IGF1 and IGF2 specificities to the two insulin receptor isoforms are determined by insulin receptor amino acid 718

ConclusionMutating position 718 in human IR-B to the proline found at position 718 in human IR-A increased IGF1 and IGF2 affinity to a level comparable to IR-A and mutating position 718 in IR-A to the lysine found at position 718 in IR-B decreased IGF1 and IGF2 affinity to a level comparable to IR-B, whereas a negatively charged glutamate did not. These changes in the affinities were also reflected in the IR phosphorylation pattern, meaning that position 718 is important for both affinity and activation of the receptor. It should be emphasized that none of the mutations affected insulin affinity, indicating that the mutations did not alter the overall receptor structure and that the effect is ligand specific.

http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0178885

Source: PLoS One - June 1, 2017 Category: Biomedical Science Authors: Mie Andersen Source Type: research