Etomidate and Etomidate Analog Binding and Positive Modulation of γ-Aminobutyric Acid Type A Receptors

McGrath, Megan; Yu, Zhiyi; Jayakar, Selwyn S.; Ma, Celena; Tolia, Mansi; Zhou, Xiaojuan; Miller, Keith W.; Cohen, Jonathan B.; Raines, Douglas E.

doi:10.1097/aln.0000000000002356

Cited by 9 publications

(12 citation statements)

References 28 publications

(39 reference statements)

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“…40 mg/kg) or a 2-hr etomidate analog infusion lost their righting reflexes. Such a lack of sedative-hypnotic activity among the etomidate analogs is consistent with previous electrophysiological work showing that these analogs are essentially devoid of the GABA A receptor positive modulatory actions thought to mediate the sedative-hypnotic effects of etomidate [24,38,39].…”

Section: Discussionsupporting

confidence: 90%

“…However, the active site cavity volumes of these two enzymes are estimated to be 360 Å 3 (11b-hydroxylase) and 334 Å 3 (18hydroxylase), which are only modestly larger than the molecular volume of etomidate (269.7 Å 3 ) [31]. The addition of the various bulky substituents groups to etomidate (to form our four etomidate analogs) increases molecular volume by between 39.9 Å 3 and 52.7 Å 3 , potentially introducing steric hindrance and reducing the binding affinity to these enzymes [24]. Such a reduction in affinity could explain -at least in part -why the four phenyl ring substituent-containing analogs tended to produce smaller reductions in plasma corticosterone and aldosterone concentrations than etomidate.…”

Section: Discussionmentioning

confidence: 96%

“…As part of a strategy to overcome this limitation we developed (R)-ethyl 1-(1-(3,5dimethoxyphenyl)ethyl)-1H-imidazole-5-carboxylate (dimethoxy-etomidate), a phenyl ring substituted etomidate analog that retains the potent 11β-hydroxylase inhibitory activity of etomidate but is essentially devoid of the drug's GABA A receptor modulatory and sedative-hypnotic actions [23]. In the current manuscript, we describe studies to further define the pharmacology of this compound along with three additional phenyl ring substituted etomidate analogs that are similarly lacking in significant GABA A receptor modulatory activity (Fig 2) [24]. We also characterized the pharmacology of etomidate to provide context.…”

Section: Introductionmentioning

confidence: 99%

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Behavioral and Steroidogenic Pharmacology of Phenyl Ring Substituted Etomidate Analogs in Rats

McGrath

Hofmann

Raines

2019

Preprint

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Background: Cushing’s syndrome is an endocrine disorder characterized by the overproduction of adrenocortical steroids and associated with significant morbidity. Steroidogenesis enzyme inhibitors are the mainstays of pharmacological treatment. Unfortunately, they produce side effects that limit dosing, efficacy, and patient tolerability. Among the most potent inhibitors is the general anesthetic etomidate whose GABAA receptor-mediated sedative-hypnotic actions restrict use. In this study, we defined the sedative-hypnotic and steroidogenesis inhibiting actions of etomidate and four phenyl-ring substituted etomidate analogs (dimethoxy-etomidate, isopropoxy-etomidate, naphthalene-etomidate, and naphthalene(2)-etomidate) that possess negligible GABAA receptor modulatory activities. Methods: In the first set of experiments, male Sprague-Dawley rats were assessed for loss of righting reflexes (LoRR) after receiving intravenous boluses of either etomidate (1 mg/kg) or an etomidate analog (40 mg/kg). In the second set of experiments, rats were assessed for LoRR and their abilities to produce adrenocortical and androgenic steroids after receiving 2-hr infusions (0.5 mg kg-1min-1) of either etomidate or an etomidate analog. Results: All rats that received etomidate boluses or infusions had LoRR that persisted for minutes or hours, respectively. In contrast, no rat that received an etomidate analog had LoRR. Compared to rats in the vehicle control group, rats that received etomidate analog infusions had plasma corticosterone and aldosterone concentrations that were reduced by 80 – 84% and 68 – 94%, respectively. Rats that received etomidate infusions had plasma corticosterone and aldosterone concentrations that were also significantly reduced (by 92% and 96%, respectively). Rats that received etomidate or isopropoxy-etomidate had significant reductions (90% and 57%, respectively) in plasma testosterone concentrations whereas those that received naphthalene-etomidate had significant increases (1,400%) in plasma dehydroepiandrosterone concentrations. Neither etomidate nor any etomidate analog significantly affected plasma androstenedione and dihydrotestosterone concentrations. Conclusions: Our studies demonstrate that the four phenyl-ring substituted etomidate analogs form a novel class of compounds that are devoid of sedative-hypnotic activities and suppress plasma concentrations of adrenocortical steroids but vary in their effects on plasma concentrations of androgenic steroids. They provide a proof-of-concept for the development of non-sedating etomidate analogs to treat Cushing’s syndrome and other pathologies whose clinical courses may be improved by altering steroid biosynthesis.

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

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Behavioral and Steroidogenic Pharmacology of Phenyl Ring Substituted Etomidate Analogs in Rats

McGrath

Hofmann

Raines

2019

Preprint

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“…The degree of selectivity for such general sites has been surprising. Ligand-gated ion channels, such as the GABA A -R or Gloeobacter Ligand-gated Ion Channel (GLIC) for example, show considerable selectivity for sites - [3,[6][7][8][9] -despite producing similar changes in activity ( Figure 1). Even volatile anesthetics may exhibit a degree of non-overlapping site occupancy as suggested by recent photolabeling studies [3].…”

Section: Site Character and Selectivitymentioning

confidence: 99%

“…This approach has verified a large number of plausible targets, including, but not limited to: specific ligand-gated ion channels [147,148], voltage-gated channels [149,150], hyperpolarizationactivated cyclic nucleotide (HCN)-gated and tandem pore potassium (K 2 P) channels [151], and mitochondrial proteins [152]. Attempts to distinguish functional significance of these many targets has used sensitivity, stereoselectivity [153], alkanol cutoff effect [9,154], and other phenomenological observations, some of which has caused further ambiguity. Nevertheless, this has been a powerful approach that has constrained the degree of potential complexity.…”

mentioning

confidence: 99%

Towards a Comprehensive Understanding of Anesthetic Mechanisms of Action: A Decade of Discovery

Hemmings

Riegelhaupt

Kelz

et al. 2019

Trends in Pharmacological Sciences

166

180

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Significant progress has been made in the 21 st century towards a comprehensive understanding of the mechanisms of action of general anesthetics, coincident with progress in structural biology and molecular, cellular, and systems neuroscience. This review summarizes important new findings that include target identification through structural determination of anesthetic binding sites, details of receptors and ion channels involved in neurotransmission, and the critical roles of neuronal networks in anesthetic effects on memory and consciousness. These recent developments provide a comprehensive basis for conceptualizing pharmacologic control of amnesia, unconsciousness, and immobility.

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Endocrine disruptors of inhibiting testicular 3β-hydroxysteroid dehydrogenase

Zhang

Wang

et al. 2019

Chemico-Biological Interactions

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Etomidate and Etomidate Analog Binding and Positive Modulation of γ-Aminobutyric Acid Type A Receptors

Cited by 9 publications

References 28 publications

Behavioral and Steroidogenic Pharmacology of Phenyl Ring Substituted Etomidate Analogs in Rats

Behavioral and Steroidogenic Pharmacology of Phenyl Ring Substituted Etomidate Analogs in Rats

Towards a Comprehensive Understanding of Anesthetic Mechanisms of Action: A Decade of Discovery

Endocrine disruptors of inhibiting testicular 3β-hydroxysteroid dehydrogenase

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