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Three-Dimensional Tumor Spheroids of Pancreatic and Colorectal Cancer Cell Lines for High-Throughput Screening of Drug Candidates.

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ACS omega 📖 저널 OA 100% 2021: 1/1 OA 2022: 1/1 OA 2023: 5/5 OA 2024: 4/4 OA 2025: 53/53 OA 2026: 70/70 OA 2021~2026 2025 Vol.10(48) p. 58194-58204
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Trofimov M, Bulatov I, Donskaia I, Efremov A, Litau E, Lavrinenko V, Popov V, Petrova V, Bukatin A, Tyazhelnikov S

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Over the past decade, three-dimensional (3D) cancer models have emerged as crucial tools in high-throughput screening (HTS), providing a more reliable bridge between in vitro and in vivo drug testing.

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APA Trofimov M, Bulatov I, et al. (2025). Three-Dimensional Tumor Spheroids of Pancreatic and Colorectal Cancer Cell Lines for High-Throughput Screening of Drug Candidates.. ACS omega, 10(48), 58194-58204. https://doi.org/10.1021/acsomega.5c03607
MLA Trofimov M, et al.. "Three-Dimensional Tumor Spheroids of Pancreatic and Colorectal Cancer Cell Lines for High-Throughput Screening of Drug Candidates.." ACS omega, vol. 10, no. 48, 2025, pp. 58194-58204.
PMID 41502656 ↗

Abstract

Over the past decade, three-dimensional (3D) cancer models have emerged as crucial tools in high-throughput screening (HTS), providing a more reliable bridge between in vitro and in vivo drug testing. These models demonstrate higher predictive accuracy compared to traditional two-dimensional (2D) cultures, although the lack of reproducibility and standardization is the main challenge for their translation into quantitative disease modeling and therapeutic response. Therefore, optimization and standardization of 3D spheroid cultivation protocols for HTS for various cancer cell types remain pertinent. This study establishes optimized protocols for cultivating four cancer cell lines (HCT116, SW620, PANC-1, and BxPc-3) as 3D spheroids for drug screening applications. Through systematic parameter optimization, we determined optimal seeding densities (500-1000 cells/well), formation times (3 days), and incubation periods (7-21 days) for each cell line. The application of both IC and score metrics allowed for a comprehensive assessment of drug efficacy, overcoming limitations associated with standard sigmoidal dose-response analysis. Testing a library of more than 100 potential CDK inhibitors identified five CDK7 inhibitors and one CDK8 inhibitor with nanomolar potency, with colorectal cancer spheroids showing approximately 10% greater sensitivity than pancreatic cancer spheroids in the cases of iCDK7_4 and iCDK7_5. This standardized approach improves reproducibility in 3D cancer model screening, potentially accelerating the preclinical evaluation of novel anticancer agents against these challenging malignancies.
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