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The leak stops here: platelets as delivery vehicles for coagulation factors

机译:泄漏在这里停止:血小板作为凝血因子的输送工具

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摘要

Gene therapy is an attractive approach for the treatment of hemophilia, as continuous expression of donated clotting factor VIII (FVIII) DNA would ensure clotting factor replacement at constant circulating levels rather than at the peaks and troughs that characterize the current protein infusion therapeutic approach. In this issue of the JCI, Shi et al. describe an interesting variant of a gene transfer approach for hemophilia (see the related article beginning on page 1974). They show that targeted expression of FVIII in megakaryocytes, with storage in the α-granules of platelets, has the advantage of delivering clotting factors directly to the site of an injury, where platelets accumulate in large numbers and undergo activation accompanied by release of granule contents. Earlier clinical experience with gene transfer into hematopoietic cells highlighted the potential safety risks of this approach, but an F8 transgene may represent a lower risk than transgenes for growth factors or their receptors.
机译:基因疗法是治疗血友病的一种有吸引力的方法,因为连续表达捐赠的凝血因子VIII(FVIII)DNA将确保在恒定的循环水平而不是在表征当前蛋白质输注治疗方法的高峰和低谷时替代凝血因子。在JCI的这一期中,Shi等人。描述了一种针对血友病的基因转移方法的有趣变体(请参阅从1974年开始的相关文章)。他们表明,巨核细胞中FVIII的靶向表达以及储存在血小板的α颗粒中,具有将凝血因子直接传递至损伤部位的优势,在损伤部位血小板大量积聚并受到激活,并伴随颗粒成分的释放。将基因转移到造血细胞中的早期临床经验强调了这种方法的潜在安全风险,但是F8转基因的生长因子或其受体的风险可能低于转基因。

著录项

  • 作者

    High, Katherine A.;

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  • 年度 2006
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  • 原文格式 PDF
  • 正文语种 en
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