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一种生物材料方法,用于影响可注射细胞疗法中干细胞的命运。

A biomaterials approach to influence stem cell fate in injectable cell-based therapies.

机构信息

Centre for Biomolecular Sciences, School of Pharmacy, University of Nottingham, Nottingham, UK.

出版信息

Stem Cell Res Ther. 2018 Feb 21;9(1):39. doi: 10.1186/s13287-018-0789-1.

Abstract

BACKGROUND

Numerous stem cell therapies use injection-based administration to deliver high-density cell preparations. However, cell retention rates as low as 1% have been observed within days of transplantation. This study investigated the effects of varying administration and formulation parameters of injection-based administration on cell dose recovery and differentiation fate choice of human mesenchymal stem cells.

METHODS

The impact of ejection rate via clinically relevant Hamilton micro-syringes and biomaterial-assisted delivery was investigated. Cell viability, the percentage of cell dose delivered as viable cells, proliferation capacity as well as differentiation behaviour in bipotential media were assessed. Characterisation of the biomaterial-based cell carriers was also carried out.

RESULTS

A significant improvement of in-vitro dose recovery in cells co-ejected with natural biomaterials was observed, with ejections within 2% (w/v) gelatin resulting in 87.5 ± 14% of the cell dose being delivered as viable cells, compared to 32.2 ± 19% of the dose ejected in the commonly used saline vehicle at 10 μl/min. Improvement in cell recovery was not associated with the rheological properties of biomaterials utilised, as suggested by previous studies. The extent of osteogenic differentiation was shown to be substantially altered by choice of ejection rate and cell carrier, despite limited contact time with cells during ejection. Collagen type I and bone-derived extracellular matrix cell carriers yielded significant increases in mineralised matrix deposited at day 21 relative to PBS.

CONCLUSIONS

An enhanced understanding of how administration protocols and biomaterials influence cell recovery, differentiation capacity and choice of fate will facilitate the development of improved administration and formulation approaches to achieve higher efficacy in stem cell transplantation.

摘要

背景

许多干细胞疗法采用注射给药的方式来输送高密度的细胞制剂。然而,在移植后的几天内,观察到细胞保留率低至 1%。本研究探讨了不同的注射给药方式和制剂参数对人骨髓间充质干细胞的细胞剂量回收和分化命运选择的影响。

方法

研究了通过临床相关的 Hamilton 微量注射器进行喷射速度以及生物材料辅助输送的影响。评估了细胞活力、作为活细胞输送的细胞剂量百分比、增殖能力以及在双潜能培养基中的分化行为。还对基于生物材料的细胞载体进行了特征描述。

结果

与在通常使用的 10 μl/min 的生理盐水载体中喷射时相比,与天然生物材料共同喷射时,观察到细胞的体外剂量回收有显著改善,2%(w/v)明胶的喷射速度可使 87.5 ± 14%的细胞剂量作为活细胞输送,而在生理盐水载体中仅为 32.2 ± 19%。如先前的研究表明,细胞回收的改善与所使用的生物材料的流变特性无关。尽管在喷射过程中与细胞的接触时间有限,但喷射速度和细胞载体的选择对成骨分化的程度有很大影响。与 PBS 相比,I 型胶原和骨源性细胞外基质细胞载体在第 21 天沉积的矿化基质显著增加。

结论

更深入地了解给药方案和生物材料如何影响细胞回收、分化能力和命运选择,将有助于开发改进的给药和制剂方法,以提高干细胞移植的疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0942/5822649/40d6ed8d5e57/13287_2018_789_Fig1_HTML.jpg

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