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Interdependencies govern multidomain architecture in ribosomal small subunit assembly.

机译:相互依赖性控制核糖体小亚基组装中的多域结构。

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摘要

The 30S subunit is composed of four structural domains, the body, platform, head, and penultimate/ultimate stems. The functional integrity of the 30S subunit is dependent upon appropriate assembly and precise orientation of all four domains. We examined 16S rRNA conformational changes during in vitro assembly using directed hydroxyl radical probing mediated by Fe(II)-derivatized ribosomal protein (r-protein) S8. R-protein S8 binds the central domain of 16S rRNA directly and independently and its iron derivatized substituents have been shown to mediate cleavage in three domains of 16S rRNA, thus making it an ideal probe to monitor multidomain orientation during assembly. Cleavages in minimal ribonucleoprotein (RNP) particles formed with Fe(II)-S8 and 16S rRNA alone were compared with that in the context of the fully assembled subunit. The minimal binding site of S8 at helix 21 exists in a structure similar to that observed in the mature subunit, in the absence of other r-proteins. However, the binding site of S8 at the junction of helices 25-26a, which is transcribed after helix 21, is cleaved with differing intensities in the presence and absence of other r-proteins. Also, assembly of the body helps establish an architecture approximating, but perhaps not identical, to the 30S subunit at helix 12 and the 5' terminus. Moreover, the assembly or orientation of the neck is dependent upon assembly of both the head and the body. Thus, a complex interrelationship is observed between assembly events of independent domains and the incorporation of primary binding proteins during 30S subunit formation.
机译:30S亚基由四个结构域组成,即身体,平台,头部和倒数第二个/倒数第二个茎。 30S亚基的功能完整性取决于所有四个结构域的适当组装和精确定位。我们检查了体外组装过程中使用由Fe(II)衍生的核糖体蛋白(r-蛋白)S8介导的定向羟基自由基探测的16S rRNA构象变化。 R蛋白S8直接和独立地结合16S rRNA的中央结构域,其铁衍生的取代基已显示出介导16S rRNA的三个结构域的切割,因此使其成为监测组装过程中多结构域方向的理想探针。将仅由Fe(II)-S8和16S rRNA形成的最小核糖核蛋白(RNP)颗粒的裂解与完全组装的亚基的裂解进行了比较。在没有其他r蛋白的情况下,S8在螺旋21处的最小结合位点的结构类似于在成熟亚基中观察到的结构。但是,在存在和不存在其他r蛋白的情况下,在螺旋21之后转录的螺旋25-26a交界处的S8结合位点被裂解。而且,身体的组装有助于建立与螺旋12和5'末端的30S亚基近似但可能不相同的结构。而且,颈部的组装或定向取决于头部和身体的组装。因此,在30S亚基形成过程中,独立域的组装事件与主要结合蛋白的掺入之间观察到复杂的相互关系。

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