The search for the “next” euphoric non-fentanil novel synthetic opioids on the illicit drugs market: current status and horizon scanning

The antinociceptive effects of the N-substituted cyclomethylbenzamides were explored by Brittain et al. [17] at the United Kingdom pharmaceutical company, Allen and Hanburys Limited, in collaboration with the University of Aston, Birmingham, UK. The company had been acquired by Glaxo in 1958, but retained its name until 1978 after which it was subsumed into Glaxo Group Research Ltd. A series of compounds were synthesized and tested in vivo in mice. Harper et al. [11] published details of the synthesis of a series of 60 cyclohexyl derivatives (1-(3,4-dichloro-benzamidomethyl)cyclohexyl-dimethylamines). Thirty-five of these were subjected to preliminary pharmacological screening. Tests were carried out at oral doses of 100 mg/kg (behaviour, body temperature, antimaximal electroshock, antagonism of leptazol-induced convulsions, and effects on phenylquinone-induced writhing); oral doses of 50 mg/kg (tremor, hypothermia); and a subcutaneous dose of 100 mg/kg (hot-plate effects observed directly and on interaction with morphine). The N-substituted benzamide derivatives, identified as compounds 51-53, 57 and 58 in the paper [11], some of which were also reported in the Brittain et al. paper referred to using their “AH” codes [17], were identified as the most promising compounds (see Fig. 1 for the generic structure and Table 1 for structural details). One compound in particular, 3,4-dichloro-N-[1-(dimethylamino)-cyclohexyl]methylbenzamide, named AH-7921, was identified as having the greatest analgesic properties, approximately 0.8 times that of morphine in comparative studies, and was selected for further acute animal studies. This work, including detailed synthesis methods, was submitted as a United States patent in 1974, assigned to Allen and Hanburys Limited, the patent being granted in 1976 [28]. During these studies, there was evidence of the addictive potential of AH-7921, with physical dependence observed in the animals tested and so trials were discontinued at that time [17]. Further animal testing was carried out by the Glaxo Group Research Ltd, later confirming that undesirable effects (e.g. Straub tail response, hypothermia, sedation, respiratory depression and inhibition of gastrointestinal propulsion) occurred at concentrations similar to those required for analgesia confirming that this compound should not be selected for further study [29].

N-Substituted benzamides and acetamides From 1973, chemists at the Upjohn Company synthesized a series of N-(2-aminocycloaliphatic)benzamide compounds leading, in 1975, to the discovery of the selective kappa-opioid receptor (KOR) agonist, U-50488 (trans-2-(3,4-dichlorophenyl)-N-methyl-N-(1S,2S)-2-(pyrrolidin-1-yl)cyclohexyl)-acetamide), Fig. 2. The (−) trans-(1S,2S) isomer, also referred to as U-50488H, had greater affinity for KOR than the (+) trans-(1R,2R) or either of the cis-configurations or the (±) trans-racemic mixture, highlighting the need to take into account the important effect of stereochemistry on their pharmacological behaviour [15]. A large number of related compounds were patented in 1978 [12] and further related patents followed [e.g. 30, 31]. Information on some of these compounds is provided in Table 2. A number of different methodologies to determine in vitro opioid receptor binding affinity (K_D) have been used in the cited literature and care should be taken when comparing such data directly between studies. Perhaps a more useful measure of comparison between studies is the relative affinity of the test compound to the different opioid receptors. Binding affinity to a target receptor is of itself not a direct measure of “potency” and such methods do not take into account off-target pharmacological effects which may affect downstream biological effects and toxicity.

A detailed description of U-50488H was first published in the peer reviewed literature in 1982 [18, 19]. It did not cause respiratory depression and was not habit-forming, but was found to cause sedation, diuresis and dysphoria, the latter properties being undesirable in medicinal products and indicative of KOR-mediated effects. The (−) trans-(1S,2S) U-50488 (U-50488H) and the (±) trans-racemic mixture are commercially available as reagents from specialist chemical supply companies (e.g. Merck, Tocris Bioscience, Axon Medchem etc.) and are widely used as model KOR agonists in experimental studies [15]. The discovery and deconvolution of the structure activity relationships of U-50488H, and its related compounds, including the important role of stereochemistry in agonist activity, was elegantly described by the Upjohn chemist responsible for its development, Jacob Szmuszkovicz [15]. The generic structure of the N-substituted benzamides and acetamides is shown in Fig. 2a. The structural requirements for a potent KOR agonist appear to be a combination of the following: (1) a (−) trans-(1S,2S) configuration; (2) the presence of an N-methyl group on the nitrogen adjacent to the carbonyl and (3) the presence of a methylene (CH₂) “spacer” [15]. This is further illustrated by the modifications of the U-50488H structure which lead to the synthesis of two further highly selective KOR agonists with a (−) trans-(1S,2S) configuration; U-62066 (spiradoline, 2-(3,4-dichlorophenyl)-N-methyl-N-[(5R,7S,8S)-7-pyrrolidin-1-yl-1-oxaspiro[4.5]decan-8-yl]acetamide) and U-69593 (N-methyl-2-phenyl-N-[(5R,7S,8S)-7-pyrrolidin-1-yl-1-oxaspiro[4.5]decan-8-yl]acetamide) both of which have a heterocyclic ring structure fused to the cyclohexyl moiety in the R₃ position (Fig. 2a, Table 1) [20‐22].

The properties of U-50488H were compared to those of the assumed novel mu-opioid (MOR) agonists U-47109 (3,4-dichloro-N-(2-(dimethylamino)cyclohexyl)benzamide), U-47700 and U-51754 (2-(3,4-dichlorophenyl)-N-[2-(dimethylamino)cyclohexyl]-N-methyl-acetamide) (Fig. 2) to demonstrate the drug’s selectivity for the KOR [13]. In this study, U-47700, which has a (+) trans-(1R,2R) configuration (and it is assumed U-47109 and U-51754 also have the same configuration), was found to have 7.5, eight and three times greater analgesic effect than morphine in antinociceptive tests (tail flick, tail pinch and hydrochloric acid writhing respectively). U-50488H, U-51754 and U-47109 were found to be less potent than morphine, but still had measurable analgesic effects [13]. Characteristic MOR mediated effects (Straub tail, arched back, increased locomotor activity) were observed when mice were treated with U-47700, U-51754 and U-47109 but were not observed for U-50488H.

Further deconvolution of the “U-drug” structure activity relationships to MOR and KOR was reported in 1988 [14]. The removal of a chlorine atom in the meta-position on the phenyl moiety of U-47700 to give U-48520 (4-chloro-N-(2-(dimethylamino)cyclohexyl)-N-methylbenzamide) leads to an apparent decrease in MOR affinity and further removing the chlorine in the para-position and replacing it with a hydroxyl group leads to a complete loss of affinity to both MOR and KOR (Table 2). The presence of the methylene bridge in the structure appears to decrease affinity to MOR and increase affinity to KOR (Table 2).

Opioid receptor binding profiles and the antinociceptive properties of further related compounds were investigated in 1989 by Fujimoto et al. [32] including U-77891 (trans-3,4-dibromo-N-methyl-N-[1-methyl-1-azaspiro[4.5]decan-6-yl]benzamide) (Table 2). This compound was first described in an Upjohn Company patent from 1985 [30] and is an N-substituted tertiary amide containing a heterocyclic ring structure on the cyclohexyl moiety, an N-methyl group adjacent to the carbonyl and halogen atoms in the 3,4-positions of the aromatic ring (bromines instead of chlorines of U-50488/U-47700), but unlike U-50488 and U-51754 no methylene spacer is present. Other closely related analogues (referred to as compounds 29-32 in the paper) are also described. The lack of the methylene spacer (and possibly a (+) trans-(1R, 2R) configuration—although this is not specifically mentioned) in the structures of U-77891 and compounds 29-32 appears to produce highly selective MOR agonists. The presence of halogens in the 3,4-position of the aromatic ring appears to enhance activity and is likely to protect the aromatic moiety from enzymatic hydroxylation once the substance is consumed. The selective MOR agonist properties of U-47700 were further confirmed in a more recent study [33]. Despite the development of a wide range of related compounds in later patents, U-47700 has remained one of the substances in this class with the greatest reported analgesic potency and greatest MOR binding.

4-Aminocyclohexanols Around the same time that the N-substituted benzamide and acetamide compounds were being developed at the Upjohn Company, a patent was filed in 1979 and published in 1982 for a series of 4-aminocyclohexanol compounds [34]. Trans-4-(p-Bromophenyl)-4-(dimethylamino)-1-phenethylcyclohexanol, referred to simply as “compound 1” in the original research paper (BDPC, also referred to as bromadol in online drug user discussion fora and vendor sites) was found to be a highly potent analgesic in animal studies (tail flick, tail pinch, hydrochloric acid writhing), effects that were reversed by naloxone, indicating that the analgesic activity was mediated via the MOR [35]. The trans isomer was determined to be considerably more potent than the cis isomer (Fig. 3), the molecular structure being found to be superimposable upon the molecular structure of the potent synthetic opioid fentanyl [35].

It was originally stated that BDPC/bromadol had 10,000 times the analgesic potency of morphine in animal studies [34] although a more recent study, comparing analgesic potency using a standard mouse hot plate assay where BDPC/bromadol was introduced by intraperitoneal injection, suggests that its analgesic potency may be lower, at around 500 times that of morphine and 2.9 times that of fentanyl [36]. BDPC/bromadol was the lead compound for a further series of 4-amino-4-arylcyclohexanone analogues and their derivatives prepared by the Upjohn team to provide structure activity relationship data [16, 37, 38]. None had analgesic properties greater than BDPC/bromadol, although a trans-chlorinated analogue showed similar potency as did an analogue where the phenethyl moiety was replaced with a cyclohex-3-ene moiety [37]. Another analogue of BDPC/bromadol, trans-4-(p-bromophenyl)-4-(dimethylamino)-1-(2-thiophen-2-yl-ethyl)-cyclohexanol (C8813, thiobromadol Fig. 3.) was synthesized and characterized in 2003 [36]. This work was the first to study receptor binding affinities for both BDPC/bromadol (K_i = 1.49 nM for MOR) and C8813 (K_i = 1.37, 3.24 and > 1000 nM for MOR, DOR and KOR respectively). The antinociceptive potency observed previously and in the same study is perhaps greater than that expected given the opioid receptor binding affinity data presented and so warrants further detailed study. As far as the authors are aware, none of these substances have been subject to clinical trials and none have been developed commercially, although a method for the purification of BDPC/bromadol after synthesis was published by a Chinese research team in 2014 and refers to a “commercially available bromadol” solution bought from a Chinese vendor [39].

There are a number of drug-related internet fora and online drug user communities. The benefits and risks of the use of data from such fora for novel illicit drug research purposes have been discussed previously [103, 104]. When using such sites, users are generally seeking reports of drug use and experiential information and will also post self-reports on the characteristics of novel drugs and their subjective experiences with them. Previous studies have identified four main themes of the discussion threads on such fora where users sought (1) reliable information on novel and emerging substances, (2) dosage and administration information, (3) information on subjectively experienced effects of novel and emerging substances, and (4) support and safety information from other users [103]. Online communities such as this have been previously described as having a self-regulating approach to novel drugs appearing on the illicit market, rapidly sharing information on either harms associated with novel substances or if subjective effects are positive or negative. Researchers seeking information from such fora must acknowledge that the motivation for users to post information about new substances cannot be verified and the actual substance taken by the user can also not be verified—a user may not have been sold the substance they believe they have been sold by a web vendor. In addition, researchers must be aware of the placebo effect with regards to a self-reported subjective experience; the fact that users may have used other substances before, during or after the substance under test; and as regular drug users, they are likely to have built up tolerances to, in this case, opioids which will affect their response to a particular substance. Nevertheless, some useful information can be obtained on the timeline of the appearance of new drugs on the market and users subjective experience of them. The information provided below gives examples of online discussion fora threads only and is not an exhaustive list of such discussions available online.

Online discussions on U-49900 have already been reported previously [83] and are not discussed in detail here. Postings referencing either U-51754 or its alternative name, methene-U-47700, began to appear between May and September 2016 indicating that the drug had appeared on web vendor sites. One user referred to U-51754 as an alternative to U-47700 after the latter had “become illegal” and predicted that it might be dysphoric rather than euphoric [105]. Another user reported taking the drug rectally and claimed the effects were strong, dysphoric and dissociative and with a relatively short duration of around 45 min [106]. Forum posts in another discussion thread, discuss the original research published by the Upjohn Company [107]. Other users reported unpleasant dissociative experiences with no euphoria [108]. The reaction from forum users is generally negative and advice to avoid the substance has been communicated. Postings referencing U-48800 began to appear in April 2017 [109, 110]. In general, the response to this drug by users of online fora has been, as for U-51754, generally negative, although some posts have indicated a more positive, but mild experience [110]. User fora discussions of U-47931E/bromadoline started to appear around September 2017 and appear to identify variability in the products sold as U-47931E/bromadoline on vendor websites and also indicate that vendors were providing samples for testing with other purchases. In early posts, at least two distinct batches of the drug were discussed, one white in colour and one brown/tan. Detailed user reports for both batches describe distinct subjective user experience differences between the two [111, 112]. Insufflation of the brown/tan sample allegedly produced a rush and euphoria whilst another user states that the subjective effects of U-47931e/bromadoline are milder than for U-47700, but last longer [113, 114].

Discussions relating to 3-4-methylenedioxy-U47700 appeared in May and June 2017 [115, 116] and for isopropyl-U-47700 appear to start around November and December 2017 with users stating the latter drug had been offered for sale on vendor sites [117, 118]. The user response to these substances appears almost uniformly negative.

BDPC/bromadol has been discussed on online user fora for many years [e.g. 119, 120]; however, substances purporting to be BDPC/bromadol seem to have recently increased in prevalence on vendor sites (early to mid 2017). Since then a number of experiential reports have been posted and a common theme of such user reports is the lack of the sought after euphoric effects [8, 121]. Some users posting on a German language forum have reported buying BDPC/bromadol as a purported 10 mg/mL solution [121]. Due to its reported analgesic potency in animal studies, its reported MOR affinity, its appearance on vendor sites in a number of forms and the potential for harm, the prevalence of this compound in drug seizures and toxicological samples should be closely monitored.

It seems clear, at least from the limited information provided from drug user forum posts, that novel U-drug analogues and BDPC/bromadol are appearing on web vendor sites, although they may appear and disappear over relatively short time periods based on availability and user demand or response. Their actual prevalence in casework and appearance in biological samples is mostly unknown, but would be expected, at this time, to be very low. In general, the majority of these compounds, in the reports available, have been viewed negatively relative to the user experiences relating to U-47700. Given an understanding of the structure activity relationships and known pharmacology of those U-drug analogues that have been studied, this may be seen as not overly surprising. It will be interesting to observe if users will grow tired of trying these subjectively unpopular analogues or if they will continue to experiment with new analogues as they enter the market in the hope of a more subjectively positive user experience.