[HTML][HTML] Growth and characterization of irradiated organoids from mammary glands
BC Hacker, JD Gomez, CAS Batista… - Journal of visualized …, 2019 - ncbi.nlm.nih.gov
Journal of visualized experiments: JoVE, 2019•ncbi.nlm.nih.gov
Organoids derived from the digested tissue are multicellular three-dimensional (3D)
constructs that better recapitulate in vivo conditions than cell monolayers. Although they
cannot completely model in vivo complexity, they retain some functionality of the original
organ. In cancer models, organoids are commonly used to study tumor cell invasion. This
protocol aims to develop and characterize organoids from the normal and irradiated mouse
mammary gland tissue to evaluate the radiation response in normal tissues. These …
constructs that better recapitulate in vivo conditions than cell monolayers. Although they
cannot completely model in vivo complexity, they retain some functionality of the original
organ. In cancer models, organoids are commonly used to study tumor cell invasion. This
protocol aims to develop and characterize organoids from the normal and irradiated mouse
mammary gland tissue to evaluate the radiation response in normal tissues. These …
Abstract
Organoids derived from the digested tissue are multicellular three-dimensional (3D) constructs that better recapitulate in vivo conditions than cell monolayers. Although they cannot completely model in vivo complexity, they retain some functionality of the original organ. In cancer models, organoids are commonly used to study tumor cell invasion. This protocol aims to develop and characterize organoids from the normal and irradiated mouse mammary gland tissue to evaluate the radiation response in normal tissues. These organoids can be applied to future in vitro cancer studies to evaluate tumor cell interactions with irradiated organoids. Mammary glands were resected, irradiated to 20 Gy and digested in a collagenase VIII solution. Epithelial organoids were separated via centrifugal differentiation, and 3D organoids were developed in 96-well low-adhesion microplates. Organoids expressed the characteristic epithelial marker cytokeratin 14. Macrophage interaction with the organoids was observed in co-culture experiments. This model may be useful for studying tumor-stromal interactions, infiltration of immune cells, and macrophage polarization within an irradiated microenvironment.
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