AI Article Synopsis

  • The central melanocortin (MC) system regulates body weight by integrating signals through alpha-MSH (an agonist) and agouti-related protein (AgRP, an antagonist) at MC3 and MC4 receptors.
  • Recent research indicates that the human MC4R has constitutive activity, meaning it is active even without stimulation, and AgRP(83-132) can suppress this activity by acting as an inverse agonist.
  • This study suggests a new regulatory mechanism in the melanocortin system that could impact body weight regulation, allowing for further exploration of the roles of MC4R activity and AgRP's inverse agonism.

Article Abstract

The central melanocortin (MC) system has been demonstrated to act downstream of leptin in the regulation of body weight. The system comprises alpha-MSH, which acts as agonist, and agouti-related protein (AgRP), which acts as antagonist at the MC3 and MC4 receptors (MC3R and MC4R). This property suggests that MCR activity is tightly regulated and that opposing signals are integrated at the receptor level. We here propose another level of regulation within the melanocortin system by showing that the human (h) MC4R displays constitutive activity in vitro as assayed by adenylyl cyclase (AC) activity. Furthermore, human AgRP(83-132) acts as an inverse agonist for the hMC4R since it was able to suppress constitutive activity of the hMC4R both in intact B16/G4F melanoma cells and membrane preparations. The effect of AgRP(83-132) on the hMC4R was blocked by the MC4R ligand SHU9119. Also the hMC3R and the mouse(m)MC5R were shown to be constitutively active. AgRP(83-132) acted as an inverse agonist on the hMC3R but not on the mMC5R. Thus, AgRP is able to regulate MCR activity independently of alpha-MSH. These findings form a basis to further investigate the relevance of constitutive activity of the MC4R and of inverse agonism of AgRP for the regulation of body weight.

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Source
http://dx.doi.org/10.1210/mend.15.1.0578DOI Listing

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