调节转基因小鼠中外周蛋白/视网膜变性慢蛋白的表达:临界水平及过表达的影响。
Modulating expression of peripherin/rds in transgenic mice: critical levels and the effect of overexpression.
作者信息
Nour May, Ding Xi-Qin, Stricker Heidi, Fliesler Steven J, Naash Muna I
机构信息
Department of Cell Biology, University of Oklahoma Health Sciences Center, Oklahoma City, 73104, USA.
出版信息
Invest Ophthalmol Vis Sci. 2004 Aug;45(8):2514-21. doi: 10.1167/iovs.04-0065.
PURPOSE
Mutations in the photoreceptor-specific protein peripherin/rds are associated with multiple retinal diseases. To date, attempts to achieve complete structural and functional rescue in animal models of peripherin/rds-induced retinal degeneration have not been successful. Gene therapy-directed approaches have been hindered by the haploinsufficiency phenotype, which dictates well-regulated expression of peripherin/rds protein levels.
METHODS
Using a transgenic mouse line expressing wild-type peripherin/rds (NMP), the authors evaluated the critical in vivo level of peripherin/rds needed to maintain photoreceptor structure and ERG function and assessed the consequences of peripherin/rds overexpression in both rods and cones by Western blot and immunoprecipitation analyses, immunohistochemistry, electron microscopy, and electroretinography. The NMP transgene included a C-terminal modification (P341Q) to facilitate detection of the transgenic protein in the presence of wild-type peripherin/rds, using the monoclonal antibody 3B6.
RESULTS
Peripherin/rds protein levels in NMP homozygotes were approximately 60% of wild-type levels. Western blot and immunoprecipitation analyses confirmed normal biochemical properties of the NMP protein when compared with wild-type peripherin/rds. Immunohistochemistry demonstrated appropriate localization of transgenic peripherin/rds protein to the disc rim region of photoreceptor outer segments. Total peripherin/rds levels in the retina were modulated by crossing NMP transgenic mice into different rds genetic backgrounds. A positive correlation was observed between peripherin/rds expression levels and the structural and functional integrity of photoreceptor outer segments. Overexpression of peripherin/rds caused no detectable adverse effects on rod or cone structure and function.
CONCLUSIONS
These findings may have significant implications regarding therapeutic intervention in peripherin/rds-associated retinal diseases.
目的
光感受器特异性蛋白外周蛋白/视网膜变性慢(peripherin/rds)的突变与多种视网膜疾病相关。迄今为止,在peripherin/rds诱导的视网膜变性动物模型中实现完全结构和功能挽救的尝试尚未成功。基因治疗导向的方法受到单倍剂量不足表型的阻碍,该表型要求peripherin/rds蛋白水平受到良好调控的表达。
方法
作者使用表达野生型peripherin/rds的转基因小鼠品系(NMP),评估维持光感受器结构和视网膜电图(ERG)功能所需的peripherin/rds的关键体内水平,并通过蛋白质免疫印迹和免疫沉淀分析、免疫组织化学、电子显微镜和视网膜电图评估peripherin/rds在视杆细胞和视锥细胞中过表达的后果。NMP转基因包含一个C端修饰(P341Q),以利于在存在野生型peripherin/rds的情况下使用单克隆抗体3B6检测转基因蛋白。
结果
NMP纯合子中的peripherin/rds蛋白水平约为野生型水平的60%。与野生型peripherin/rds相比,蛋白质免疫印迹和免疫沉淀分析证实NMP蛋白具有正常的生化特性。免疫组织化学显示转基因peripherin/rds蛋白正确定位于光感受器外段的盘缘区域。通过将NMP转基因小鼠与不同的rds遗传背景杂交,可调节视网膜中总的peripherin/rds水平。观察到peripherin/rds表达水平与光感受器外段的结构和功能完整性之间存在正相关。peripherin/rds的过表达对视杆细胞或视锥细胞的结构和功能未产生可检测到的不利影响。
结论
这些发现可能对外周蛋白/视网膜变性慢相关视网膜疾病的治疗干预具有重要意义。
Zotero 插件