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A Novel In Vivo Rat Mesentery Model for Studying Tumor Spheroid-Induced Microvascular Remodeling. | LitMetric

AI Article Synopsis

  • The tumor microenvironment consists of cancer cells and various host cells, prompting the development of models to study cell interactions.
  • The study utilized a tumor spheroid-rat mesentery model to observe how tumor spheroids affect blood and lymphatic vessel remodeling after being transplanted onto rat tissues.
  • Results showed that tumor spheroids increased vascular density and connections, demonstrating the model's relevance for understanding tumor-induced vascular changes.

Article Abstract

Introduction: The tumor microenvironment is comprised of neoplastic cells and a variety of host cell types. Investigation of cell dynamics within this environment has motivated in vitro and ex vivo biomimetic model development. Our lab recently introduced the tumor spheroid-rat mesentery model to investigate cancer-induced lymphatic/blood vessel remodeling. To validate the physiological relevance of this model, the objective of this study was to determine the effect of tumor spheroids on microvascular remodeling after transplantation onto rat mesenteric.

Methods: Spheroids derived from H1299 lung cancer cells were seeded onto rat mesenteric tissues during a survival surgical procedure. Tissues were harvested 3-5 days post-seeding and stained with PECAM and LYVE-1 to identify blood and lymphatic vessels respectively.

Results: At all timepoints, cancer cells remained adhered to the tissue. Tissues seeded with tumor spheroids were shown to have increased vascular density, capillary sprouting, and tortuosity compared to sham tissues exposed to sterile saline only. Tumor spheroids also induced the formation of lymphatic/blood vessel connections and LYVE-1 negative protrusions emerging from lymphatic vessels.

Conclusion: Overall, this study underscores the use of in vivo modeling to aid in the discovery of novel vascular growth dynamics and offers new methodologies for studying tumor-induced remodeling.

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Source
http://dx.doi.org/10.1159/000543011DOI Listing

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