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Small protein B interacts with the large and the small subunits of a stalled ribosome during trans-translation

机译:在翻译过程中,小蛋白B与停滞的核糖体的大亚基和小亚基相互作用

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摘要

During trans-translation, stalled bacterial ribosomes are rescued by small protein B (SmpB) and by transfer-messenger RNA (tmRNA). Stalled ribosomes switch translation from the defective messages to a short internal reading frame on tmRNA that tags the nascent peptide chain for degradation and recycles the ribosomes. We present evidences that SmpB binds the large and small ribosomal subunits in vivo and in vitro. The binding between SmpB and the ribosomal subunits is very tight, with a dissociation constant of 1.7 x 10(-10) M, similar to its K-D for the 70S ribosome or for tmRNA. tmRNA displaces SmpB from its 50S binding but not from the 30S. In vivo, SmpB is detected on the 50S when trans-translation is impaired by lacking tmRNA or a functional SmpB. SmpB contacts the large subunit transiently and early during the trans-translational process. The affinity of SmpB for the two ribosomal subunits is modulated by tmRNA in the course of trans-translation. It is the first example of two copies of the same protein interacting with two different functional sites of the ribosomes.
机译:在转译过程中,停滞的细菌核糖体通过小蛋白B(SmpB)和传递信使RNA(tmRNA)进行拯救。失速的核糖体将翻译从有缺陷的信息转换为tmRNA上较短的内部阅读框,该框架将新生肽链标记为降解并回收了核糖体。我们提供的证据表明,SmpB在体内和体外结合了大大小小的核糖体亚基。 SmpB与核糖体亚基之间的结合非常紧密,解离常数为1.7 x 10(-10)M,与70S核糖体或tmRNA的解离常数相似。 tmRNA取代了SmpB的50S结合而不是30S。在体内,当由于缺少tmRNA或功能性SmpB而使转译受损时,会在50S上检测到SmpB。在转译过程中,SmpB会短暂且短暂地接触大亚基。在转译过程中,tmRNA调节SmpB对两个核糖体亚基的亲和力。这是相同蛋白质的两个拷贝与核糖体的两个不同功能位点相互作用的第一个例子。

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