比较聚苯乙烯和水凝胶微载体在粘附细胞光学成像中的应用。

IF 3 3区 医学 Q2 BIOCHEMICAL RESEARCH METHODS
Journal of Biomedical Optics Pub Date : 2024-06-01 Epub Date: 2024-06-13 DOI:10.1117/1.JBO.29.S2.S22708
Oscar R Benavides, Berkley P White, Holly C Gibbs, Roland Kaunas, Carl A Gregory, Kristen C Maitland, Alex J Walsh
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引用次数: 0

摘要

意义重大:几十年来,观察和监测细胞密度和形态的能力对于评估细胞培养物的健康状况以及生产高质量、高产量的细胞培养物至关重要。用于大规模细胞扩增过程的基于微载体的培养物,由于其厚度和材料成分,与传统的可视化方法(如宽视场显微镜)不兼容。目的:在此,我们评估了商用聚苯乙烯微载体与定制明胶甲基丙烯酰(gelMA)微载体的光学成像兼容性,以便对整个微载体表面进行非破坏性和非侵入性观察、直接细胞计数以及间充质干细胞/基质细胞的亚细胞观察:方法:对聚苯乙烯和凝胶MA 微载体进行米氏散射和波前误差模拟,以评估基于弹性散射的附着细胞成像的潜力。通过改装蔡司 Z.1 光片显微镜,利用平面侧照的无标记弹性散射对比进行光片层析成像,从而实现光学切片,并对微载体上培养的细胞进行无创、无损的三维高分辨率整体观察:聚苯乙烯微载体无法利用荧光或弹性散射对比技术观察微载体远半部分的细胞,而凝胶MA微载体则可以利用光片荧光显微镜和层析成像技术高保真地观察细胞形态并量化细胞密度:结论:光学质量的凝胶MA 微载体与无标记光片断层成像技术相结合,将有助于加强对生物反应器-微载体细胞培养过程的控制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparison of polystyrene and hydrogel microcarriers for optical imaging of adherent cells.

Significance: The ability to observe and monitor cell density and morphology has been imperative for assessing the health of a cell culture and for producing high quality, high yield cell cultures for decades. Microcarrier-based cultures, used for large-scale cellular expansion processes, are not compatible with traditional visualization-based methods, such as widefield microscopy, due to their thickness and material composition.

Aim: Here, we assess the optical imaging compatibilities of commercial polystyrene microcarriers versus custom-fabricated gelatin methacryloyl (gelMA) microcarriers for non-destructive and non-invasive visualization of the entire microcarrier surface, direct cell enumeration, and sub-cellular visualization of mesenchymal stem/stromal cells.

Approach: Mie scattering and wavefront error simulations of the polystyrene and gelMA microcarriers were performed to assess the potential for elastic scattering-based imaging of adherent cells. A Zeiss Z.1 light-sheet microscope was adapted to perform light-sheet tomography using label-free elastic scattering contrast from planar side illumination to achieve optical sectioning and permit non-invasive and non-destructive, in toto, three-dimensional, high-resolution visualization of cells cultured on microcarriers.

Results: The polystyrene microcarrier prevents visualization of cells on the distal half of the microcarrier using either fluorescence or elastic scattering contrast, whereas the gelMA microcarrier allows for high fidelity visualization of cell morphology and quantification of cell density using light-sheet fluorescence microscopy and tomography.

Conclusions: The combination of optical-quality gelMA microcarriers and label-free light-sheet tomography will facilitate enhanced control of bioreactor-microcarrier cell culture processes.

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来源期刊
CiteScore
6.40
自引率
5.70%
发文量
263
审稿时长
2 months
期刊介绍: The Journal of Biomedical Optics publishes peer-reviewed papers on the use of modern optical technology for improved health care and biomedical research.
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