Literature DB >> 24176801

Shape in migration: quantitative image analysis of migrating chemoresistant HCT-8 colon cancer cells.

Alessia Pasqualato1, Vittorio Lei2, Alessandra Cucina3, Simona Dinicola4, Fabrizio D'Anselmi5, Sara Proietti4, Maria Grazia Masiello4, Alessandro Palombo6, Mariano Bizzarri7.   

Abstract

Unsuccessful cytotoxic anticancer treatments may contribute to tumor morphologic instability and consequent tissue invasion, promoting the selection of a more malignant phenotype. Indeed, morphological changes have been demonstrated to be more pronounced in strongly vs. weakly metastatic cells. By means of normalized bending energy, we have previously quantitatively defined the link between cell shape modifications and the acquisition of a more malignant phenotype by 5-FU-resistant colon cancer cells (HCT-8FUres). Such changes were significantly correlated with an increase in motility speed. Herein, we propose a method to quantitatively analyze the shape of wild and chemoresistant HCT-8 migration front cells during wound healing assay. We evaluated the reliability of parameters (area/perimeter ratio [A/p], circularity, roundness, fractal dimension, and solidity) in describing the biological behavior of the two cell lines, enabling hence in distinguishing the chemoresistant line from the other one. We found solidity index the parameter that better described the difference between chemoresistant and wild cells. Moreover, solidity is able to capture the differences between chemoresistant and wild cells at each time point of the migration process. Indeed, motility speed was found to be inversely correlated with solidity, a quantitative index of cell deformability. Deformability is an outstanding hallmark of the process leading to metastatic spread; consequently, solidity may be considered a marker of acquired metastatic property.

Entities:  

Keywords:  cell shape; chemoresistance; deformability; metastasis; solidity; wound healing assay

Mesh:

Substances:

Year:  2013        PMID: 24176801      PMCID: PMC3903690          DOI: 10.4161/cam.26765

Source DB:  PubMed          Journal:  Cell Adh Migr        ISSN: 1933-6918            Impact factor:   3.405


  37 in total

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