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人骨髓祖细胞和长期培养起始细胞的高效逆转录病毒转导:通过gp91 - phox表达部分重建X连锁慢性肉芽肿病患者的细胞

Efficient retroviral transduction of human bone marrow progenitor and long-term culture-initiating cells: partial reconstitution of cells from patients with X-linked chronic granulomatous disease by gp91-phox expression.

作者信息

Porter C D, Parkar M H, Collins M K, Levinsky R J, Kinnon C

机构信息

Division of Cell and Molecular Biology, Institute of Child Health, London, UK.

出版信息

Blood. 1996 May 1;87(9):3722-30.

PMID:8611697
Abstract

The primary immunodeficiencies are attractive candidates for the development of gene therapy approaches based on the transduction of hematopoietic cells. We have constructed a high-titer recombinant retrovirus for expression of gp91-phox, deficiencies of which cause the X-linked form of chronic granulomatous disease (X-CGD). We have used this vector to transduce human bone marrow, using either unfractionated mononuclear cells or purified CD34+ cells as targets and evaluated several infection protocols. Efficient gene transfer to progenitors and long-term culture-initiating cells (LTC-IC) was obtained for each target population. Importantly for potential clinical application, this could be achieved without the use of exogenous cytokines or polybrene. Progenitors representing each of the lineages detectable in vitro were transduced at equal efficiencies. The vector was shown partially to restore gp91-phox deficiency and nicotinamide adenine dinucleotide phosphate (NADPH) oxidase activity in transduced cells derived from X-CGD patients. These data demonstrate that it is possible to transduce primitive human hematopoietic cells efficiently and reconstitute NADPH oxidase.

摘要

原发性免疫缺陷病是基于造血细胞转导的基因治疗方法的理想候选对象。我们构建了一种高滴度重组逆转录病毒,用于表达gp91 - phox,其缺陷会导致X连锁型慢性肉芽肿病(X - CGD)。我们使用该载体转导人骨髓,以未分离的单核细胞或纯化的CD34 +细胞作为靶细胞,并评估了几种感染方案。对于每个靶细胞群体,均实现了向祖细胞和长期培养起始细胞(LTC - IC)的高效基因转移。对于潜在的临床应用而言重要的是,无需使用外源性细胞因子或聚凝胺即可实现这一点。体外可检测到的每个谱系的祖细胞均以相同效率被转导。该载体在源自X - CGD患者的转导细胞中部分恢复了gp91 - phox缺陷和烟酰胺腺嘌呤二核苷酸磷酸(NADPH)氧化酶活性。这些数据表明,高效转导原始人类造血细胞并重建NADPH氧化酶是可行的。

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