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首页> 外文期刊>Cell death & disease. >mRNA for N-Bak, a neuron-specific BH3-only splice isoform of Bak, escapes nonsense-mediated decay and is translationally repressed in the neurons
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mRNA for N-Bak, a neuron-specific BH3-only splice isoform of Bak, escapes nonsense-mediated decay and is translationally repressed in the neurons

机译:N-Bak的mRNA,Bak的一种神经元特异性BH3剪接异构体,逃避了无意义的介导的衰变,并在神经元中被翻译抑制

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mRNA for neuronal Bak (N-Bak), a splice variant of pro-apoptotic Bcl-2 family member Bak is expressed in the neurons. Surprisingly the endogeneous N-Bak protein cannot be demonstrated in the neurons, although the antibodies recognize N-Bak protein from in vitro translation or transiently transfected cells. As N-Bak mRNA contains premature termination codon (PTC) at 89 nucleotides upstream from the last exon–exon junction, it could be degraded by nonsense-mediated decay (NMD) during the pioneer round of translation thus explaining the absence of the protein. We show here that the endogeneous neuronal N-Bak mRNA is not the NMD substrate, as it is not accumulating by cycloheximide treatment, it has a long lifetime, and even prevention of PTC by interfering with the alternative splicing did not lead to translation of the Bak mRNA. N-Bak protein is also not revealed by proteasome inhibitors. Our data suggest strong translational arrest of N-Bak mRNA in the neurons. We show that this arrest is partially mediated by 5′-untranslated region of Bak mRNA and it is not released during mitochondrial apoptosis.. ? 2012 Macmillan Publishers Limited
机译:神经元Bak(N-Bak)的mRNA在神经元中表达,N-Bak是凋亡前Bcl-2家族成员Bak的剪接变体。令人惊讶的是,尽管抗体从体外翻译或瞬时转染的细胞中识别出N-Bak蛋白,但无法在神经元中证明其内源性N-Bak蛋白。由于N-Bak mRNA在最后一个外显子-外显子连接上游的89个核苷酸处包含过早终止密码子(PTC),因此在先驱翻译过程中它可能会被无义介导的衰变(NMD)降解,从而解释了该蛋白的缺失。我们在此处显示,内源性神经元N-Bak mRNA不是NMD底物,因为它不会通过环己酰亚胺处理积聚,使用寿命长,甚至通过干扰替代剪接来预防PTC也不会导致Bak mRNA。蛋白酶体抑制剂也未揭示N-Bak蛋白。我们的数据表明神经元中N-Bak mRNA的强烈翻译停滞。我们显示该逮捕是由Bak mRNA的5'-非翻译区部分介导的,并且在线粒体凋亡过程中没有释放。 2012 Macmillan Publishers Limited

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