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The Opportunities and Challenges regarding Induced Platelets from Human Pluripotent Stem Cells

机译:对人多能干细胞诱导血小板的机遇和挑战

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As a standard clinical treatment, platelet transfusion has been employed to prevent hemorrhage in patients with thrombocytopenia or platelet dysfunctions. Platelets also show therapeutic potential for aiding liver regeneration and bone healing and regeneration and for treating dermatological conditions. However, the supply of platelets rarely meets the rising clinical demand. Other issues, including short shelf life, strict storage temperature, and allogeneic immunity caused by frequent platelet transfusions, have become serious challenges that require the development of high-yielding alternative sources of platelets. Human pluripotent stem cells (hPSCs) are an unlimited substitution source for regenerative medicine, and patient-derived iPSCs can provide novel research models to explore the pathogenesis of some diseases. Many studies have focused on establishing and modifying protocols for generating functional induced platelets (iPlatelets) from hPSCs. To reach high efficiency production and eliminate the exogenous antigens, media supplements and matrix have been optimized. In addition, the introduction of some critical transgenes, such as c-MYC , BMI1 , and BCL-XL , can also significantly increase hPSC-derived platelet production; however, this may pose some safety concerns. Furthermore, many novel culture systems have been developed to scale up the production of iPlatelets, including 2D flow systems, 3D rotary systems, and vertical reciprocal motion liquid culture bioreactors. The development of new gene-editing techniques, such as CRISPR/Cas9, can be used to solve allogeneic immunity of platelet transfusions by knocking out the expression of B2M . Additionally, the functions of iPlatelets were also evaluated from multiple aspects, including but not limited to morphology, structure, cytoskeletal organization, granule content, DNA content, and gene expression. Although the production and functions of iPlatelets are close to meeting clinical application requirements in both quantity and quality, there is still a long way to go for their large-scale production and clinical application. Here, we summarize the diverse methods of platelet production and update the progresses of iPlatelets. Furthermore, we highlight recent advances in our understanding of key transcription factors or molecules that determine the platelet differentiation direction.
机译:作为一个标准的临床治疗,输注血小板已被用来防止患者血小板减少或血小板功能障碍出血。血小板还显示帮助肝脏再生和骨愈合和再生,并用于治疗皮肤病的治疗潜力。然而,血小板的供应很少满足不断上升的需求临床。其他问题,包括保质期短,严格的储存温度,并造成频繁血小板输注异体免疫能力,已经成为需要高产血小板替代能源发展的严峻挑战。人多能干细胞(hPSCs)是用于再生医学无限替代源,和患者来源的iPSC可以提供新颖的研究模型,探讨了一些疾病的发病机理。许多研究已经集中在建立和修改的​​协议用于从hPSCs官能诱导血小板(iPlatelets)。为了达到高效率的生产,消除了外源性抗原,媒体的补充和矩阵进行了优化。此外,引入了一些关键的转基因,如c-MYC,BMI1,和BCL-XL的,也可以增加显著HPSC衍生的血小板生成;但是,这可能会造成一些安全问题。此外,许多新颖培养系统已经被开发以扩大生产iPlatelets的,包括二维流动系统,3D旋转系统和垂直往复运动的液体培养生物反应器。的新的基因编辑技术,如CRISPR / Cas9的发展,可以使用通过敲除B2M的表达来解决血小板输注的同种异体免疫力。另外,iPlatelets的功能也从多个方面,包括评价,但不限于形态,结构,细胞骨架组织,颗粒含量,DNA含量和基因表达。虽然生产和iPlatelets的功能接近的数量和质量满足临床应用的要求,还有很长的路要走他们的大规模生产和临床应用。在这里,我们总结血小板生成的各种方法和更新iPlatelets的进展。此外,我们强调在我们的关键转录因子或分子确定血小板分化方向的了解最新进展。

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