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琼脂糖斑点迁移分析检测细胞外囊泡的趋化潜力:在再生医学和癌症转移中的应用。

Agarose spot migration assay to measure the chemoattractant potential of extracellular vesicles: applications in regenerative medicine and cancer metastasis.

机构信息

REMAR-IGTP Group, Germans Trias i Pujol Research Institute (IGTP) & Nephrology Department, University Hospital Germans Trias i Pujol (HUGTiP), Can Ruti Campus, Badalona, Barcelona, Catalonia, 08916, Spain.

Department of Cell Biology, Physiology and Immunology, Universitat Autònoma de Barcelona (UAB), Bellaterra, Spain.

出版信息

BMC Biol. 2023 Oct 26;21(1):236. doi: 10.1186/s12915-023-01729-5.

Abstract

BACKGROUND

The recruitment of effector cells is one of the novel functions described for extracellular vesicles (EVs) that needs further study. For instance, cell recruitment by mesenchymal stromal cell derived-EVs (MSC-EVs) is one of the features by which MSC-EVs may induce regeneration and ameliorate tissue injury. On the other hand, increasing evidence suggests that cancer EVs play an important role in the preparation of the pre-metastatic niche (PMN) by recruiting their primary tumour cells. Understanding and measuring the potential of MSC-EVs or cancer-EVs to induce cell migration and recruitment is essential for cell-free therapeutic approaches and/or for a better knowledge of cancer metastasis, respectively. In this context, classical in vitro migration assays do not completely mimic the potential situation by which EVs exert their chemotactic capacity.

RESULTS

We adapted an agarose spot migration assay as an in vitro system to evaluate the cell recruitment capacity of locally delivered or localized EVs. Cell migration was tracked for 12 h or 48 h, respectively. Thereafter, endpoint migration images and time-lapse videos were analysed to quantify several parameters aiming to determine the migration of cells to either MSC-EV or pro-metastatic EV. The number of cells contained inside the agarose spots, the migration distance, the area occupied by cells, the directionality of the cell movement, and the Euclidean distance were measured. This multi-parametric evaluation revealed the potential of different MSC-EV preparations to recruit endothelial cells and to detect an enhanced recruitment capacity of highly metastatic PC3-derived EVs (PC3-EVs) compared to low-metastatic LNCaP-EVs in a tumour cell-specific manner.

CONCLUSIONS

Overall, this agarose spot migration assay may offer a diversity of measurements and migration settings not provided by classical migration assays and reveal its potential use in the EV field in two different contexts with recruitment in common: regeneration and cancer metastasis.

摘要

背景

细胞募集是细胞外囊泡(EVs)的新功能之一,需要进一步研究。例如,间充质基质细胞衍生的 EV(MSC-EVs)通过募集其原发性肿瘤细胞来诱导再生和改善组织损伤,这是 MSC-EVs 的特征之一。另一方面,越来越多的证据表明,癌症 EVs 通过募集其原发性肿瘤细胞在预转移龛(PMN)的准备中发挥重要作用。了解和衡量 MSC-EVs 或癌症-EVs 诱导细胞迁移和募集的潜力,对于无细胞治疗方法和/或更好地了解癌症转移分别是至关重要的。在这种情况下,经典的体外迁移测定并不能完全模拟 EV 发挥趋化能力的潜在情况。

结果

我们将琼脂糖点迁移测定法改编为体外系统,以评估局部递送或局部化 EV 对细胞募集能力的影响。分别跟踪细胞迁移 12 小时或 48 小时。此后,分析终点迁移图像和延时视频,以量化几个参数,旨在确定细胞向 MSC-EV 或促转移 EV 的迁移。测量琼脂糖斑点内包含的细胞数量、迁移距离、细胞占据的面积、细胞运动的方向性和欧几里得距离。这种多参数评估揭示了不同 MSC-EV 制剂招募内皮细胞的潜力,并以肿瘤细胞特异性的方式检测到高度转移性 PC3 衍生 EV(PC3-EVs)的募集能力增强,而低转移性 LNCaP-EVs 的募集能力增强。

结论

总的来说,这种琼脂糖点迁移测定法可能提供多种测量和迁移设置,这些设置是经典迁移测定法无法提供的,并在两个具有共同募集的不同背景下,揭示了其在 EV 领域的潜在用途:再生和癌症转移。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a75d/10605981/da03ffb91cb4/12915_2023_1729_Fig1_HTML.jpg

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