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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >The Ras-ERK MAPK regulatory network controls dedifferentiation in Caenorhabditis elegans germline
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The Ras-ERK MAPK regulatory network controls dedifferentiation in Caenorhabditis elegans germline

机译:Ras-ERK MAPK调控网络控制秀丽隐杆线虫种系的去分化

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How a committed cell can be reverted to an undifferentiated state is a central question in stem cell biology. This process, called dedifferentiation, is likely to be important for replacing stem cells as they age or get damaged. Tremendous progress has been made in understanding this fundamental process, but its mechanisms are poorly understood. Here we demonstrate that the aberrant activation of Ras-ERK MAPK signaling promotes cellular dedifferentiation in the Caenorhabditis elegans germline. To activate signaling, we removed two negative regulators, the PUF-8 RNA-binding protein and LIP-1 dual specificity phosphatase. The removal of both of these two regulators caused secondary spermatocytes to dedifferentiate and begin mitotic divisions. Interestingly, reduction of Ras-ERK MAPK signaling, either by mutation or chemical inhibition, blocked the initiation of dedifferentiation. By RNAi screening, we identified RSKN-1/P90 RSK as a downstream effector of MPK-1/ERK that is critical for dedifferentiation: rskn-1 RNAi suppressed spermatocyte dedifferentiation and instead induced meiotic divisions. These regulators are broadly conserved, suggesting that similar molecular circuitry may control cellular dedifferentiation in other organisms, including humans.
机译:如何将定型细胞还原为未分化状态是干细胞生物学中的核心问题。这个过程称为去分化,可能对替换老化或受损的干细胞很重要。在理解这一基本过程方面已经取得了巨大的进步,但是人们对其机制的了解却很少。在这里,我们证明Ras-ERK MAPK信号转导的异常激活促进秀丽隐杆线虫种系中的细胞去分化。为了激活信号,我们删除了两个负调节剂,PUF-8 RNA结合蛋白和LIP-1双特异性磷酸酶。去除这两种调节剂均导致继发精母细胞去分化并开始有丝分裂。有趣的是,通过突变或化学抑制降低了Ras-ERK MAPK信号传导,阻止了去分化的启动。通过RNAi筛选,我们确定RSKN-1 / P90 RSK是MPK-1 / ERK的下游效应,这对去分化至关重要:rskn-1 RNAi抑制了精母细胞的去分化,而是诱导了减数分裂。这些调节剂是广泛保守的,表明相似的分子电路可以控制包括人在内的其他生物体中的细胞去分化。

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