4.6 Article

Dual-Phase, Surface Tension-Based Fabrication Method for Generation of Tumor Millibeads

期刊

LANGMUIR
卷 30, 期 13, 页码 3817-3825

出版社

AMER CHEMICAL SOC
DOI: 10.1021/la500402m

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资金

  1. NSF [NSF-CBET-1150854]
  2. Auburn University Research Initiative in Cancer (AURIC) Seed Grant Program
  3. AU-CMB Peaks of Excellence Summer Graduate Research Fellowship [NSF-EPS-1158862]
  4. AU-CMB Peaks of Excellence Undergraduate Summer Research Fellowship
  5. Alabama EPSCoR Graduate Research Scholarship Program
  6. Directorate For Engineering
  7. Div Of Chem, Bioeng, Env, & Transp Sys [1150854] Funding Source: National Science Foundation

向作者/读者索取更多资源

Numerous methods have been developed for the fabrication of poly(ethylene glycol)-based hydrogel microstructures for drug-delivery and tissue-engineering applications. However, present methods focus on the fabrication of submicrometer scale hydrogel structures which have limited applications in creating larger tissue constructs, especially in recreating cancer tissue microenvironments. We cultured in a three-dimensional (3D) environment, which closely replicates the native cancer microenvironment and aimed to establish a platform where cancer cells can be facilitates efficient testing of anticancer drugs. This study demonstrated a novel surface tension-based fabrication technique for the generation of millimeter-scale hydrogel beads using a liquid liquid dual phase system. The hydrogel millibeads obtained by this method were larger than previously reported, highly uniform in shape and size with better ease of size control and a high degree of consistency and reproducibility between batches. In addition, human breast cancer cells were encapsulated within these hydrogel constructs to generate tumor millibeads, which were subsequently maintained in long-term 3D culture. Microscopic visualization using fluorescence imaging and microstructure analysis showed the morphology and uniform distribution of the cells within the 3D matrix and arrangement of cells with the surrounding scaffold material. Cell viability analysis revealed the creation of a core region of dead cells surrounded by healthy, viable cell layers at the periphery following long-term culture. These observations closely matched with those of native and in vivo tumors. Based on these results, this study established.a rapidly reproducible surface tension-based fabrication technique for making spherical hydrogel millibeads and demonstrated the potential of this method in creating engineered 3D tumor tissues. It is envisioned that the developed hydrogel millibead system will facilitate the formation of physiologically relevant in vitro tumor models which will closely simulate the native tumor microenvironmental conditions and could enable future highthroughput testing of different anticancer drugs in preclinical trials.

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