooks, 2007; Schwendener & Mete, 2014).…”

Section: Discussionmentioning

confidence: 99%

“…Previous studies have demonstrated that in order to maintain their phenotype in culture, PCs require components of the tumor microenvironment such as survival factors and/or BM stromal cells (Cassese et al, 2003; Wardemann et al, 2004; Cretu & Brooks, 2007; Wols et al, 2014). These reports have also indicated the importance of IL-6 for the maintenance of plasma cells in vitro as well as playing a key role in the pathogenesis in myeloma cells (Scheller et al, 2011; Schwendener & Mete, 2014). Thus, new models are necessary to investigate the molecular mechanisms that regulate PC homeostasis.…”

Section: Introductionmentioning

confidence: 98%

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Structural and Ultrastructural Analysis of the Multiple Myeloma Cell Niche and a Patient-Specific Model of Plasma Cell Dysfunction

et al. 2021

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Multiple myeloma (MM) is a deadly, incurable malignancy in which antibody-secreting plasma cells (PCs) become neoplastic. Previous studies have shown that the PC niche plays a role cancer progression. Bone marrow (BM) cores from MM and a premalignant condition known as monoclonal gammopathy of unknown significance (MGUS) patients were analyzed with confocal and transmission electron microscopy. The BM aspirates from these patients were used to generate 3D PC cultures. These in vitro cultures were then assayed for the molecular, cellular, and ultrastructural hallmarks of dysfunctional PC at days 1 and 5. In vivo, evidence of PC endoplasmic reticulum stress was found in both MM and MGUS BM; however, evidence of PC autophagy was found only in MM BM. Analysis of in vitro cultures found that MM PC can survive and maintain a differentiated phenotype over an unprecedented 5 days, had higher levels of paraprotein production when compared to MGUS-derived cultures, and showed evidence of PC autophagy as well. Increased fibronectin deposition around PC associated with disease severity and autophagy dysregulation was also observed. 3D cultures constructed from BM aspirates from MGUS and MM patients allow for long-term culture of functional PC while maintaining their distinct morphological phenotypes.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 98%

Structural and Ultrastructural Analysis of the Multiple Myeloma Cell Niche and a Patient-Specific Model of Plasma Cell Dysfunction

et al. 2021

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“…(15,16) Tumor associated macrophages (TAM) is a major component of the inflammatory cells those infiltrate in the tumor microenvironment, derived from the white blood cells from bone marrow and evolved from peripheral blood monocytes. (17) Studies have shown that there are two polarization types of TAM in different environmental conditions, i.e., M1 and M2. (18) Among them, M2 polarization inhibits the anti-tumor immune response and releases various factors, to directly or indirectly promote tumor angiogenesis, tumor growth and tumor metastasis.…”

mentioning

confidence: 99%

ETV1 inhibition depressed M2 polarization of tumor-associated macrophage and cell process in gastrointestinal stromal tumor via down-regulating PDE3A

Guo

Wan

et al. 2023

J. Clin. Biochem. Nutr.

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M2-type polarization of tumor associated-macrophage (TAM) is involved in the malignancy of gastrointestinal stromal tumor (GIST) progression. ETS variant 1 (ETV1) has been previously validated to regulate GIST pathogenesis. Our study intended to explore the role and mechanism of ETV1 in mediating the M2polarization of TAM in GIST progression. First, we analyzed the correlation between ETV1 expression and M2-polarization in GIST tissues. IL-4 was used to treat THP-1-derived TAM cells and IL-4stimulated TAM were co-cultured with GIST-T1 cells to mimic the GIST microenvironment. A loss-of-function assay was performed to explore the role of ETV1. Results showed that ETV1 elevation was positively correlated with M2-polarization. IL-4-induced TAM promoted ETV1 expression, silencing ETV1 inhibited proliferation, invasion and KIT activation in IL-4-treated GIST cells, while cell apoptosis was enhanced. Besides, co-culture of ETV1-silenced GIST cells significantly depressed M2-polarization in TAM, presented as decreased levels of CD206, Agr-1 and cytokines, as well as the proportion of CD206-positive TAM. PDE3A was positively correlated with ETV1 and M2-polarization. Overexpressing PDE3A reversed the inhibitory effects of ETV1 silencing. Generally, ETV1 inhibition depressed M2-polarization of TAM in GIST and its promotion on pathological aggravation via down-regulating PDE3A. This evidence may provide a new target for GIST regulation.

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A New Approach to Cancer Therapy: The Tumor Microenvironment as Target

Cited by 2 publications

References 402 publications

Structural and Ultrastructural Analysis of the Multiple Myeloma Cell Niche and a Patient-Specific Model of Plasma Cell Dysfunction

Structural and Ultrastructural Analysis of the Multiple Myeloma Cell Niche and a Patient-Specific Model of Plasma Cell Dysfunction

ETV1 inhibition depressed M2 polarization of tumor-associated macrophage and cell process in gastrointestinal stromal tumor via down-regulating PDE3A

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