Nascent peptide exit tunnel

In the first step of the peptidyl transferase reaction, a peptidyl tRNA molecule is bound in the P-site with its nascent peptide extending down the peptide exit tunnel (Fig. 4.1). An elongation factor binds to a factor binding site (FBS) and positions an aminoacyl-tRNA in the A-site. The a amino group of the aminoacyl-tRNA nucleophilically attacks the ester bond which connects the peptide to the tRNA bound in the P-site (Fig. 4.2). The ester bond is broken as an amide bond forms, and the peptide becomes one amino acid longer, and is now attached to the tRNA that in the A-site. Translocation of the products follows peptide bond formation, as the newly formed deacylated- tRNA of the P-site moves into the E-site, and as the newly elongated peptidyl-tRNA moves from the A-site into the P-site. 

The bound macrolides almost completely occlude the peptide exit tunnel, which explains the two distinctive characteristics of macrolide inhibition. Firstly, the reason that macrolides do not inhibit ribosomes that are already actively making protein is that the nascent peptide in the exit tunnel blocks access to the macrolide binding site. Secondly, the reason macrolides do not directly inhibit the peptidyl transferase reaction is that they bind near to, but not directly at, the active site. Only after a few peptide bonds are formed will the peptide contact the bound macrolide and be blocked from further elongation. As a result, short di-, tri- and tetra-peptides will accumulate. 

Macrolides are a group of antibiotics, produced in nature by many actinomycetes strains, that are composed of a 12- to 16-membered lactone ring, to which one or more sugar substituents is attached. They target the peptidyl transferase center on the 50S ribosomal subunit and function primarily by interfering with movement of the nascent peptide away from the active site and into the exit tunnel. 

Figures 2 and 3). Peptide bond formation takes place at the peptidyl transferase center (PTC) and as the nascent peptide is extended, the single-stranded protein is extruded out the exit tunnel to further fold. One of the first... 

Deposition binding might cause a great conformational change in the overall three-dimensional structure essential for peptidyltransferase activity and the introduction of nascent peptide into the exit tunnel. Such modification also probably renders correct alignment of the peptidyl and aminoacyl substrates at the ribosome catalytic site, hindering peptide formation. In this connection, additional investigation is needed to obtain clear direct evidence. 

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