Dormancy in Metastatic Colorectal Cancer: Tissue Engineering Opportunities for Modeling.
3/5 보강
TL;DR
The current state of in vitro CRC dormancy models are summarized, highlighting the techniques utilized to give rise to dormant CRC cells: nutrient depletion, anticancer drugs, physical extracellular matrix interactions, and genetic manipulation.
OpenAlex 토픽 ·
Cancer Cells and Metastasis
3D Printing in Biomedical Research
Colorectal Cancer Surgical Treatments
The current state of in vitro CRC dormancy models are summarized, highlighting the techniques utilized to give rise to dormant CRC cells: nutrient depletion, anticancer drugs, physical extracellular m
APA
Sabrina N. VandenHeuvel, Lucia L. Nash, Shreya Raghavan (2026). Dormancy in Metastatic Colorectal Cancer: Tissue Engineering Opportunities for Modeling.. Tissue engineering. Part B, Reviews, 32(2), 126-142. https://doi.org/10.1089/ten.teb.2025.0009
MLA
Sabrina N. VandenHeuvel, et al.. "Dormancy in Metastatic Colorectal Cancer: Tissue Engineering Opportunities for Modeling.." Tissue engineering. Part B, Reviews, vol. 32, no. 2, 2026, pp. 126-142.
PMID
40195931 ↗
Abstract 한글 요약
Colorectal cancer (CRC) recurs at a striking rate, specifically in patients with liver metastasis. Dormant CRC cells disseminated following initial primary tumor resection or treatment often resurface years later to form aggressive, therapy-resistant tumors that result in high patient mortality. Routine imaging-based screenings often fail to detect dormant cancer cell clusters, and there are no overt symptomatic presentations, making dormant CRC a major clinical challenge to diagnose and treat. Tissue engineering approaches are ideally suited to model dormant cancer cells and enable the discovery of therapeutic vulnerabilities or unique mechanistic dependencies of dormant CRC. Emerging evidence suggests that tissue-engineered approaches have been successfully used to model dormant breast and lung cancer. With CRC responsible for the second most cancer-related deaths worldwide and CRC patients commonly experiencing recurrence, it is essential to expand dormancy models to understand this phenomenon in the context of CRC. Most published models of CRC dormancy simplify the complex tumor microenvironment with two-dimensional culture systems to elucidate dormancy-driving mechanisms. Building on this foundation, future research should apply tissue engineering methods to this growing field to generate competent three-dimensional models and increase mechanistic knowledge. This review summarizes the current state of CRC dormancy models, highlighting the techniques utilized to give rise to dormant CRC cells: nutrient depletion, anticancer drugs, physical extracellular matrix interactions, and genetic manipulation. The metrics used to validate dormancy within each model are also consolidated to demonstrate the lack of established standards and the ambiguity around comparing studies that have been validated differently. The methods of these studies are organized in this review to increase comprehensibility and identify needs and opportunities for future bioengineered models to address dormancy-driven mortality in patients with CRC liver metastasis.
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