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Lnx2b, an E3 ubiquitin ligase, in dorsal forerunner cells and Kupffer's vesicle is required for specification of zebrafish left-right laterality

机译:Lnx2b,一种E3泛素连接酶,位于背前体细胞和库普弗囊泡中,是指定斑马鱼左右偏向性的必要条件

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摘要

The establishment of left-right (LR) axis in zebrafish embryos relies on numerous genes expressed in the cluster of dorsal forerunner cells (DFCs) that form Kupffer's vesicle (KV), the transient cilia-rich organ with functional similarity to mouse node in the case of LR axis determination. Even though several genes in the DFCs and KV have been identified to be implicated in LR body patterning so far, the underlying regulatory mechanisms in particular dependent upon ubiquitin (Ub)- proteasome system have not yet been identified. In this study, we report that Lnx2b, a RING domain containing E3 Ub ligase, specifically expressed in migratory DFCs and developing KV, plays a critical role in the establishment of LR laterality. Depletion of Lnx2b using antisense morpholino oligonucleotides (MOs) inhibited the left-side biased expression of southpaw and resulted in the randomization of the heart jogging and looping in zebrafish embryos. A DFCs-specific Lnx2b loss of function approach showed that the randomization of LR patterning caused by the depletion of Lnx2b was not simply due to the early dorsoventral body patterning defects or the MO toxicity, but the loss of its function in the DFCs and KV. Collectively, our data showed that Lnx2b is the first analyzed E3 Ub ligase, which is involved in LR laterality during zebrafish embryogenesis.
机译:斑马鱼胚胎中左右(LR)轴的建立依赖于背侧先行细胞(DFC)簇中表达的众多基因,这些基因形成了库普弗囊泡(KV),这是一种短暂的纤毛丰富的器官,与小鼠结节的功能相似。 LR轴确定的情况。到目前为止,尽管已经确定了DFC和KV中的几个基因与LR体模式有关,但尚未发现潜在的调控机制,特别是依赖于泛素(Ub)-蛋白酶体系统的调控机制。在这项研究中,我们报告Lnx2b,一个包含E3 Ub连接酶的RING域,在迁移DFCs和发育中的KV中特异性表达,在LR侧向的建立中起关键作用。使用反义吗啉代寡核苷酸(MOs)耗尽Lnx2b抑制了左爪向南爪的表达,并导致斑马鱼胚胎中心脏慢跑和loop回的随机性。 DFCs特有的Lnx2b功能丧失方法显示,由Lnx2b耗竭引起的LR图案随机化不仅是由于早期腹背体图案缺陷或MO毒性,还在于DFC和KV中其功能丧失。总体而言,我们的数据表明Lnx2b是第一个分析的E3 Ub连接酶,在斑马鱼胚胎发生过程中与LR偏向有关。

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