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Development of platelet replacement therapy using human induced pluripotent stem cells

机译:使用人诱导多能干细胞的血小板替代疗法的发展

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In the body, platelets mainly work as a hemostatic agent, and the lack of platelets can cause serious bleeding. Induced pluripotent stem (iPS) cells potentially allow for a stable supply of platelets that are independent of donors and eliminate the risk of infection. However, a major challenge in iPS cell-based systems is producing the number of platelets required for a single transfusion (more than 200 billion in Japan). Thus, development in large-scale culturing technology is required. In previous studies, we generated a self-renewable, immortalized megakaryocyte cell line by transfecting iPS cell-derived hematopoietic progenitor cells with c-MYC, BMI1, and BCL-XL genes. Optimization of the culture conditions, including the discovery of a novel fluid-physical factor, turbulence, in the production of platelets in vivo, and the development of bioreactors that apply turbulence have enabled us to generate platelets of clinical quality and quantity. We have further generated platelets deleted of HLA class I expression by using genetic modification technology for patients suffering from alloimmune transfusion refractoriness, since these patients are underserved by current blood donation systems. In this review, we highlight current research and our recent work on iPS cell-derived platelet induction.
机译:在体内,血小板主要起到止血剂的作用,缺乏血小板会导致严重出血。诱导多能干细胞(iPS)有可能提供独立于供体的稳定血小板供应,并消除感染风险。然而,基于iPS细胞的系统面临的一个主要挑战是产生单次输血所需的血小板数量(日本超过2000亿)。因此,需要发展大规模养殖技术。在以前的研究中,我们通过转染含有c-MYC、BMI1和BCL-XL基因的iPS细胞源性造血祖细胞,产生了一种自我更新的永生化巨核细胞系。培养条件的优化,包括在体内血小板生产中发现一种新的流体物理因子湍流,以及应用湍流的生物反应器的开发,使我们能够产生临床质量和数量的血小板。由于目前的献血系统对同种异体免疫输血难治性患者的服务不足,我们利用基因改造技术进一步生成了HLA I类表达缺失的血小板。在这篇综述中,我们重点介绍了目前的研究和我们最近在诱导iPS细胞衍生血小板方面的工作。

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