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中空纤维生物反应器从人骨髓间充质基质细胞中生产细胞外囊泡,产生的纳米囊泡反映了产生细胞的免疫调节抗原特征。

Hollow-fiber bioreactor production of extracellular vesicles from human bone marrow mesenchymal stromal cells yields nanovesicles that mirrors the immuno-modulatory antigenic signature of the producer cell.

机构信息

Department of Biochemistry, Microbiology, and Immunology, University of Ottawa, Ottawa, Ontario, Canada.

Centre for Biologics Evaluation, Biologic and Radiopharmaceutical Drugs Directorate, Health Products and Food Branch, Health Canada, Ottawa, Ontario, Canada.

出版信息

Stem Cell Res Ther. 2021 Feb 12;12(1):127. doi: 10.1186/s13287-021-02190-3.

Abstract

BACKGROUND

Extracellular vesicles (EVs) produced by human bone marrow-derived mesenchymal stromal cells (hBM-MSCs) are currently investigated for their clinical effectiveness towards immune-mediated diseases. The large amounts of stem cell-derived EVs required for clinical testing suggest that bioreactor production systems may be a more amenable alternative than conventional EV production methods for manufacturing products for therapeutic use in humans.

METHODS

To characterize the potential utility of these systems, EVs from four hBM-MSC donors were produced independently using a hollow-fiber bioreactor system under a cGMP-compliant procedure. EVs were harvested and characterized for size, concentration, immunophenotype, and glycan profile at three separate intervals throughout a 25-day period.

RESULTS

Bioreactor-inoculated hBM-MSCs maintained high viability and retained their trilineage mesoderm differentiation capability while still expressing MSC-associated markers upon retrieval. EVs collected from the four hBM-MSC donors showed consistency in size and concentration in addition to presenting a consistent surface glycan profile. EV surface immunophenotypic analyses revealed a consistent low immunogenicity profile in addition to the presence of immuno-regulatory CD40 antigen. EV cargo analysis for biomarkers of immune regulation showed a high abundance of immuno-regulatory and angiogenic factors VEGF-A and IL-8.

CONCLUSIONS

Significantly, EVs from hBM-MSCs with immuno-regulatory constituents were generated in a large-scale system over a long production period and could be frequently harvested with the same quality and quantity, which will circumvent the challenge for clinical application.

摘要

背景

目前正在研究源自人骨髓间充质基质细胞(hBM-MSCs)的细胞外囊泡(EVs)在免疫介导性疾病方面的临床疗效。大量用于临床测试的干细胞衍生 EVs 表明,生物反应器生产系统可能比传统 EV 生产方法更适合制造用于人类治疗用途的产品。

方法

为了表征这些系统的潜在用途,我们使用符合 cGMP 要求的程序,通过中空纤维生物反应器系统独立生产了来自四个 hBM-MSC 供体的 EVs。在 25 天的时间内,在三个不同的时间点分别收获和表征 EV 的大小、浓度、免疫表型和聚糖谱。

结果

生物反应器接种的 hBM-MSCs 保持高活力,并在回收时仍保留其三系中胚层分化能力,同时仍表达 MSC 相关标志物。从四个 hBM-MSC 供体收集的 EVs 除了呈现一致的表面聚糖谱外,在大小和浓度上也表现出一致性。EV 表面免疫表型分析显示出一致的低免疫原性特征,以及存在免疫调节性 CD40 抗原。免疫调节生物标志物的 EV 货物分析显示出高丰度的免疫调节和血管生成因子 VEGF-A 和 IL-8。

结论

重要的是,具有免疫调节成分的 hBM-MSCs 的 EVs 是在大规模系统中在较长的生产周期中产生的,可以频繁地以相同的质量和数量收获,这将避免临床应用的挑战。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b80e/7881490/2b866ed897bb/13287_2021_2190_Fig1_HTML.jpg

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