The IRE is found in UTRs (untranslated regions) of various mRNAs whose products are involved in iron metabolism.

When iron concentration is low, IRPs bind the IRE in the ferritin mRNA and cause reduced translation rates.

In contrast, binding to multiple IREs in the 3' UTR of the transferrin receptor (involved in iron acquisition) leads to increased mRNA stability.

The two leading theories describe how iron probably interacts to impact posttranslational control of transcription.

The classical theory suggests that IRPs, in the absence of iron, bind avidly to the mRNA IRE.

The crystal structure and NMR data show a bulged U in the lower stem of the ferritin IRE.

[26] CDC14A encodes a dual-specificity phosphatase implicated in cell cycle control[27] and also interacts with interphase centrosomes.