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Differential regulation of EMT-related pathways by inflammatory microenvironment in 3D prostate spheroids and tumor-stroma interaction models.

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Experimental cell research 📖 저널 OA 7.9% 2022: 0/3 OA 2023: 0/2 OA 2024: 0/7 OA 2025: 1/26 OA 2026: 5/36 OA 2022~2026 2026 Vol.457(2) p. 114962 Cancer Cells and Metastasis
TL;DR The optimized 3D spheroid and co-culture models provide a robust and powerful platform to unravel the functional consequences of inflammation and offer mechanistic insight into cellular processes underlying PCa progression, supporting the development of targeted therapeutic strategies.
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PubMed DOI OpenAlex Semantic 마지막 보강 2026-04-30
OpenAlex 토픽 · Cancer Cells and Metastasis Prostate Cancer Treatment and Research Mathematical Biology Tumor Growth

Calisir FGA, Arziman S, Isel E, Debelec Butuner B

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The optimized 3D spheroid and co-culture models provide a robust and powerful platform to unravel the functional consequences of inflammation and offer mechanistic insight into cellular processes unde

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APA Fersu G.A. CALISIR, Suleyman Arziman, et al. (2026). Differential regulation of EMT-related pathways by inflammatory microenvironment in 3D prostate spheroids and tumor-stroma interaction models.. Experimental cell research, 457(2), 114962. https://doi.org/10.1016/j.yexcr.2026.114962
MLA Fersu G.A. CALISIR, et al.. "Differential regulation of EMT-related pathways by inflammatory microenvironment in 3D prostate spheroids and tumor-stroma interaction models.." Experimental cell research, vol. 457, no. 2, 2026, pp. 114962.
PMID 41765160 ↗

Abstract

Chronic inflammation plays a major role in the initiation, progression, and metastasis of prostate cancer (PCa) by driving tumorigenic processes such as Epithelial-Mesenchymal Transition (EMT). To investigate these mechanisms in physiologically relevant settings, we optimized two complementary in vitro tumor models: 3D prostate spheroids that mimics multicellular interactions and an epithelial-myofibroblast co-culture system that reflects key tumor-stroma dynamics under inflammatory conditions. Our optimization revealed that successful spheroid formation depends on cell line-specific molecular features rather than a universal spheroid size. Compared with conventional 2D cultures, inflammatory stimuli modulated EMT mediators significantly in a cell line-dependent manner; notably, fibronectin, vimentin, and TWIST1 were differentially regulated in 3D spheroids, indicating enhanced invasive features driven by inflammatory cues. The co-culture model successfully represented reactive stroma formation, and stromal influence dramatically shaped inflammation-induced anoikis resistance and cell migration. Overall, our findings demonstrated that tumor-stroma interactions critically contribute to the impact of inflammation on EMT in PCa. Our optimized 3D spheroid and co-culture models provide a robust and powerful platform to unravel the functional consequences of inflammation and offer mechanistic insight into cellular processes underlying PCa progression, supporting the development of targeted therapeutic strategies.

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