首页> 美国卫生研究院文献>The Plant Cell >The Recessive Epigenetic swellmap Mutation Affects the Expression of Two Step II Splicing Factors Required for the Transcription of the Cell Proliferation Gene STRUWWELPETER and for the Timing of Cell Cycle Arrest in the Arabidopsis Leaf
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The Recessive Epigenetic swellmap Mutation Affects the Expression of Two Step II Splicing Factors Required for the Transcription of the Cell Proliferation Gene STRUWWELPETER and for the Timing of Cell Cycle Arrest in the Arabidopsis Leaf

机译:隐性表观遗传膨胀图突变影响拟南芥叶中细胞增殖基因STRUWWELPETER的转录和细胞周期停滞的时间所需的两个步骤II剪接因子的表达。

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摘要

Generally, cell division can be uncoupled from multicellular development, but more recent evidence suggests that cell cycle progression and arrest is coupled to organogenesis and growth. We describe a recessive mutant, swellmap (smp), with reduced organ size and cell number. This defect is partially compensated for by an increase in final cell size. The mutation causes a precocious arrest of cell proliferation in the organ primordium and possibly reduces the rate of cell division there. The mutation proved to be an epigenetic mutation (renamed smpepi) that defined a single locus, SMP1, but affected the expression of both SMP1 and a second very similar gene, SMP2. Both genes encode CCHC zinc finger proteins with similarities to step II splicing factors involved in 3′ splice site selection. Genetic knockouts demonstrate that the genes are functionally redundant and essential. SMP1 expression is associated with regions of cell proliferation. Overexpression of SMP1 produced an increase in organ cell number and a partial decrease in cell expansion. The smpepi mutation does not affect expression of eukaryotic cell cycle regulator genes CYCD3;1 and CDC2A but affects expression of the cell proliferation gene STRUWWELPETER (SWP) whose protein has similarities to Med150/Rgr1-like subunits of the Mediator complex required for transcriptional activation. Introduction of SWP cDNA into smpepi plants fully restored them to wild-type, but the expression of both SMP1 and SMP2 were also restored in these lines, suggesting a physical interaction among the three proteins and/or genes. We propose that step II splicing factors and a transcriptional Mediator-like complex are involved in the timing of cell cycle arrest during leaf development.
机译:通常,细胞分裂可以与多细胞发育脱钩,但是最近的证据表明,细胞周期的进展和停滞与器官发生和生长有关。我们描述了一种隐性突变体,swellmap(smp),具有减小的器官大小和细胞数量。通过增加最终单元尺寸可以部分弥补此缺陷。该突变导致器官原基中的细胞增殖过早地停止,并可能降低那里的细胞分裂速度。该突变被证明是表观遗传突变(重命名为smp epi ),该突变定义了一个基因座SMP1,但同时影响了SMP1和第二个非常相似的基因SMP2的表达。这两个基因都编码CCHC锌指蛋白,与3'剪接位点选择中涉及的第二步剪接因子相似。基因敲除表明基因在功能上是多余的并且是必需的。 SMP1表达与细胞增殖区域有关。 SMP1的过表达导致器官细胞数量增加和细胞扩增部分减少。 smp epi 突变不会影响真核细胞周期调节基因CYCD3; 1和CDC2A的表达,但会影响细胞增殖基因STRUWWELPETER(SWP)的表达,该蛋白质的结构类似于Med150 / Rgr1的亚基。转录激活所需的介体复合物。将swp cDNA导入smp epi 植物完全使其恢复为野生型,但是SMP1和 SMP2 的表达在这些品系中也得以恢复,表明它们之间存在物理相互作用。三种蛋白质和/或基因。我们建议第二步剪接因子和转录介体样复合体参与叶片发育过程中细胞周期停滞的时间。

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