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Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation
Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation
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Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation
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Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation
Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation

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Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation
Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation
Journal Article

Characterizing viscoelastic properties of breast cancer tissue in a mouse model using indentation

2018
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Overview
Breast cancer is one of the leading cancer forms affecting females worldwide. Characterizing the mechanical properties of breast cancer tissue is important for diagnosis and uncovering the mechanobiology mechanism. Although most of the studies were based on human cancer tissue, an animal model is still describable for preclinical analysis. Using a custom-build indentation device, we measured the viscoelastic properties of breast cancer tissue from 4T1 and SKBR3 cell lines. A total of 7 samples were tested for each cancer tissue using a mouse model. We observed that a viscoelastic model with 2-term Prony series could best describe the ramp and stress relaxation of the tissue. For long-term responses, the SKBR3 tissues were stiffer in the strain levels of 4–10%, while no significant differences were found for the instantaneous elastic modulus. We also found tissues from both cell lines appeared to be strain-independent for the instantaneous elastic modulus and for the long-term elastic modulus in the strain level of 4–10%. In addition, by inspecting the cellular morphological structure of the two tissues, we found that SKBR3 tissues had a larger volume ratio of nuclei and a smaller volume ratio of extracellular matrix (ECM). Compared with prior cellular mechanics studies, our results indicated that ECM could contribute to the stiffening the tissue-level behavior. The viscoelastic characterization of the breast cancer tissue contributed to the scarce animal model data and provided support for the linear viscoelastic model used for in vivo elastography studies. Results also supplied helpful information for modeling of the breast cancer tissue in the tissue and cellular levels.