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Concise Review: Mesenchymal Stem Cell‐Based Drug Delivery: The Good the Bad the Ugly and the Promise

机译:简要评论:间充质干细胞为基础的药物输送:好的坏的丑陋的和诺言

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摘要

The development of mesenchymal stem cells (MSCs) as cell‐based drug delivery vectors for numerous clinical indications, including cancer, has significant promise. However, a considerable challenge for effective translation of these approaches is the limited tumor tropism and broad biodistribution observed using conventional MSCs, which raises concerns for toxicity to nontarget peripheral tissues (i.e., the bad). Consequently, there are a variety of synthetic engineering platforms in active development to improve tumor‐selective targeting via increased homing efficiency and/or specificity of drug activation, some of which are already being evaluated clinically (i.e., the good). Unfortunately, the lack of robust quantification and widespread adoption of standardized methodologies with high sensitivity and resolution has made accurate comparisons across studies difficult, which has significantly impeded progress (i.e., the ugly). Herein, we provide a concise review of active and passive MSC homing mechanisms and biodistribution postinfusion; in addition to in vivo cell tracking methodologies and strategies to enhance tumor targeting with a focus on MSC‐based drug delivery strategies for cancer therapy. Stem Cells Translational Medicine 2018;1–13
机译:间充质干细胞(MSCs)作为基于细胞的药物传递载体的开发,可用于包括癌症在内的许多临床适应症,具有重大前景。然而,对于这些方法的有效翻译而言,相当大的挑战是使用常规MSC观察到的有限的肿瘤嗜性和广泛的生物分布,这引起了对对非靶标周围组织的毒性(即不良)的关注。因此,有各种各样的合成工程平台正在积极开发中,以通过提高归巢效率和/或药物激活的特异性来改善肿瘤选择性靶向,其中一些已经在临床上进行评估(即良好)。不幸的是,由于缺乏可靠的量化方法以及具有高灵敏度和分辨率的标准化方法的广泛采用,使得跨研究的准确比较变得困难,这严重阻碍了研究进展(即丑陋)。在这里,我们提供了主动和被动MSC归巢机制和输注后生物分布的简要回顾。除了体内细胞跟踪方法和策略以增强肿瘤靶向性为重点,重点是用于癌症治疗的基于MSC的药物递送策略。干细胞转化医学2018; 1-13

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