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基于生物反应器制造可调节小胶质细胞的细胞外囊泡,对间充质基质细胞对炎症信号的形态学反应进行高通量筛选。

High throughput screening of mesenchymal stromal cell morphological response to inflammatory signals for bioreactor-based manufacturing of extracellular vesicles that modulate microglia.

作者信息

Larey Andrew M, Spoerer Thomas M, Daga Kanupriya R, Morfin Maria G, Hynds Hannah M, Carpenter Jana, Hines Kelly M, Marklein Ross A

机构信息

School of Chemical, Materials, and Biomedical Engineering, University of Georgia, Athens, GA, USA.

Regenerative Bioscience Center, University of Georgia, Athens, GA, USA.

出版信息

bioRxiv. 2023 Nov 19:2023.11.19.567730. doi: 10.1101/2023.11.19.567730.

Abstract

Due to their immunomodulatory function, mesenchymal stromal cells (MSCs) are a promising therapeutic with the potential to treat neuroinflammation associated with neurodegenerative diseases. This function can be mediated by secreted extracellular vesicles (MSC-EVs). Despite established safety, MSC clinical translation has been unsuccessful due to inconsistent clinical outcomes resulting from functional heterogeneity. Current approaches to mitigate functional heterogeneity include 'priming' MSCs with inflammatory signals to enhance function. However, comprehensive evaluation of priming and its effects on MSC-EV function has not been performed. Clinical translation of MSC-EV therapies requires significant manufacturing scale-up, yet few studies have investigated the effects of priming in bioreactors. As MSC morphology has been shown to predict their immunomodulatory function, we screened MSC morphological response to an array of priming signals and evaluated MSC-EV identity and potency in response to priming in flasks and bioreactors. We identified unique priming conditions corresponding to distinct morphologies. These conditions demonstrated a range of MSC-EV preparation quality and lipidome, allowing us to discover a novel MSC-EV manufacturing condition, as well as gain insight into potential mechanisms of MSC-EV microglia modulation. Our novel screening approach and application of priming to MSC-EV bioreactor manufacturing informs refinement of larger-scale manufacturing and enhancement of MSC-EV function.

摘要

由于其免疫调节功能,间充质基质细胞(MSCs)是一种很有前景的治疗手段,具有治疗与神经退行性疾病相关的神经炎症的潜力。这种功能可由分泌的细胞外囊泡(MSC-EVs)介导。尽管已证实其安全性,但由于功能异质性导致临床结果不一致,MSC的临床转化尚未成功。目前减轻功能异质性的方法包括用炎症信号“预处理”MSCs以增强功能。然而,尚未对预处理及其对MSC-EV功能的影响进行全面评估。MSC-EV疗法的临床转化需要大幅扩大生产规模,但很少有研究调查在生物反应器中预处理的效果。由于已证明MSC形态可预测其免疫调节功能,我们筛选了MSC对一系列预处理信号的形态学反应,并评估了在培养瓶和生物反应器中预处理后MSC-EV的特性和效能。我们确定了与不同形态相对应的独特预处理条件。这些条件展示了一系列MSC-EV的制备质量和脂质组,使我们能够发现一种新的MSC-EV生产条件,并深入了解MSC-EV调节小胶质细胞的潜在机制。我们新颖的筛选方法以及将预处理应用于MSC-EV生物反应器生产,为大规模生产的优化和MSC-EV功能的增强提供了依据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eaa4/10680807/7e0b775ea0f8/nihpp-2023.11.19.567730v1-f0002.jpg

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