| Literature DB >> 25771018 |
Yukie Yoshii1, Takako Furukawa2, Atsuo Waki2, Hiroaki Okuyama3, Masahiro Inoue3, Manabu Itoh4, Ming-Rong Zhang2, Hidekatsu Wakizaka2, Chizuru Sogawa5, Yasushi Kiyono6, Hiroshi Yoshii7, Yasuhisa Fujibayashi2, Tsuneo Saga2.
Abstract
Anti-cancer drug development typically utilizes high-throughput screening with two-dimensional (2D) cell culture. However, 2D culture induces cellular characteristics different from tumors in vivo, resulting in inefficient drug development. Here, we report an innovative high-throughput screening system using nanoimprinting 3D culture to simulate in vivo conditions, thereby facilitating efficient drug development. We demonstrated that cell line-based nanoimprinting 3D screening can more efficiently select drugs that effectively inhibit cancer growth in vivo as compared to 2D culture. Metabolic responses after treatment were assessed using positron emission tomography (PET) probes, and revealed similar characteristics between the 3D spheroids and in vivo tumors. Further, we developed an advanced method to adopt cancer cells from patient tumor tissues for high-throughput drug screening with nanoimprinting 3D culture, which we termed Cancer tissue-Originated Uniformed Spheroid Assay (COUSA). This system identified drugs that were effective in xenografts of the original patient tumors. Nanoimprinting 3D spheroids showed low permeability and formation of hypoxic regions inside, similar to in vivo tumors. Collectively, the nanoimprinting 3D culture provides easy-handling high-throughput drug screening system, which allows for efficient drug development by mimicking the tumor environment. The COUSA system could be a useful platform for drug development with patient cancer cells.Entities:
Keywords: 3D cell culture; High-throughput drug screening; Hypoxia; Nanoimprinting technology; Spheroid
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Year: 2015 PMID: 25771018 DOI: 10.1016/j.biomaterials.2015.02.008
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479