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利用基于猴免疫缺陷病毒的慢病毒载体的基因修饰脂肪组织源性干细胞/基质细胞治疗乙型血友病。

Genetically modified adipose tissue-derived stem/stromal cells, using simian immunodeficiency virus-based lentiviral vectors, in the treatment of hemophilia B.

机构信息

Institute of Advanced Biomedical Engineering and Science, Tokyo Women's Medical University, Tokyo, Japan.

出版信息

Hum Gene Ther. 2013 Mar;24(3):283-94. doi: 10.1089/hum.2012.162.

Abstract

Hemophilia is an X-linked bleeding disorder, and patients with hemophilia are deficient in a biologically active coagulation factor. This study was designed to combine the efficiency of lentiviral vector transduction techniques with murine adipose tissue-derived stem/stromal cells (mADSCs) as a new method to produce secreted human coagulation factor IX (hFIX) and to treat hemophilia B. mADSCs were transduced with simian immunodeficiency virus (SIV)-hFIX lentiviral vector at multiplicities of infection (MOIs) from 1 to 60, and the most effective dose was at an MOI of 10, as determined by hFIX production. hFIX protein secretion persisted over the 28-day experimental period. Cell sheets composed of lentiviral vector-transduced mADSCs were engineered to further enhance the usefulness of these cells for future therapeutic applications in transplantation modalities. These experiments demonstrated that genetically transduced ADSCs may become a valuable cell source for establishing cell-based gene therapies for plasma protein deficiencies, such as hemophilia.

摘要

血友病是一种 X 连锁出血性疾病,患者缺乏生物活性凝血因子。本研究旨在将慢病毒载体转导技术的效率与鼠脂肪组织来源的干细胞/基质细胞(mADSCs)相结合,作为一种产生分泌型人凝血因子 IX(hFIX)并治疗乙型血友病的新方法。mADSCs 被猴免疫缺陷病毒(SIV)-hFIX 慢病毒载体以 1 到 60 的感染复数(MOI)转导,最有效的剂量是在 MOI 为 10 时确定的,这是由 hFIX 的产生决定的。hFIX 蛋白分泌在 28 天的实验期间持续存在。由慢病毒载体转导的 mADSCs 组成的细胞片被构建,以进一步增强这些细胞在未来移植方式的治疗应用中的有用性。这些实验表明,基因转导的 ADSCs 可能成为建立基于细胞的血浆蛋白缺乏症(如血友病)基因治疗的有价值的细胞来源。

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