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Critical role of connexin43 in zebrafish late primitive and definitive hematopoiesis

机译:连接蛋白43在斑马鱼晚期原始和确定性造血中的关键作用

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摘要

In vitro studies have suggested that connexin43 (cx43) expression is of particular importance during establishment and regeneration of the mammalian hematopoietic system. However, little is known about its in vivo functions during hematopoiesis due to the embryonic lethality of mammalian knockout models. In this study, we observed that zebrafish cx43 is not only expressed in the eyes, cerebellum, heart, and vasculature, but also expressed, albeit at low levels, in intermediate cell mass (ICM, the primitive hematopoietic site). Knockdown of cx43 leads to vacuolization in the wedge of the ICM and an apparent reduction in the number of circulating blood cells, but does not affect their cellular morphology. Whole-mount in situ hybridization analysis revealed that the hemangioblastic marker flk-1 and the primitive hematopoietic markers lmo2 and scl are basically maintained at normal levels in cx43 morphant embryos at 12-13 h postfertilization (hpf) compared with the con-MO injected embryos. However, subsequent expression of the definitive hematopoietic stem cell (HSC) marker c-myb was severely downregulated in the ventral wall of the dorsal aorta of cx43-depleted embryos at 36 hpf. Furthermore, we confirmed this phenotype by injection of cx43-MO into Tg(gata1:EGFP) embryos. Together, our results show that cx43 contributes to late primitive and definitive hematopoiesis in zebrafish embryos.
机译:体外研究表明,在哺乳动物造血系统的建立和再生过程中,连接蛋白43(cx43)的表达特别重要。然而,由于哺乳动物基因敲除模型的胚胎致死性,其在造血过程中的体内功能知之甚少。在这项研究中,我们观察到斑马鱼cx43不仅在眼睛,小脑,心脏和脉管系统中表达,而且还在中间细胞团(ICM,原始造血部位)中表达,尽管水平较低。击倒cx43会导致ICM楔形中的空泡化和循环血细胞数量的明显减少,但不会影响其细胞形态。整个原位杂交分析表明,与con-MO注入的胚胎相比,在受精后12-13 h(hpf),成血管细胞标记flk-1和原始造血标记lmo2和scl基本保持在cx43 morphant胚胎的正常水平。 。但是,最终的造血干细胞(HSC)标记c-myb的后续表达在36 hpf时在cx43耗竭的胚胎的背主动脉腹壁严重下调。此外,我们通过将cx43-MO注射到Tg(gata1:EGFP)胚胎中证实了这种表型。在一起,我们的结果表明,cx43有助于斑马鱼胚胎后期的原始和确定的造血功能。

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