GRF analogs and fragments: correlation between receptor binding, activity and structure.
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Campbell RM, Lee Y, Rivier J, Heimer EP, Felix AM, Mowles TF
GRF analogs and fragments: correlation between receptor binding, activity and structure.
Peptides. 1991 May-Jun;12(3):569-74.
- PubMed ID
- 1656403 [ View in PubMed]
- Abstract
GH-releasing activity in vitro was directly correlated with GRF receptor binding affinity for all hGRF analogs examined. hGRF(1-29)-NH2 analogs with Ala15-substitution (for Gly15) displayed 4-5 times higher affinity for the GRF receptor relative to hGRF(1-44)-NH2. Replacement of Gly15 with Sar15 resulted in a dramatic loss of activity and receptor binding. The present data supports the proposal that Ala15-substitution increases receptor affinity, and hence potency, due to increased amphiphilic alpha-helical interactions. Fragments of hGRF, representative of DPP-IV and trypsin-like cleavage, are inactive as a consequence of greatly diminished GRF receptor binding. These results provide a comprehensive analysis of the structural features required for both GRF receptor binding and activation.
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