Figure 1.

Model for miRNA-mediated repression. The interaction between GW182 and any of the Ago proteins is the first event of or occurs during micro(mi)RNA-target interaction. Several different pathways downstream of GW182 are possible. The specific pathway is probably determined by the composition of the RNA-induced silencing complex (RISC) and interaction with mRNA-ribonucleoprotein (mRNP) complex), microRNA-associated ribonucleoproteins (miRNPs), or cellular factors. (a) GW182 mediates deadenylation, followed by de-capping and mRNA degradation via NOT/CCR4/CAF1 complexes; this is the primary non-cleaving degradation pathway and considered separate from the translational repression pathway. (b) GW182 competes with eIF4G in association with poly-A binding protein (PABP), preventing the circularization required for efficient translation. (c) The 60S ribosome is prevented from joining with the 40S ribosome to form 80S ribosomes. Steps (b) and (c) represent initiation blocks. (d) Slowed or stalled ribosomes along the mRNA, representing a translation elongation block. (e) Premature translation termination and (f) co-translation degradation.