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Murine Models of Acute Myeloid Leukaemia

机译:急性髓细胞白血病的小鼠模型

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Acute myeloid leukaemia (AML) is a rare but severe form of human cancer that results from a limited number of functionally cooperating genetic abnormalities leading to uncontrolled proliferation and impaired differentiation of hematopoietic stem and progenitor cells. Before the identification of genetic driver lesions, chemically, irradiation or viral infection-induced mouse leukaemia models provided platforms to test novel chemotherapeutics. Later, transgenic mouse models were established to test the in vivo transforming potential of newly cloned fusion genes and genetic aberrations detected in patients’ genomes. Hereby researchers constitutively or conditionally expressed the respective gene in the germline of the mouse or reconstituted the hematopoietic system of lethally irradiated mice with bone marrow virally expressing the mutation of interest. More recently, immune deficient mice have been explored to study patient-derived human AML cells in vivo. Unfortunately, although complementary to each other, none of the currently available strategies faithfully model the initiation and progression of the human disease. Nevertheless, fast advances in the fields of next generation sequencing, molecular technology and bioengineering are continuously contributing to the generation of better mouse models. Here we review the most important AML mouse models of each category, briefly describe their advantages and limitations and show how they have contributed to our understanding of the biology and to the development of novel therapies.
机译:急性髓细胞性白血病(AML)是人类癌症的一种罕见但严重的形式,其源于有限的功能上相互配合的遗传异常,导致不受控制的增殖以及造血干细胞和祖细胞的分化受损。在鉴定遗传驱动因子损伤之前,化学,辐射或病毒感染引起的小鼠白血病模型提供了测试新型化学疗法的平台。后来,建立了转基因小鼠模型,以测试新克隆的融合基因在体内的转化潜力以及在患者基因组中检测到的遗传异常。因此,研究人员在小鼠的种系中组成性或有条件地表达了相应的基因,或用骨髓病毒重组了致死性照射小鼠的造血系统,该骨髓病毒表达了感兴趣的突变。最近,已经探索了免疫缺陷小鼠在体内研究患者来源的人AML细胞。不幸的是,尽管彼此互补,但是目前没有可用的策略能够忠实地模拟人类疾病的发生和发展。然而,下一代测序,分子技术和生物工程领域的快速发展正在不断为更好的小鼠模型的产生做出贡献。在这里,我们回顾每个类别中最重要的AML小鼠模型,简要描述它们的优点和局限性,并展示它们如何有助于我们对生物学的理解和新型疗法的发展。

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