SOLUTION STRUCTURE OF SELENOCYSTEINE-INSERTING TRANSFER RNA(SEC) FROM ESCHERICHIA-COLI - COMPARISON WITH CANONICAL TRANSFER RNA(SER)

被引:61
作者
BARON, C [1 ]
WESTHOF, E [1 ]
BOCK, A [1 ]
GIEGE, R [1 ]
机构
[1] UNIV MUNICH,LEHRSTUHL MIKROBIOL,W-8000 MUNICH 19,GERMANY
关键词
SELENOCYSTEINE-INSERTING TRANSFER RNA; CHEMICAL PROBES; NUCLEIC ACID CONFORMATION; GRAPHIC MODELING;
D O I
10.1006/jmbi.1993.1282
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Selenocysteine-inserting tRNAs (or tRNASec) are structurally untypical tRNAs that are charged by seryl-tRNA synthetase before being recognized by the selenocysteine synthase that converts serine into selenocysteine. tRNASec from Escherichia coli contains 95 nucleotides and is the longest tRNA known to date, in contrast to canonical tRNASer, 88 nucleotides-long. We have studied its solution conformation by chemical and enzymatic probing. Global structural features were obtained by cobra venom and S1 nuclease mapping, as well as by probing with Pb2+. Accessibilities of phosphate groups were measured by ethylnitrosourea probing. Information about positions in bases involved in Watson-Crick pairing, in stacking or in tertiary interactions were obtained by chemical probing with dimethylsulfate, diethylpyrocarbonate, kethoxal and carbodiimide. On the basis of these chemical data, a three-dimensional model was constructed by computer modeling and compared to that of canonical tRNASer. tRNASec resembles tRNASer at the level of its T-arm and anticodon-arm conformations, as well as at the joining of the D- and T-loops by a tertiary Watson-Crick G19-C56 interaction. Its extra-long variable arm is a double-stranded structure closed by a four nucleotide loop that is linked to the body of the tRNA in a way different from that found in tRNASer. As anticipated from the peculiar features of the sequence in the D-loop and at the junction of amino acid and D-arms, tRNASec possesses a novel but restricted set of tertiary interactions in the core of its three-dimensional structure: a G8-A21-UI4 triple pair and a novel interaction between C16 of the D-loop and C59 of the T-loop. A third triple interaction involving C15-G20a-G48 is suggested but some experimental evidence for it is still lacking. It is furthermore concluded that the D-arm has six base-pairs instead of three, as in canonical class II tRNASer, with the D-loop containing only four nucleotides. Finally, the amino acid accepting arm forms a stack of eight Watson-Crick base-pairs (instead of 7 in other tRNAs). The biological relevance of this model with regard to interaction with seryl-tRNA synthetase and enzymes from the selenocysteine metabolism is discussed. © 1993 Academic Press, Inc.
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页码:274 / 292
页数:19
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