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基因修饰血小板模型系统。

Model systems of genetically modified platelets.

机构信息

Laboratory for Thrombosis Research, KU Leuven campus Kortrijk, Kortrijk, Belgium.

出版信息

Blood. 2012 Feb 16;119(7):1634-42. doi: 10.1182/blood-2011-10-381715. Epub 2011 Dec 16.

Abstract

Although platelets are the smallest cells in the blood, they are implied in various processes ranging from immunology and oncology to thrombosis and hemostasis. Many large-scale screening programs, genome-wide association, and "omics" studies have generated lists of genes and loci that are probably involved in the formation or physiology of platelets under normal and pathologic conditions. This creates an increasing demand for new and improved model systems that allow functional assessment of the corresponding gene products in vivo. Such animal models not only render invaluable insight in the platelet biology, but in addition, provide improved test systems for the validation of newly developed anti-thrombotics. This review summarizes the most important models to generate transgenic platelets and to study their influence on platelet physiology in vivo. Here we focus on the zebrafish morpholino oligonucleotide technology, the (platelet-specific) knockout mouse, and the transplantation of genetically modified human or murine platelet progenitor cells in myelo-conditioned mice. The various strengths and pitfalls of these animal models are illustrated by recent examples from the platelet field. Finally, we highlight the latest developments in genetic engineering techniques and their possible application in platelet research.

摘要

尽管血小板是血液中最小的细胞,但它们参与了从免疫学和肿瘤学到血栓形成和止血等各种过程。许多大规模的筛选计划、全基因组关联和“组学”研究已经生成了一系列基因和基因座的列表,这些基因和基因座可能涉及正常和病理条件下血小板的形成或生理功能。这就产生了对新的和改进的模型系统的需求,这些系统允许在体内对相应的基因产物进行功能评估。这些动物模型不仅为血小板生物学提供了宝贵的见解,而且还为新开发的抗血栓药物的验证提供了改进的测试系统。本文总结了生成转基因血小板并研究其对体内血小板生理学影响的最重要模型。本文重点介绍斑马鱼形态发生素寡核苷酸技术、(血小板特异性)敲除小鼠,以及在骨髓条件化小鼠中移植基因修饰的人类或鼠血小板祖细胞。通过血小板领域的最新实例来说明这些动物模型的优缺点。最后,我们强调了基因工程技术的最新进展及其在血小板研究中的可能应用。

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