AI Article Synopsis
- Nerve injury and inflammation increase dynorphin A levels in the spinal cord, leading to heightened pain sensitivity through interactions with bradykinin receptors, which can't be blocked by standard opioid antagonists.
- Structural studies on dynorphin A have highlighted two promising ligands that maintain key features for effective bradykinin receptor binding but suffer from poor stability in plasma.
- Modifications, including cyclizing one of these ligands, have enhanced its metabolic stability while retaining binding affinity, indicating potential for developing a new drug scaffold.
Article Abstract
Nerve injury and inflammation cause up-regulation of an endogenous opioid ligand, dynorphin A (Dyn A), in the spinal cord resulting in hyperalgesia via the interaction with bradykinin receptors (BRs). This is a non-opioid neuroexcitatory effect that cannot be blocked by opioid antagonists. Our systematic structure-activity relationships study on Dyn A identified lead ligands 1 and 4, along with the key structural feature (i.e. amphipathicity) for the BRs. However, the ligands showed very low metabolic stability in plasma (t <1h) and therefore, in order to improve their metabolic stabilities with retained biological activities, various modifications were performed. Cyclization of ligand 4 afforded a cyclic Dyn A analogue 5 that retained the same range of binding affinity as the linear ligand with improved metabolic stability (t >5h) and therefore possesses the potential as a pharmacophoric scaffold to be utilized for drug development.
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Source |
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5159310 | PMC |
| http://dx.doi.org/10.1016/j.bmcl.2016.10.010 | DOI Listing |
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