Possible role of flanking nucleotides in recognition of the AUG initiator codon by eukaryotic ribosomes.
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Sequences flanking the initiator codon in eukaryotic mRNAs are not random. Out of 153 messages examined, 151 have either a purine in position -3, or a G in position +4, or both. Thus, [A/G]XXAUGG emerges as the favored sequence for eukaryotic initiation sites. Nucleotides flanking nonfunctional AUG triplets, which occur in the 5'-noncoding region of a few eukaryotic messages, are different from those found at most functional sites. Whereas most authentic initiator codons are preceded by a purine (usually A) in position -3, most nonfunctional AUGs have a pyrimidine in that position. The observed asymmetry suggests that purines in positions -3 and +4 might facilitate recognition of the AUG condon during formation of initiation complexes. To test this idea, in vitro binding studies were carried out with 32P-labeled oligonucleotides. Binding of AUG-containing oligonucleotides to wheat germ ribosomes was significantly enhanced by placing a purine in position -3 or +4. The scanning model, which postulates that 40S ribosomal subunits attach at the 5'-end of a message and migrate down to the AUG codon, is discussed in light of these new observations. A modified version of the scanning mechanism is proposed.
[1] P. H. Hofschneider,et al. Current Topics in Microbiology and Immunology , 1981, Current Topics in Microbiology and Immunology.
[2] R. Schimke,et al. Biological Regulation and Development , 1979, Biological Regulation and Development.
[3] E. Reich. Procedures in Nucleic Acid Research. G. L. Cantoni and David R. Davies, Eds. Harper and Row, New York, 1966. 683 pp., illus. $25 , 1967 .
[4] V. Georgiev. Virology , 1955, Nature.