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用新型磁化藻酸盐对重组细胞进行封装以用于磁共振成像。

Encapsulation of recombinant cells with a novel magnetized alginate for magnetic resonance imaging.

作者信息

Shen Feng, Li Anna Aihua, Gong Yong-Kuan, Somers Sat, Potter Murray A, Winnik Françoise M, Chang Patricia L

机构信息

Department of Pediatrics, Faculty of Health Sciences, McMaster University, Hamilton, ON, Canada.

出版信息

Hum Gene Ther. 2005 Aug;16(8):971-84. doi: 10.1089/hum.2005.16.971.

Abstract

Implanting recombinant cells encapsulated in alginate microcapsules to express therapeutic proteins has been proven effective in treating several mouse models of human diseases (neurological disorders, dwarfism, hemophilia, lysosomal storage disease, and cancer). In anticipation of clinical application, we have reported the synthesis and characterization of a magnetized ferrofluid alginate that potentially allows tracking of these microcapsules in vivo by magnetic resonance imaging (MRI). We now report the properties of these ferrofluid microcapsules important for applications in gene therapy. When a mouse myoblast cell line was encapsulated in these microcapsules, it showed similar viability as in regular unmodified alginate capsules, both in vitro and in vivo, in mice. The permeability of these magnetized microcapsules, a critical parameter for immunoisolation devices, was comparable to that of classic alginate in the transit of various recombinant molecules of various molecular masses (human factor IX, 65 kDa; murine IgG, 150 kDa; and beta-glucuronidase, 300 kDa). When followed by MRI in vitro and in vivo, the ferrofluid microcapsules remained intact and visible for extended periods, allowing quantitative monitoring of microcapsules. At autopsy, the ferrofluid microcapsules were mostly free within the intraperitoneal cavities, with no overt inflammatory response. Serological analyses demonstrated a high level of biocompatibility comparable to that of unmodified alginate. In conclusion, ferrofluid-enhanced alginate microcapsules are comparable to classic alginate microcapsules in permeability and biocompatibility. Their visibility and stability to MRI monitoring permitted qualitative and quantitative tracking of the implanted microcapsules without invasive surgery. These properties are important advantages for the application of immunoisolation devices in human gene therapy.

摘要

将包裹在藻酸盐微胶囊中的重组细胞植入体内以表达治疗性蛋白质,已被证明在治疗多种人类疾病的小鼠模型(神经疾病、侏儒症、血友病、溶酶体贮积病和癌症)方面是有效的。预期到临床应用,我们已报道了一种磁化铁流体藻酸盐的合成与表征,其有可能通过磁共振成像(MRI)在体内追踪这些微胶囊。我们现在报告这些铁流体微胶囊对于基因治疗应用而言重要的特性。当将小鼠成肌细胞系包裹在这些微胶囊中时,其在体外和体内(在小鼠体内)均显示出与常规未修饰藻酸盐胶囊相似的活力。这些磁化微胶囊的通透性是免疫隔离装置的一个关键参数,在各种不同分子量的重组分子(人凝血因子IX,65 kDa;鼠IgG,150 kDa;以及β-葡萄糖醛酸酶,300 kDa)的转运过程中,其与经典藻酸盐的通透性相当。当在体外和体内通过MRI进行追踪时,铁流体微胶囊在很长一段时间内保持完整且可见,从而允许对微胶囊进行定量监测。尸检时,铁流体微胶囊大多在腹腔内处于游离状态,没有明显的炎症反应。血清学分析表明其具有与未修饰藻酸盐相当的高生物相容性。总之,铁流体增强的藻酸盐微胶囊在通透性和生物相容性方面与经典藻酸盐微胶囊相当。它们对MRI监测的可见性和稳定性允许在无需侵入性手术的情况下对植入的微胶囊进行定性和定量追踪。这些特性对于免疫隔离装置在人类基因治疗中的应用而言是重要的优势。

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