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Should inverse agonists be defined by pharmacological mechanism or clinical effect?

Published online by Cambridge University Press:  20 March 2019

Ethan S. Burstein*
Affiliation:
Department of Biosciences, ACADIA Pharmaceuticals, Inc., San Diego, CA, USA
*
*Address for correspondence: Ethan S. Burstein, ACADIA Pharmaceuticals, Inc., 3611 Valley Center Drive, San Diego, CA 92130, USA. (Email: eburstein@acadia-pharm.com)
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Abstract

Type
Editorial
Copyright
© Cambridge University Press 2019 

Pimavanserin was recently approved for treating hallucinations and delusions associated with Parkinson’s disease.Reference Hacksell, Burstein and McFarland 1 It is the first approved drug that selectively targets the 5-HT2A receptor and is termed a selective serotonin inverse agonist. This has motivated a debate about which drugs should be classified as inverse agonists – those that display clear evidence of inverse agonist activity in vitro, or only those that have demonstrated clinical evidence of inverse agonism.Reference Nutt, Stahl and Blier 2 This is a valid question. Here I advance the view that drugs are defined by their in vitro pharmacological profiles and mechanisms of action to the extent that these mechanisms are understood. Constitutive receptor activity and inverse agonism are now well-defined pharmacological properties, documented at the structural level. Therefore, calling pimavanserin an inverse agonist based on its molecular pharmacology properties is appropriate.

Definitions

Constitutive activity or basal activity is defined as receptor-mediated activity in the absence of agonists. Receptors are flexible proteins and undergo spontaneous conformational changes between inactive conformations and active conformations capable of signaling. This model is formally identical to the allosteric model of enzyme activation.Reference Monod, Wyman and Changeux 3 In this context, agonists increase receptor activity by stabilizing active conformations, and inverse agonists suppress receptor activity by stabilizing inactive conformations.Reference Neubig, Spedding and Kenakin 4

Antagonists are defined as compounds that reduce the receptor-mediated responses to other compounds. Commonly this means blocking the actions of an agonist by competing for the same binding site (competitive antagonism), although other forms of antagonism also exist (e.g., allosteric antagonism). In practice, many antagonists are also inverse agonists because they both suppress spontaneous or constitutive receptor activity and block actions of agonists. This is the case for pimavanserin.

Structural Basis

The theoretical model for receptor constitutive activity and the actions of agonists and inverse agonists have all been captured in fine structural detail. Excellent examples can be found in a recent paper from Manglik et al.Reference Manglik, Kim and Masureel 5 These studies employed 19F-fluorine NMR and double electron-electron resonance spectroscopy to visualize the structural dynamics of spontaneous conformational changes of the β2 adrenergic receptor (β2AR) and interactions of β2AR receptors with agonists, inverse agonists, and G-proteins.

Manglik et al. showed that there are at least two forms, each of active and inactive conformations (see Figure 6A in ref. [5]). Furthermore, they observed that an inverse agonist destabilized the active conformations and stabilized two rapidly interconverting inactive conformations. They further described two active conformations, a partially active conformation that was promoted by agonist binding and a fully activated conformation that was stabilized by both an agonist and the G-protein. These results are consistent with the concept of spontaneous transitions occurring between inactive and active conformations, with inverse agonists favoring inactive conformations, and agonists and G-proteins promoting active conformations.

Pharmacological Consequences

A variety of pharmacological data are explained by these structural observations. It is known that mutations often constitutively activate G-protein-coupled receptors (GPCRs). These observations validate the concept that constitutive activity is an intrinsic property of GPCRs, and that many GPCR ligands are inverse agonists. In a classic study, all 19 possible amino acid substitutions for the wild-type alanine at position 293 constitutively activated the α1b adrenergic receptor.Reference Kjelsberg, Cotecchia and Ostrowski 6 Since such divergent amino acid substitutions all raised constitutive activity, it was inferred that the mutations disrupted a “constraining function” of that region of the receptor, releasing spontaneous receptor activity. This would only happen if there was a natural tendency for the receptor to adopt active conformations.

We reached a similar conclusion from a series of studies employing large-scale random mutagenesis that showed that constitutively activating mutations (CAMs) are common, are clustered in key conformational “switch” regions, and divergent classes of amino acid substitutions are capable of constitutively activating the M5 receptor, similar to what was observed with the α1b adrenergic receptor.Reference Spalding and Burstein 7 Together, these studies support the concept of receptors as flexible proteins that interconvert between inactive and active states, which in turn can be promoted by inverse agonists and agonists, respectively.

Another important implication from the structural studies described above is that G-proteins would be expected to stabilize active conformations of GPCRs. This predicts that GPCRs coupled to G-proteins would have higher affinity for agonists than uncoupled GPCRs; that overexpressing G-proteins would promote the constitutive activity of GPCRs; and that inverse agonists would suppress G-protein-induced constitutive activity – all of which have been demonstrated experimentally.Reference Burstein, Spalding and Brann 8

Constitutive Activity of GPCRs, 5-HT2A Receptors, and Inverse Agonist Activity of Pimavanserin

Using a proprietary high-throughput functional assay called Receptor Selection and Amplification Technology (RSAT™) that is very sensitive to differences in the constitutive activity of GPCRs, we evaluated well over 100 GPCR targets during the course of our drug discovery efforts.Reference Burstein, Piu and Ma 9 These assessments were carried out with wild-type, unmutated receptors. We observed a tremendous variability in the degree of constitutive activity for each receptor, ranging from very low (H1 histamine, 5-HT2B) to very high (5-HT2C).Reference Weiner, Burstein and Nash 10 Where comparisons are possible, our findings correlated with observations of others. Receptors with high constitutive activity in RSAT™ were receptors for which others observed constitutive activity in native systems or in vivo, such as the M2 muscarinic receptor,Reference Spalding and Burstein 7 the ghrelin receptor,Reference Burstein, Spalding and Brann 8 , Reference Mear, Enjalbert and Thirion 11 and the 5-HT2C receptor.Reference Weiner, Burstein and Nash 10 , Reference Aloyo, Berg and Clarke 12 Compared to all of the receptors we tested, the 5-HT2A receptor has constitutive activity levels ranking approximately in the top third, below the levels we saw for 5-HT2C and ghrelin, but well above many other receptors such as the 5-HT2b serotonin receptor (Burstein, unpublished observations).

Several reports describe the constitutive activity of 5-HT2A receptors in vivo in regulating the responses to an associative learning test – the acquisition of the rabbit’s learned eyeblink response (extension of the nictitating membrane) to a conditioned stimulus.Reference Aloyo, Berg and Clarke 12 The reflexive or motor response to an unconditioned stimulus was also recorded. The authors described three classes of 5-HT2A drugs: agonists that enhanced learning, antagonists that had no effect on learning, and inverse agonists that impeded learning. Moreover, they demonstrated that the antagonists could block the effects of both agonists and inverse agonists in this paradigm. To confirm the genuine constitutive activity of 5-HT2A receptors, these experiments were successfully repeated with depletion of endogenous 5-HT by the neurotoxin 5,7-dihydroxytryptamine.Reference Romano, Quinn and Liu 13

We profiled many of the compounds described in ref. [12] in RSAT™. All of the compounds we identified as inverse agonists in RSAT™ (M100907, Ritanserin, Mianserin, SR46349N, Ketanserin) were inverse agonists in the learned eyeblink test, and all but Ketanserin were inverse agonists in the motor response. Two compounds, d-Bromolysergic acid diethylamide (BOL) and LY-53,857, were identified as pure antagonists in both the learned and motor eyeblink response. We did not profile BOL but found that LY-53,857 behaves like a pure 5-HT2A antagonist in RSAT™ in that it blocks the effects of both agonists, such as 5-carboxytryptamine, and inverse agonists, such as ritanserin and pimavanserin, but has little intrinsic activity of its own (Burstein, unpublished observations).

Recently a number of valid issues have been raised regarding extrapolating the clinical relevance of findings from in vitro pharmacology experiments. Using slow wave sleep (SWS) as an example, the difficulties of distinguishing the in vivo actions of 5-HT2A inverse agonists from 5-HT2A antagonists have been noted.Reference Nutt, Stahl and Blier 2 The attempt to correlate SWS with inverse agonism is confounded by the fact that many of the compounds listed in Table 1 of Nutt et al. are not selective, and interact with other receptors that may affect SWS. There are published reports distinguishing 5-HT2A inverse agonism from antagonism in vivo, suggesting that these different in vitro profiles may have meaningful consequences in vivo.Reference Aloyo, Berg and Clarke 12 Despite this report, the physiological impact of the constitutive activity of 5-HT2A receptors in vivo is still not well understood, and thus it is difficult to say what clinical differences may exist between 5-HT2A inverse agonists and pure antagonists. Further work is warranted to understand the biological significance of inverse agonism at 5-HT2A receptors. Nevertheless, our position is that pimavanserin is appropriately defined by its pharmacological properties, which are consistent with the most current understanding of GPCR pharmacology. The term “inverse agonist” is a pharmacological term that accurately describes the pharmacological properties of pimavanserin, and that is our basis for designating pimavanserin as a selective serotonin inverse agonist.

Disclosures

Dr. Burstein is an employee of ACADIA Pharmaceuticals, Inc.

References

References:

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