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蓝氏贾第鞭毛虫大亚基核糖体RNA的结构域V:一种早期分支真核生物肽基转移酶环的结构及其与抗生素敏感性的相关性

Domain V of Giardia lamblia large-subunit rRNA: structure of the peptidyl transferase loop from an early-branching eukaryote and correlation with antibiotic sensitivity.

作者信息

Edlind T D, Cha M E, Prah G N, Katiyar S K

机构信息

Department of Microbiology and Immunology, Medical College of Pennsylvania, Philadelphia 19129.

出版信息

Gene. 1993 Feb 14;124(1):67-74. doi: 10.1016/0378-1119(93)90762-r.

DOI:10.1016/0378-1119(93)90762-r
PMID:8440482
Abstract

Large subunit rRNA (LSR) sequences that have been implicated in peptide bond formation form a specific secondary structure called the peptidyl transferase loop (PTL). Although well conserved, the PTLs of eubacteria, archaebacteria, and eukaryotes have several distinct differences. These differences correlate with different sensitivities to peptidyl transferase and translocase inhibitors. To shed light on the basis for these kingdom-specific differences in PTL structure and function, we have analyzed the sequence and secondary structure of LSR domain V, which contains the PTL, from Giardia lamblia. This parasitic protozoan derives from a very early branch in eukaryotic evolution, and its rRNA was previously shown to have bacteria-like features. In vitro and cell-free systems were also used to test the sensitivity of G. lamblia protein synthesis to specific PTL-targeted inhibitors. Our results indicate that the PTL structure and inhibitor sensitivity typical of higher eukaryotes is conserved in G. lamblia. However, several adjacent domain V sequences more closely resemble archaebacterial rRNA, confirming the 'primitive' nature of G. lamblia rRNA. Thus, the eukaryotic PTL has been conserved over a vast evolutionary period. We speculate that the eukaryotic PTL is primordial and employs specific RNA-RNA interactions to catalyze protein synthesis. Three potential interactions were identified.

摘要

已被证实与肽键形成有关的大亚基核糖体RNA(LSR)序列形成了一种特定的二级结构,称为肽基转移酶环(PTL)。尽管PTL高度保守,但真细菌、古细菌和真核生物的PTL仍存在一些明显差异。这些差异与对肽基转移酶和转位酶抑制剂的不同敏感性相关。为了阐明这些PTL结构和功能在不同界别中的差异根源,我们分析了来自蓝氏贾第鞭毛虫的包含PTL的LSR结构域V的序列和二级结构。这种寄生原生动物起源于真核生物进化的一个非常早期的分支,其rRNA先前已被证明具有类似细菌的特征。体外和无细胞系统也被用于测试蓝氏贾第鞭毛虫蛋白质合成对特定PTL靶向抑制剂的敏感性。我们的结果表明,高等真核生物典型的PTL结构和抑制剂敏感性在蓝氏贾第鞭毛虫中是保守的。然而,几个相邻的结构域V序列与古细菌rRNA更相似,证实了蓝氏贾第鞭毛虫rRNA的“原始”性质。因此,真核生物的PTL在漫长的进化过程中一直保持保守。我们推测真核生物的PTL是原始的,并利用特定的RNA-RNA相互作用来催化蛋白质合成。我们确定了三种潜在的相互作用。

相似文献

1
Domain V of Giardia lamblia large-subunit rRNA: structure of the peptidyl transferase loop from an early-branching eukaryote and correlation with antibiotic sensitivity.蓝氏贾第鞭毛虫大亚基核糖体RNA的结构域V:一种早期分支真核生物肽基转移酶环的结构及其与抗生素敏感性的相关性
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