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磁共振成像跟踪铁氧体标记的人神经干细胞:临床应用相关研究。

Magnetic resonance imaging tracking of ferumoxytol-labeled human neural stem cells: studies leading to clinical use.

机构信息

Departments of Neurosciences.

出版信息

Stem Cells Transl Med. 2013 Oct;2(10):766-75. doi: 10.5966/sctm.2013-0049. Epub 2013 Sep 6.

Abstract

Numerous stem cell-based therapies are currently under clinical investigation, including the use of neural stem cells (NSCs) as delivery vehicles to target therapeutic agents to invasive brain tumors. The ability to monitor the time course, migration, and distribution of stem cells following transplantation into patients would provide critical information for optimizing treatment regimens. No effective cell-tracking methodology has yet garnered clinical acceptance. A highly promising noninvasive method for monitoring NSCs and potentially other cell types in vivo involves preloading them with ultrasmall superparamagnetic iron oxide nanoparticles (USPIOs) to enable cell tracking using magnetic resonance imaging (MRI). We report here the preclinical studies that led to U.S. Food and Drug Administration approval for first-in-human investigational use of ferumoxytol to label NSCs prior to transplantation into brain tumor patients, followed by surveillance serial MRI. A combination of heparin, protamine sulfate, and ferumoxytol (HPF) was used to label the NSCs. HPF labeling did not affect cell viability, growth kinetics, or tumor tropism in vitro, and it enabled MRI visualization of NSC distribution within orthotopic glioma xenografts. MRI revealed dynamic in vivo NSC distribution at multiple time points following intracerebral or intravenous injection into glioma-bearing mice that correlated with histological analysis. Preclinical safety/toxicity studies of intracerebrally administered HPF-labeled NSCs in mice were also performed, and they showed no significant clinical or behavioral changes, no neuronal or systemic toxicities, and no abnormal accumulation of iron in the liver or spleen. These studies support the clinical use of ferumoxytol labeling of cells for post-transplant MRI visualization and tracking.

摘要

目前有许多基于干细胞的疗法正在进行临床研究,包括使用神经干细胞(NSCs)作为载体将治疗剂靶向侵袭性脑肿瘤。在将干细胞移植到患者体内后,能够监测其时间进程、迁移和分布,这将为优化治疗方案提供关键信息。目前还没有有效的细胞追踪方法获得临床认可。一种非常有前途的非侵入性方法,可以监测体内的 NSCs 和潜在的其他细胞类型,包括将它们预先加载到超小超顺磁性氧化铁纳米颗粒(USPIO)中,以便使用磁共振成像(MRI)进行细胞追踪。我们在此报告了导致美国食品和药物管理局批准 ferumoxytol 用于首例人体临床试验的临床前研究,该研究将 ferumoxytol 用于 NSCs 移植到脑肿瘤患者之前进行标记,随后进行连续 MRI 监测。肝素、硫酸鱼精蛋白和 ferumoxytol(HPF)的组合用于标记 NSCs。HPF 标记不会影响细胞活力、生长动力学或体外肿瘤趋向性,并且能够可视化 NSC 在原位胶质瘤异种移植物中的分布。MRI 显示了在脑内或静脉内注射到携带胶质瘤的小鼠后多个时间点的体内 NSC 分布情况,与组织学分析相关。还对脑内给予 HPF 标记的 NSCs 的小鼠进行了临床前安全性/毒性研究,结果显示没有明显的临床或行为变化、没有神经元或全身毒性、肝脏或脾脏内没有异常铁积累。这些研究支持使用 ferumoxytol 标记细胞进行移植后 MRI 可视化和追踪的临床应用。

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