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首页> 外文期刊>Molecular biology of the cell >R9AP targeting to rod outer segments is independent of rhodopsin and is guided by the SNARE homology domain
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R9AP targeting to rod outer segments is independent of rhodopsin and is guided by the SNARE homology domain

机译:R9AP靶向杆外段独立于视紫红质,并由SNARE同源域指导

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摘要

In vertebrate photoreceptor cells, rapid recovery from light excitation is dependent on the RGS9?Gβ5 GTPase-activating complex located in the light-sensitive outer segment organelle. RGS9?Gβ5 is tethered to the outer segment membranes by its membrane anchor, R9AP. Recent studies indicated that RGS9?Gβ5 possesses targeting information that excludes it from the outer segment and that this information is overridden by association with R9AP, which allows outer segment targeting of the entire complex. It was also proposed that R9AP itself does not contain specific targeting information and instead is delivered to the outer segment in the same post-Golgi vesicles as rhodopsin, because they are the most abundant transport vesicles in photoreceptor cells. In this study, we revisited this concept by analyzing R9AP targeting in rods of wild-type and rhodopsin-knockout mice. We found that the R9AP targeting mechanism does not require the presence of rhodopsin and further demonstrated that R9AP is actively targeted in rods by its SNARE homology domain.
机译:在脊椎动物的感光细胞中,光激发的快速恢复依赖于位于感光外部区段细胞器中的RGS9βGβ5GTPase激活复合物。 RGS9?Gβ5通过其膜锚R9AP拴在外段膜上。最近的研究表明,RGS9βGβ5具有靶向信息,该信息将其排除在外链段之外,并且该信息被与R9AP的结合所覆盖,从而可以靶向整个复合物。还提出,R9AP本身不包含特定的靶向信息,而是与视紫红质一起在高尔基体后小泡中递送至外部部分,因为它们是感光细胞中最丰富的运输小泡。在这项研究中,我们通过分析野生型和视紫红质基因敲除小鼠的棒中的R9AP靶向,重新审视了这一概念。我们发现R9AP靶向机制不需要视紫红质的存在,并进一步证明R9AP的SNARE同源域在棒中被有效靶向。

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