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Nxnl2 splicing results in dual functions in neuronal cell survival and maintenance of cell integrity

机译:Nxnl2剪接导致神经元细胞存活和维持细胞完整性的双重功能

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摘要

The rod-derived cone viability factors, RdCVF and RdCVF2, have potential therapeutical interests for the treatment of inherited photoreceptor degenerations. In the mouse lacking Nxnl2, the gene encoding RdCVF2, the progressive decline of the visual performance of the cones in parallel with their degeneration, arises due to the loss of trophic support from RdCVF2. In contrary, the progressive loss of rod visual function of the Nxnl2-/- mouse results from a decrease in outer segment length, mediated by a cell autonomous mechanism involving the putative thioredoxin protein RdCVF2L, the second spliced product of the Nxnl2 gene. This novel signaling mechanism extends to olfaction as shown by the progressive impairment of olfaction in aged Nxnl2-/- mice and the protection of olfactory neurons by RdCVF2. This study shows that Nxnl2 is a bi-functional gene involved in the maintenance of both the function and the viability of sensory neurons.
机译:杆衍生的圆锥生存力因子RdCVF和RdCVF2对于遗传性光感受器变性的治疗具有潜在的治疗意义。在缺少Nxn12的小鼠中,由于RdCVF2失去了营养支持,因此出现了编码RdCVF2的基因,即视锥的视觉性能与退化同时下降。相反,Nxnl2-/-小鼠视杆视功能的逐渐丧失是由外段长度的减少导致的,这是由涉及推定的硫氧还蛋白蛋白RdCVF2L(Nxnl2基因的第二个剪接产物)的细胞自主机制介导的。这种新的信号传导机制已扩展到嗅觉,如老年Nxnl2-/-小鼠嗅觉的逐步损害和RdCVF2对嗅觉神经元的保护所表明的。这项研究表明,Nxnl2是一个双功能基因,与感觉神经元的功能和生存能力有关。

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