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通过逆转录病毒介导的基因转移在兔肝细胞中表达人凝血因子IX:B型血友病基因治疗的潜力

Expression of human factor IX in rabbit hepatocytes by retrovirus-mediated gene transfer: potential for gene therapy of hemophilia B.

作者信息

Armentano D, Thompson A R, Darlington G, Woo S L

机构信息

Howard Hughes Medical Institute, Department of Cell Biology, Baylor College of Medicine, Houston, TX 77030.

出版信息

Proc Natl Acad Sci U S A. 1990 Aug;87(16):6141-5. doi: 10.1073/pnas.87.16.6141.

Abstract

Hemophilia B (Christmas disease) is a chromosome X-linked blood clotting disorder which results when factor IX is deficient or functionally defective. The enzyme is synthesized in the liver, and the existence of animal models for this genetic disease will permit the development of somatic gene therapy protocols aimed at transfer of the functional gene into the liver. We report the construction of an N2-based recombinant retroviral vector, NCMVFIX, for efficient transfer and expression of human factor IX cDNA in primary rabbit hepatocytes. In this construct the human cytomegalovirus immediate early promoter directs the expression of factor IX. Hepatocytes were isolated from 3-week-old New Zealand White rabbits, infected with the recombinant virus, and analyzed for secretion of active factor IX. The infected rabbit hepatocytes produced human factor IX that is indistinguishable from enzyme derived from normal human plasma. The recombinant protein is sufficiently gamma-carboxylated and is functionally active in clotting assays. These results establish the feasibility of using infected hepatocytes for the expression of this protein and are a step toward the goal of correcting hemophilia B by hepatic gene transfer.

摘要

血友病B(克里斯马斯病)是一种X染色体连锁的凝血障碍疾病,由凝血因子IX缺乏或功能缺陷引起。该酶在肝脏中合成,这种遗传病动物模型的存在将有助于开发旨在将功能基因导入肝脏的体细胞基因治疗方案。我们报告了一种基于N2的重组逆转录病毒载体NCMVFIX的构建,用于在原代兔肝细胞中高效转移和表达人凝血因子IX cDNA。在该构建体中,人巨细胞病毒立即早期启动子指导凝血因子IX的表达。从3周龄的新西兰白兔中分离肝细胞,用重组病毒感染,并分析活性凝血因子IX的分泌情况。感染的兔肝细胞产生的人凝血因子IX与源自正常人血浆的酶无法区分。重组蛋白具有充分的γ-羧化作用,并且在凝血试验中具有功能活性。这些结果证实了使用感染的肝细胞表达这种蛋白质的可行性,并且朝着通过肝脏基因转移纠正血友病B的目标迈进了一步。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea37/54488/391df00ded03/pnas01041-0143-a.jpg

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