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Caudal genes in blood development and leukemia

机译:血液发育和白血病中的尾基因

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Members of the caudal gene family (in mice and humans: Cdx1, Cdx2, and Cdx4) have been studied during early development as regulators of axial elongation and anteroposterior patterning. In the adult, Cdx1 and Cdx2, but not Cdx4, have been intensively explored for their function in intestinal tissue homeostasis and the pathogenesis of gastrointestinal cancers. Involvement in embryonic hematopoiesis was first demonstrated in zebrafish, where cdx genes render posterior lateral plate mesoderm competent to respond to genes specifying hematopoietic fate, and compound mutations in cdx genes thus result in a bloodless phenotype. Parallel studies performed in zebrafish embryos and murine embryonic stem cells (ESCs) delineate conserved pathways between fish and mammals, corroborating a BMP/Wnt-Cdx-Hox axis during blood development that can be employed to augment derivation of blood progenitors from pluripotent stem cells in vitro. The molecular regulation of Cdx genes appears complex, as more recent data suggest involvement of non-Hox-related mechanisms and the existence of auto- and cross-regulatory loops governed by morphogens. Here, we will review the role of Cdx genes during hematopoietic development by comparing effects in zebrafish and mice and discuss their participation in malignant blood diseases.
机译:在早期开发期间,尾部基因家族(小鼠和人类:CDX1,CDX2和CDX4)的成员作为轴向伸长率和前后模板的调节器,已经研究过。在成人,CDX1和CDX2,但不是CDX4,在肠组织稳态和胃肠道癌症的发病机制中被密集探索了它们的功能。 Zebrafish首先参与胚胎造血酶,其中CDX基因呈现后侧板Mesoderm伴随着指定造血命运的基因,CDX基因中的复合突变导致无缺陷的表型。在斑马鱼胚胎和鼠胚胎干细胞(ESC)中进行的并行研究在鱼类和哺乳动物之间描绘了保守的途径,在血液发育过程中证实了BMP / WNT-CDX-Hox轴线,其可用于增强来自多能干细胞的血液祖细胞的衍生物体外。随着更近期数据表明非HOX相关机制的参与,CDX基因的分子调节似乎很复杂,并且存在由变态酚治到的自动和跨监管循环的存在。在这里,我们将通过比较斑马鱼和小鼠的效​​果来审查CDX基因在造血过程中的作用,并讨论他们参与恶性血液疾病。

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