Methocinnamox

Not to be confused with Methoclocinnamox.

Methocinnamox (MCAM) is an opioid receptor antagonist.^[1][2] It is a pseudo-irreversible non-competitive antagonist of the μ-opioid receptor and a competitive antagonist of the κ- and δ-opioid receptors.^[1][2] The drug has a very long duration of action of up to months with a single dose due to its pseudo-irreversibility.^[1][2] It is administered in animals by intravenous or subcutaneous injection.^[1]

Methocinnamox

Clinical data
Other names	MCAM; M-CAM
Routes of administration	Intravenous, subcutaneous injection[1]
Drug class	Opioid receptor antagonist[1]
Identifiers
IUPAC name (E)-N-[(4R,4aS,7aR,12bR)-3-(Cyclopropylmethyl)-9-hydroxy-7-oxo-2,4,5,6,7a,13-hexahydro-1H-4,12-methanobenzofuro[3,2-e]isoquinolin-4a-yl]-3-(4-methylphenyl)prop-2-enamide
CAS Number	117339-76-1 N
PubChem CID	46877713
ChemSpider	24673142
ChEMBL	ChEMBL610884
Chemical and physical data
Formula	C30H32N2O4
Molar mass	484.596 g·mol−1
3D model (JSmol)	Interactive image
SMILES CC1=CC=C(C=C1)/C=C/C(=O)N[C@@]23CCC(=O)[C@H]4[C@@]25CCN([C@@H]3CC6=C5C(=C(C=C6)O)O4)CC7CC7
InChI InChI=1S/C30H32N2O4/c1-18-2-4-19(5-3-18)8-11-25(35)31-30-13-12-23(34)28-29(30)14-15-32(17-20-6-7-20)24(30)16-21-9-10-22(33)27(36-28)26(21)29/h2-5,8-11,20,24,28,33H,6-7,12-17H2,1H3,(H,31,35)/b11-8+/t24-,28+,29+,30-/m1/s1 Key:PJOHVEQSYPOERL-SHEAVXILSA-N

It was first described in the scientific literature in 2000.^[1][3][4] It has not been studied in humans as of 2022.^[1] There is interest in methocinnamox in the potential treatment of opioid use disorder and opioid overdose due to its much longer-lasting and insurmountable effects relative to other opioid antagonists like naloxone and naltrexone.^[1][2] Clinical trials of the drug are expected.^[3][5]

Methocinnamox should not be confused with methoclocinnamox (MCCAM), which is a closely related but structurally different compound (chlorine instead of methyl on one of the benzene rings).^[6][7] The drug was derived via structural modification of buprenorphine.^[8]

Pharmacology

Pharmacodynamics

Methocinnamox is an opioid receptor antagonist, it works at the μ-opioid receptor.^[1][2][9] By acting as an antagonist, it binds to the receptor but does not activate it, thus blocking the action of agonists such as heroin and fentanyl.^[1][2] It is a pseudo-irreversible non-competitive antagonist of the μ-opioid receptor and a competitive antagonist of the κ- and δ-opioid receptors.^[1][2]

Methocinnamox has affinity values for the opioid receptors of 0.6 nM for the μ-opioid receptor, 2.2 nM for the δ-opioid receptor, and 4.9 nM for the κ-opioid receptor.^[2] Hence, it has about 3.7-fold preferential affinity for the μ-opioid receptor over the δ-opioid receptor and about 8.2-fold higher affinity for the μ-opioid receptor over the κ-opioid receptor.^[2]

The antagonism of the μ-opioid receptor by methocinnamox is not irreversible as the drug does not form a covalent bond with the receptor.^[2] This is in contrast to prototypical μ-opioid receptor alkylating agents like β-funaltrexamine and β-chlornaltrexamine.^[2][4] However, in spite of its lack of covalent binding to the μ-opioid receptor, methocinnamox appears to not dissociate from the μ-opioid receptor or dissociates from it extremely slowly.^[2] Hence, methocinnamox has been described as a pseudo-irreversible antagonist of the μ-opioid receptor or as a "functionally irreversible" antagonist.^[2] The mechanism underlying the pseudo-irreversible antagonism of methocinnamox hasn't been fully elucidated.^[1] Also unlike irreversible μ-opioid receptor antagonists like β-funaltrexamine and β-chlornaltrexamine, methocinnamox lacks κ-opioid receptor agonism and is more selective for the μ-opioid receptor in its actions.^[4]

Methocinnamox has been found to bind to two distinct sites on the μ-opioid receptor.^[1] It binds to the orthosteric site as a pseudo-irreversible and non-competitive antagonist, thereby directly blocking opioid binding.^[1] In addition, methocinnamox has been found to bind to and act as an antagonist of an unknown allosteric site on the μ-opioid receptor with lower affinity that modulates the affinity and/or intrinsic activity of orthosteric μ-opioid receptor agonists.^[1]

The μ-opioid receptor antagonism of methocinnamox is non-competitive and insurmountable by μ-opioid receptor agonists like morphine and fentanyl.^[2][1] It has been found to completely block the effects of morphine at morphine doses of up to 1,000 mg/kg in animals, with the dose–response curve of morphine being shifted rightward by up to 100-fold.^[2][8] Doses of morphine of 1,000 mg/kg are normally often fatal.^[2] The insurmountability of methocinnamox's μ-opioid receptor antagonism is in contrast to that with competitive μ-opioid receptor antagonists like naloxone and naltrexone, which can be overcome with higher doses of μ-opioid receptor agonists.^[1][2]

In contrast to the μ-opioid receptor, the antagonism of the κ- and δ-opioid receptors by methocinnamox is competitive and reversible.^[1] Moreover, methocinnamox shows a short duration in the body.^[1] The actions of methocinnamox in vivo are selective for μ-opioid receptor antagonism, with a lack of significant antagonism of the effects of κ-opioid receptor agonists like bremazocine or δ-opioid receptor agonists like BW373U86.^[2]

The actions of methocinnamox are dose-dependent.^[2] A single dose of 3.2 mg/kg blocked the effects of morphine for approximately 2 weeks in animals whereas a single 10 mg/kg dose blocked the effects of morphine for over 2 months.^[2]

Pharmacokinetics

In animals, methocinnamox reached peak concentrations 15 to 45 minutes following injection and had an elimination half-life of approximately 70 minutes.^[1] In spite of this short duration in the body however, the μ-opioid receptor antagonist effects of methocinnamox persist for up to months with a single injection.^[1][2] These findings suggest that the long-lasting effects of methocinnamox are not due to pharmacokinetic factors but rather its pharmacodynamic properties and pseudo-irreversible antagonism.^[1]

Chemistry

In terms of chemical structure, methocinnamox is a cinnamoylamidomorphinan and is closely related to clocinnamox and methoclocinnamox.^[2][6] It was derived via structural modification of buprenorphine.^[8]

History

Clocinnamox was first described in the scientific literature by 1992.^[10] Methoclocinnamox, which is metabolically converted into clocinnamox and is a μ-opioid receptor partial agonist, was first described by 1995.^[11] Methocinnamox was first described in 2000.^[1][3][4]

Research

Opioid overdose and/or opioid use disorder

Methocinnamox is able to reverse the respiratory depressant effects of fentanyl and heroin in animals.^{[1][12][13][14]} However, unlike naloxone, another opioid antagonist, its action lasts around 2 weeks if administered subcutaneously and up to 5 days if administered intravenously.^[1][15] This could make it a better antidote than naloxone in opioid overdoses, because naloxone usually lasts around 30 minutes, there is a need for repeated administration and a danger of renarcotization.^[1][16] By acting longer, methocinnamox prevents these dangers.^[1]

Methocinnamox has not yet been tested in humans as of 2022.^[1] However, it has been tested in rodents and monkeys.^[2] It was reported in March 2020 that clinical trials of methocinnamox were expected to begin within 18 to 24 months.^[3] In March 2023, it was reported that a phase 1 clinical trial of methocinnamox funded by the National Institutes of Health (NIH) would possibly start in 2024.^[5]

See also

• 14-Cinnamoyloxycodeinone
• Fourphit