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当延伸因子Tu与核糖体结合时,会诱导出该因子上的第二个tRNA结合位点。

A second tRNA binding site on elongation factor Tu is induced while the factor is bound to the ribosome.

作者信息

Van Noort J M, Kraal B, Bosch L

出版信息

Proc Natl Acad Sci U S A. 1985 May;82(10):3212-6. doi: 10.1073/pnas.82.10.3212.

Abstract

Previously, we reported that the antibiotic kirromycin induces two tRNA-binding sites on the elongation factor Tu. The classical binding site (site I) binds aminoacyl-tRNA and, with much less affinity, deacylated tRNA. The kirromycin-induced site II binds aminoacyl-tRNA, peptidyl-tRNA, and deacylated tRNA with comparable affinities. Accordingly, 3'-oxidized tRNA can be cross-linked in the presence of the antibiotic to two specific sites of EF-Tu: Lys-237 and Lys-208. Here, we report that 3'-oxidized tRNAPhe, bound to a ribosome-poly(U) complex, can also be cross-linked to either one of these two sites. When located in the ribosomal peptidyl site, it cross-links exclusively to Lys-208; when located in the ribosomal aminoacyl site, it cross-links exclusively to Lys-237, irrespective of the presence of kirromycin. Since no cross-linking could be detected in the absence of ribosomes and kirromycin, we conclude that the tRNA-binding site II is induced upon interaction of aminoacyl-tRNA-EF-Tu-GTP with the ribosome-mRNA complex. The results indicate that, on the ribosome, EF-Tu interacts with peptidyl-site-bound peptidyl-tRNA through tRNA-binding site II and with aminoacyl-site-bound aminoacyl-tRNA through tRNA-binding site I.

摘要

此前,我们报道过抗生素奇霉素可在延伸因子Tu上诱导出两个tRNA结合位点。经典结合位点(位点I)结合氨酰tRNA,对脱酰基tRNA的亲和力则低得多。奇霉素诱导产生的位点II以相当的亲和力结合氨酰tRNA、肽基tRNA和脱酰基tRNA。因此,在抗生素存在的情况下,3'-氧化的tRNA可与延伸因子Tu的两个特定位点交联:赖氨酸-237和赖氨酸-208。在此,我们报道结合到核糖体-聚(U)复合物上的3'-氧化苯丙氨酰tRNA也能与这两个位点之一交联。当位于核糖体肽基位点时,它仅与赖氨酸-208交联;当位于核糖体氨酰位点时,它仅与赖氨酸-237交联,与奇霉素是否存在无关。由于在没有核糖体和奇霉素的情况下检测不到交联,我们得出结论,氨酰tRNA-延伸因子Tu-GTP与核糖体-mRNA复合物相互作用时会诱导产生tRNA结合位点II。结果表明,在核糖体上,延伸因子Tu通过tRNA结合位点II与肽基位点结合的肽基tRNA相互作用,并通过tRNA结合位点I与氨酰位点结合的氨酰tRNA相互作用。

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