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首页> 外文期刊>American Journal of Nephrology >Lack of association between small dense low-density lipoprotein levels and coronary artery disease in chronic hemodialysis patients.
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Lack of association between small dense low-density lipoprotein levels and coronary artery disease in chronic hemodialysis patients.

机译:在慢性血液透析患者中​​,小而密集的低密度脂蛋白水平与冠状动脉疾病之间缺乏关联。

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摘要

In both vertebrates and insects, neurons typically arise from neural stem cells or terminally dividing intermediate progenitors. Here, we describe another mode of neurogenesis where neural stem cells generate secondary precursors that undergo multiple rounds of self-renewing transit-amplifying divisions. We identify the Posterior Asense-Negative (PAN) neuroblasts, which do not express the transcription factors Asense or Prospero. PAN neuroblasts rely on the segregating determinants Numb and Brat to generate smaller, secondary neuroblasts that in turn give rise to ganglion mother cells (GMCs) and neurons throughout larval development. In brat or numb mutants, misspecified secondary neuroblasts are unable to produce differentiated progeny and initiate tumor-like overgrowth. In prospero mutants, however, tumors arise from GMCs while secondary neuroblasts are correctly specified. Our data describe a transit-amplifying lineage in the Drosophila nervous system and suggest that different vulnerabilities in intermediate cell types can affect the outcome of tumor suppressor loss in stem cell lineages.
机译:在脊椎动物和昆虫中,神经元通常来自神经干细胞或终末分裂的中间祖细胞。在这里,我们描述了神经发生的另一种模式,其中神经干细胞产生次级前体,这些前体经历了多轮自我更新的转运扩增分裂。我们鉴定出后部Asense-Negative(PAN)成神经细胞,它们不表达转录因子Asense或Prospero。 PAN成神经细胞依赖于决定簇Numb和Brat产生较小的次级成神经细胞,继而在整个幼虫发育过程中产生神经节母细胞(GMC)和神经元。在小子或麻木的突变体中,错误指定的继发性成神经细胞不能产生分化的后代并不能引发肿瘤样的过度生长。然而,在Prospero突变体中,肿瘤是由GMC引起的,而正确地指定了继发性成神经细胞。我们的数据描述了果蝇神经系统中的转运放大谱系,并表明中型细胞类型中的不同漏洞可能会影响干细胞谱系中肿瘤抑制因子丧失的结果。

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