Your search keyword '"Phencyclidine analogs & derivatives"' showing total 665 results

1. Phencyclidine-Like Abuse Liability and Psychosis-Like Neurocognitive Effects of Novel Arylcyclohexylamine Drugs of Abuse in Rodents.

Author

Shaw HE, Patel DR, Gannon BM, Fitzgerald LR, Carbonaro TM, Johnson CR, and Fantegrossi WE

Subjects

Animals, Male, Mice, Rats, Psychoses, Substance-Induced etiology, Cyclohexylamines, Motor Activity drug effects, Cognition drug effects, Conditioning, Operant drug effects, Locomotion drug effects, Illicit Drugs adverse effects, Illicit Drugs toxicity, Ketamine analogs & derivatives, Ketamine toxicity, Substance-Related Disorders psychology, Phencyclidine Abuse, Phencyclidine analogs & derivatives, Phencyclidine toxicity, Rats, Sprague-Dawley

Abstract

Abuse of novel arylcyclohexylamines (ACX) poses risks for toxicities, including adverse neurocognitive effects. In vivo effects of ring-substituted analogs of phencyclidine (PCP), eticyclidine (PCE), and ketamine are understudied. Adult male National Institutes of Health Swiss mice were used to assess locomotor effects of PCP and its 3-OH, 3-MeO, 3-Cl, and 4-MeO analogs, PCE and its 3-OH and 3-MeO analogs, and ketamine and its deschloro and 2F-deschloro analogs, in comparison with those of methamphetamine (METH), 3,4-methylenedioxymethamphetamine (MDMA), and two benzofuran analogs of MDMA. PCP-like interoceptive effects for all of these ACXs were determined using a food-reinforced drug discrimination procedure in adult male Sprague Dawley rats. A novel operant assay of rule-governed behavior incorporating aspects of attentional set-shifting was used to profile psychosis-like neurocognitive effects of PCP and 3-Cl-PCP in rats, in comparison with cocaine and morphine. PCP-like ACXs were more effective locomotor stimulants than the amphetamines, PCE-like ACXs were as effective as the amphetamines, and ketamine-like ACXs were less effective than the amphetamines. Addition of -Cl, -OH, or -OMe at the 3-position on the aromatic ring did not impact locomotor effectiveness, but addition of -OMe at the 4-position reduced locomotor effectiveness. Lethal effects were induced by drugs with -OH at the 3-position or -OMe at the 3- or 4-position. All novel ACXs substituted at least partially for PCP, and PCP and 3-Cl-PCP elicited dose-dependent psychosis-like neurocognitive deficits in the rule-governed behavior task not observed with cocaine or morphine. Novel ACXs exhibit substantial abuse liability and toxicities not necessarily observed with their parent drugs. SIGNIFICANCE STATEMENT: Novel arylcyclohexylamine analogs of PCP, PCE, and ketamine are appearing on the illicit market, and abuse of these drugs poses risks for toxicities, including adverse neurocognitive effects. These studies demonstrate that the novel ACXs exhibit PCP-like abuse liability in the drug discrimination assay, elicit varied locomotor stimulant and lethal effects in mice, and induce psychosis-like neurocognitive effects in rats., (U.S. Government work not protected by U.S. copyright.)

Published

2024

2. Intoxication by 3-MeO-PCP and O-desmethyltramadol: an unusual NPS mix.

Author

Castro AL, da Costa MJCSP, Tarelho S, Sousa L, Russo F, and Franco JM

Subjects

Humans, Male, Psychotropic Drugs analysis, Phencyclidine analogs & derivatives, Phencyclidine analysis, Tramadol analogs & derivatives

Abstract

Over the past few years, the new psychoactive substances' phenomenon has been continuously studied. Its dynamic context is characterized by a broad diversity of substances, including several groups, such as synthetic cathinones, synthetic opiates, and synthetic cannabinoids. However, and due both to this diversity and to the low number of detected cases, information on intoxication reports is always important, in order to understand their biological mechanisms. In this case, a male individual was found unresponsive, with some different powders and paraphernalia near him. After toxicological analysis to the powders, paraphernalia, and whole blood samples, five different compounds were identified. From these, two of them (3-MeO-PCP and o-desmethyltramadol) were identified and quantitated in the whole blood sample. The obtained results suggested that death was due to the presence and action of these two substances, in what may be considered an unusual mix of NPS. This case highlights the value of evaluating all the traces found in the scene investigation and the need of sending all the paraphernalia found for toxicological examination, together with all the possible information obtained on the scene, namely by relatives or witnesses. On the other hand, this case shows the significance of broad-spectrum analytical methods, in order to detect and identify, as specifically as possible, eventual substances present and used by victims., (© 2022. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2022

3. The First Fatal Intoxication with 3-MeO-PCP in the UK and a Review of the Literature.

Author

Copeland CS, Hudson S, Treble R, and Hamnett HJ

Subjects

Chromatography, Liquid, United Kingdom, Hallucinogens toxicity, Phencyclidine analogs & derivatives

Abstract

The phencyclidine derivative 3-methoxyphencyclidine (3-MeO-PCP) is a potent dissociative hallucinogen. Sought for recreational use as a novel psychoactive substance, it can also induce acute psychological agitation and pathophysiological cardiorespiratory effects. Due to the harms associated with its use, 3-MeO-PCP was added to the "Green List" of materials covered by the 1971 Convention on Psychotropic Substances as a Schedule II substance by the United Nations Commission on Narcotic Drugs in April 2021. There have been 15 previous reports of fatal intoxications following 3-MeO-PCP use, but only one was attributable to 3-MeO-PCP intoxication alone. In this report, we detail the first fatality due to 3-MeO-PCP intoxication to be reported in the UK, along with a review of the surrounding literature. While the blood concentrations associated with 3-MeO-PCP toxicity and fatality remain unclear, by providing details of sample collection and storage conditions, this case will aid in future interpretations. Furthermore, this case suggests that 3-MeO-PCP toxicity may be exacerbated by exercise. Users of 3-MeO-PCP should be cautioned against its use as a "club drug" or in a similar setting where elevations in heart rate, body temperature and blood pressure may occur., (© The Author(s) 2022. Published by Oxford University Press. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2022

4. In vitro and in vivo metabolism and detection of 3-HO-PCP, a synthetic phencyclidine, in human samples and pooled human hepatocytes using high resolution mass spectrometry.

Author

Davidsen AB, Mardal M, Johansen SS, Dalsgaard PW, and Linnet K

Subjects

Hallucinogens analysis, Hepatocytes metabolism, Humans, Phencyclidine analogs & derivatives, Phencyclidine analysis, Substance Abuse Detection methods, Tissue Distribution, Chromatography, Liquid methods, Hallucinogens pharmacokinetics, Mass Spectrometry methods, Phencyclidine pharmacokinetics

Abstract

The new psychoactive substance (NPS) 3-HO-PCP, a phencyclidine (PCP) analog, was detected in a law enforcement seizure and in forensic samples in Denmark. Compared with PCP, 3-HO-PCP is known to be a more potent dissociative NPS, but no toxicokinetic investigations of 3-HO-PCP are yet available. Therefore, 3-HO-PCP was quantified in in vivo samples, and the following were investigated: plasma protein binding, in vitro and in vivo metabolites, and metabolic targets. All samples were separated by liquid chromatography and analyzed by mass spectrometry. The unbound fraction in plasma was determined as 0.72 ± 0.09. After in vitro incubation with pooled human hepatocytes, four metabolites were identified: a piperidine-hydroxyl-and piperidine ring opened N-dealkyl-COOH metabolite, and O-glucuronidated- and O-sulfate-conjugated metabolites. In vivo, depending on the sample and sample preparation, fewer metabolites were detected, as the O-sulfate-conjugated metabolite was not detected. The N-dealkylated-COOH metabolite was the main metabolite in the deconjugated urine sample. in vivo analytical targets in blood and brain samples were 3-HO-PCP and the O-glucuronidated metabolite, with 3-HO-PCP having the highest relative signal intensity. The drug levels of 3-HO-PCP quantified in blood were 0.013 and 0.095 mg/kg in a living and a deceased subject, respectively. The 3-HO-PCP concentrations in deconjugated urine in a sample from a living subject and in post-mortem brain were 7.8 and 0.16 mg/kg, respectively. The post mortem results showed a 1.5-fold higher concentration of 3-HO-PCP in the brain tissue than in the post mortem blood sample., (© 2020 John Wiley & Sons, Ltd.)

Published

2020

5. The Abuse Potential of Novel Synthetic Phencyclidine Derivative 1-(1-(4-Fluorophenyl)Cyclohexyl)Piperidine (4'-F-PCP) in Rodents.

Author

Ryu IS, Kim OH, Lee YE, Kim JS, Li ZH, Kim TW, Lim RN, Lee YJ, Cheong JH, Kim HJ, Lee YS, Steffensen SC, Lee BH, Seo JW, and Jang EY

Subjects

Animals, Behavior, Addictive physiopathology, Dopamine metabolism, Dopamine Plasma Membrane Transport Proteins metabolism, Male, Mice, Mice, Inbred C57BL, Nucleus Accumbens metabolism, Phencyclidine metabolism, Proto-Oncogene Proteins c-fos metabolism, Psychomotor Performance drug effects, Rats, Rats, Sprague-Dawley, Receptors, Dopamine D1 metabolism, Reinforcement, Psychology, Reward, Self Administration, Phencyclidine analogs & derivatives, Phencyclidine pharmacology, Phencyclidine Abuse metabolism

Abstract

The dissociative anesthetic phencyclidine (PCP) and PCP derivatives, including 4'-F-PCP, are illegally sold and abused worldwide for recreational and non-medical uses. The psychopharmacological properties and abuse potential of 4'-F-PCP have not been fully characterized. In this study, we evaluated the psychomotor, rewarding, and reinforcing properties of 4'-F-PCP using the open-field test, conditioned place preference (CPP), and self-administration paradigms in rodents. Using Western immunoblotting, we also investigated the expression of dopamine (DA)-related proteins and DA-receptor-mediated downstream signaling cascades in the nucleus accumbens (NAc) of 4'-F-PCP-self-administering rats. Intraperitoneal administration of 10 mg/kg 4'-F-PCP significantly increased locomotor and rearing activities and increased CPP in mice. Intravenous administration of 1.0 mg/kg/infusion of 4'-F-PCP significantly enhanced self-administration during a 2 h session under fixed ratio schedules, showed a higher breakpoint during a 6 h session under progressive ratio schedules of reinforcement, and significantly altered the expression of DA transporter and DA D1 receptor in the NAc of rats self-administering 1.0 mg/kg 4'-F-PCP. Additionally, the expression of phosphorylated (p) ERK, pCREB, c-Fos, and FosB/ΔFosB in the NAc was significantly enhanced by 1.0 mg/kg 4'-F-PCP self-administration. Taken together, these findings suggest that 4'-F-PCP has a high potential for abuse, given its robust psychomotor, rewarding, and reinforcing properties via activation of DAergic neurotransmission and the downstream signaling pathways in the NAc., Competing Interests: The authors declare no conflict of interest. The funders had no role in the design of the study; in the collection, analyses, or interpretation of data; in the writing of the manuscript, or in the decision to publish the results.

Published

2020

6. 4-MeO-PCP and 3-MeO-PCMo, new dissociative drugs, produce rewarding and reinforcing effects through activation of mesolimbic dopamine pathway and alteration of accumbal CREB, deltaFosB, and BDNF levels.

Author

Abiero A, Botanas CJ, Custodio RJ, Sayson LV, Kim M, Lee HJ, Kim HJ, Lee KW, Jeong Y, Seo JW, Ryu IS, Lee YS, and Cheong JH

Subjects

Animals, Designer Drugs administration & dosage, Illicit Drugs pharmacology, Male, Mice, Mice, Inbred C57BL, Nucleus Accumbens drug effects, Phencyclidine administration & dosage, Rats, Rats, Sprague-Dawley, Reward, Self Administration, Signal Transduction drug effects, Signal Transduction physiology, Brain-Derived Neurotrophic Factor metabolism, Cyclic AMP Response Element-Binding Protein metabolism, Dopamine metabolism, Morpholines administration & dosage, Nucleus Accumbens metabolism, Phencyclidine analogs & derivatives, Proto-Oncogene Proteins c-fos metabolism

Abstract

Rationale: A high number of synthetic dissociative drugs continue to be available through online stores, leading to their misuse. Recent inclusions in this category are 4-MeO-PCP and 3-MeO-PCMo, analogs of phencyclidine. Although the dissociative effects of these drugs and their recreational use have been reported, no studies have investigated their abuse potential., Objectives: To examine their rewarding and reinforcing effects and explore the mechanistic correlations., Methods: We used conditioned place preference (CPP), self-administration, and locomotor sensitization tests to assess the rewarding and reinforcing effects of the drugs. We explored their mechanism of action by pretreating dopamine receptor (DR) D1 antagonist SCH23390 and DRD2 antagonist haloperidol during CPP test and investigated the effects of 4-MeO-PCP and 3-MeO-PCMo on dopamine-related proteins in the ventral tegmental area and nucleus accumbens. We also measured the levels of dopamine, phosphorylated cyclic-AMP response element-binding (p-CREB) protein, deltaFosB, and brain-derived neurotrophic factor (BDNF) in the nucleus accumbens. Additionally, we examined the effects of both drugs on brain wave activity using electroencephalography., Results: While both 4-MeO-PCP and 3-MeO-PCMo induced CPP and self-administration, only 4-MeO-PCP elicited locomotor sensitization. SCH23390 and haloperidol inhibited the acquisition of drug CPP. 4-MeO-PCP and 3-MeO-PCMo altered the levels of tyrosine hydroxylase, DRD1, DRD2, and dopamine, as well as that of p-CREB, deltaFosB, and BDNF. All drugs increased the delta and gamma wave activity, whereas pretreatment with SCH23390 and haloperidol inhibited it., Conclusion: Our results indicate that 4-MeO-PCP and 3-MeO-PCMo induce rewarding and reinforcing effects that are probably mediated by the mesolimbic dopamine system, suggesting an abuse liability in humans.

Published

2020

7. Severe Toxicity to the New Psychoactive Substances 3-Hydroxyphencyclidine and N-Ethylhexedrone: an Analytically Confirmed Case Report.

Author

Dunlop LC, Wood D, Archer J, Hudson S, and Dargan P

Subjects

Humans, Male, Middle Aged, Phencyclidine chemical synthesis, Phencyclidine poisoning, Poisoning physiopathology, Poisoning therapy, Predictive Value of Tests, Psychotropic Drugs chemical synthesis, Severity of Illness Index, Substance-Related Disorders physiopathology, Substance-Related Disorders therapy, Urinalysis, Phencyclidine analogs & derivatives, Poisoning diagnosis, Psychotropic Drugs poisoning, Substance Abuse Detection, Substance-Related Disorders diagnosis

Abstract

Introduction: 3-Hydroxyphencyclidine (3-HO-PCP) is a new psychoactive substance (NPS) and a hydroxy derivative of phencyclidine (PCP), and N-ethylhexedrone (Hexen) is a synthetic cathinone. We describe an analytically confirmed case of acute toxicity related to the use of both 3-hydroxyphencyclidine and N-ethylhexedrone., Case Report: A 56-year-old male was brought to the Emergency Department by ambulance with hyperthermia (39.9 °C), sinus tachycardia (150 beats per minute), reduced consciousness, ocular clonus, and vertical nystagmus. He was treated with cooled intravenous (IV) fluids and IV benzodiazepines. Following 1 hour of treatment, his temperature fell to 37.7 °C, he developed rhabdomyolysis (creatine kinase peaked at 5999 IU (normal range < 229 IU)): he was managed with supportive measures and was discharged after 25 hours. The patient admitted regular use of Hexen and recent use of 3-HO-PCP. Analysis of urine and serum identified 3-hydroxyphencyclidine and metabolites, N-ethylhexedrone and metabolites, and clephedrone and metabolites., Discussion: This is a case of analytically confirmed toxicity to 3-HO-PCP and N-ethylhexedrone. The acute toxicity reported in this patient is consistent with the use of 3-HO-PCP, but there were sympathomimetic and serotonergic features potentially consistent with the cathinone N-ethylhexedrone. The description of the acute toxicity of NPS, such as these, is vital to aid medical toxicologists and emergency medicine physicians treating patients who use them.

Published

2020

8. Intoxication with 3-MeO-PCP alone: A case report and literature review.

Author

Berar A, Allain JS, Allard S, Lefevre C, Baert A, Morel I, Bouvet R, and Gicquel T

Subjects

Adolescent, Humans, Hypertension chemically induced, Male, Phencyclidine blood, Phencyclidine poisoning, Phencyclidine urine, Substance-Related Disorders complications, Substance-Related Disorders diagnosis, Tachycardia chemically induced, Designer Drugs poisoning, Phencyclidine analogs & derivatives

Abstract

Rationale: 3-Methoxyphencyclidine (3-MeO-PCP) is a new psychoactive substance derived from phencyclidine. Although it can lead to severe intoxications, the main manifestations and optimal management have not been well characterized. Here, we report 2 cases of 3-MeO-PCP intoxication in the same patient, and summarize the manifestations of this intoxication reported in literature., Patient Concerns: A 17-year-old male purchased a bag of 3-MeO-PCP on the Internet but took an oral dose (200 mg) that corresponds to the less active isomer 4-MeO-PCP. He developed high blood pressure (158/131 mm Hg), tachycardia (100 bpm), and neurological manifestations (confusion, hypertonia, nystagmus, and then agitation). A maculopapular rash appeared, although this may have been related to the administration of midazolam. Hyperlactatemia (2.6 mmol/L) was the main laboratory finding. Seven days later, he returned to the emergency department after sniffing 50 mg of 3-MeO-PCP. High blood pressure, tachycardia, and neurological manifestations (psychomotor impairment and dysarthria) were present but less severe than after the first intoxication., Diagnosis: In the first intoxication, the blood and urine 3-MeO-PCP concentrations were, respectively, 71.1 ng/mL and 706.9 ng/mL. Conventional toxicity tests were all negative. In the second intoxication, biological samples were not available., Interventions: In the first intoxication, treatment consisted of intravenous hydration and midazolam. The patient was transferred to an intensive care unit for monitoring. After the second intoxication, he was monitored for 12 hours., Outcomes: The patient's condition improved quickly in both cases., Lessons: These cases provide additional information on the manifestations of 3-MeO-PCP intoxication. These manifestations are mainly cardiovascular (high blood pressure, tachycardia) and neurological. The fact that second (50 mg) intoxication was less severe than the first (200 mg) is suggestive of a dose-effect relationship for 3-MeO-PCP. The first case also emphasizes the risk of dosing errors caused by the similarity between the names "3-MeO-PCP" and "4-MeO-PCP."

Published

2019

9. Detectability of Dissociative Psychoactive Substances in Urine by Five Commercial Phencyclidine Immunoassays.

Author

Gomila I, Leciñena MÁ, Elorza MÁ, Pastor Y, Sahuquillo L, Servera M, Puiguriguer J, and Barcelo B

Subjects

Body Fluids, Cyclohexanones, Cyclohexylamines, Drug Overdose, Humans, Ketamine, Immunoassay, Phencyclidine analogs & derivatives, Psychotropic Drugs urine

Abstract

Methoxetamine (MXE) and the arylcyclohexylamines 3-methoxy-PCP (3-MeO-PCP) and 4-methoxy-PCP (4-MeO-PCP) are substituted analogs of the dissociative psychoactive substances ketamine and phencyclidine (PCP), respectively. They have emerged on the new psychoactive substances (NPS) market as legal alternatives to these classically banned dissociatives. Little data has been published regarding the cross-reactivity of these NPS in PCP immunoassays (IAs). The aim of this work was to explore the possibilities of detecting 3-MeO-PCP, 4-MeO-PCP, MXE and ketamine in commercial IAs for PCP. The cross-reactivity study was performed in five different PCP IAs using urine-free, spiked samples and urine samples obtained from two 3-MeO-PCP overdose cases. 3-MeO-PCP and 4-MeO-PCP showed cross-reactivity (ranging from 1-143%) in all PCP IAs evaluated. MXE only showed very weak cross-reactivity (ranged from 0.04 to 0.25%) and ketamine was not detected in any PCP IA evaluated. Urine samples from the two overdose cases were positive for PCP in all IAs evaluated. The commercial PCP IAs evaluated exhibited utility as rapid, preliminary screening techniques for 3-MeO-PCP and 4-MeO-PCP, but not for ketamine. The low reactivity of MXE limits its detectability in the PCP IAs evaluated., (© The Author(s) 2019. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2019

10. The risk of emerging new psychoactive substances: The first fatal 3-MeO-PCP intoxication in The Netherlands.

Author

de Jong LAA, Olyslager EJH, and Duijst WLJM

Subjects

Adult, Amphetamine blood, Blood Alcohol Content, Chromatography, Liquid, Designer Drugs analysis, Humans, Male, Mass Spectrometry methods, Netherlands, Phencyclidine blood, Phencyclidine poisoning, Psychotropic Drugs blood, Substance-Related Disorders blood, Designer Drugs poisoning, Phencyclidine analogs & derivatives, Psychotropic Drugs poisoning

Abstract

Structural analogs of classic drugs, also called designer drugs, are a booming market due to the easy accessibility on the internet and their legal status. One of those 'legal highs' is an analog of phencyclidine, namely 3-methoxyphencyclidine (3-MeO-PCP). Very few fatalities have been reported where 3-MeO-PCP contributed to the death of an individual. We present the first fatal case in the Netherlands and one of the few worldwide. Postmortem biological samples and the presumed abused unknown substance, sold as ant poison, were obtained. 3-MeO-PCP was detected, and the resulting concentration was 152 μg/l in whole blood. The presumed taken unknown sample was identified as 3-MeO-PCP and thus linked to the victim. The cause of death was a combination of 3-MeO-PCP, amphetamine, and alcohol. Improved diagnostic skills are necessary to face these emerging novel psychoactive substances also in light of public health and social risks., (Copyright © 2019 Elsevier Ltd and Faculty of Forensic and Legal Medicine. All rights reserved.)

Published

2019

11. Application of a molecular networking approach for clinical and forensic toxicology exemplified in three cases involving 3-MeO-PCP, doxylamine, and chlormequat.

Author

Allard S, Allard PM, Morel I, and Gicquel T

Subjects

Adolescent, Antiemetics analysis, Female, Humans, Male, Middle Aged, Phencyclidine analysis, Tandem Mass Spectrometry methods, Young Adult, Chlormequat analysis, Designer Drugs analysis, Doxylamine analysis, Forensic Toxicology methods, Phencyclidine analogs & derivatives

Abstract

Untargeted toxicological screening is an analytical challenge, given the high number of molecules and metabolites to be detected and the constant appearance of new psychoactive substances (NPS). The combination of liquid chromatography with high-resolution tandem mass spectrometry (HRMS/MS) in a data-dependent acquisition mode generates a large volume of high quality spectral data. Commercial software for processing MS data acquired during untargeted screening experiments usually compare measured features (mass, retention time, and fragmentation spectra) against a predefined list of analytes. However, there is a lack of tools for visualizing and organizing MS data of unknown compounds. Here, we applied molecular networking to untargeted toxicological screening. This bioinformatic tool allows the exploration and organization of MS/MS data without prior knowledge of the sample's chemical composition. The organization of spectral data is based on spectral similarity. Hence, important information can be obtained even before the annotation step. The link established between molecules enables the propagation of structural information. We applied this approach to three clinical and forensic cases with various matrices: (a) blood and a syringe content in a forensic case of death by self-injection, (b) hair segments in a case of drug-facilitated assault, and (c) urine and blood samples in a case of 3-methoxyphencyclidine intoxication. Data preprocessing with MZmine allows sample-to-sample comparison and generation of multisample molecular networks. Our present study shows that molecular networking can be a useful complement to conventional approaches for untargeted screening interpretation, for example for xenobiotics identification or NPS metabolism elucidation., (© 2018 John Wiley & Sons, Ltd.)

Published

2019

12. Metabolites to parent 3-MeO-PCP ratio in human urine collected in two fatal cases.

Author

Ameline A, Greney H, Monassier L, Raul JS, and Kintz P

Subjects

Adult, Autopsy, Chromatography, Liquid, Designer Drugs, Fatal Outcome, Female, Femoral Artery, Forensic Toxicology, Humans, Illicit Drugs blood, Illicit Drugs urine, In Vitro Techniques, Male, Microsomes, Liver drug effects, Microsomes, Liver metabolism, Osmolar Concentration, Phencyclidine blood, Phencyclidine urine, Tandem Mass Spectrometry, Drug Overdose blood, Drug Overdose urine, Hallucinogens blood, Hallucinogens urine, Phencyclidine analogs & derivatives, Substance Abuse Detection

Abstract

In this article, two fatal cases related to the use of 3-methoxyphencyclidine (3-MeO-PCP) are described. This compound is a new psychoactive substance that belongs to the phencyclidine family. In the recent period, this dissociative drug has gained interest because of its proposal as a legally available alternative to phencyclidine in some countries. The scientific literature related to 3-MeO-PCP is very poor. Using standard ultra-performance liquid chromatography-mass spectrometry and ultra-performance liquid chromatography-tandem mass spectrometry, the authors focused on the detection of 3-MeO-PCP and its metabolites in human urine. 3-MeO-PCP metabolism was studied in vitro after drug incubation with human liver microsomes and the identified metabolites were investigated in the urine of the two forensic cases. 3-MeO-PCP metabolites, including O-demethyl-3-MeO-PCP, piperidine-hydroxy-3-MeO-PCP, O-demethyl-piperidine-di-hydroxy-3-MeO-PCP and piperidine-di-hydroxy-3-MeO-PCP, were detectable in the urine from both cases and the ratio between metabolites and parent 3-MeO-PCP, always lower than 1, were calculated to estimate the proportionality of metabolites. At this stage, one can conclude that testing for 3-MeO-PCP metabolites does not increase the window of detection of the drug., (© The Author(s) 2018. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2019

13. Murdered while under the influence of 3-MeO-PCP.

Author

Kintz P, Ameline A, Walch A, Farrugia A, and Raul JS

Subjects

Adult, Bile chemistry, Chromatography, Liquid, Female, Gas Chromatography-Mass Spectrometry, Hair chemistry, Humans, Phencyclidine analysis, Substance Abuse Detection, Substance-Related Disorders blood, Substance-Related Disorders urine, Tandem Mass Spectrometry, Designer Drugs analysis, Drug Users, Hallucinogens analysis, Homicide, Phencyclidine analogs & derivatives

Abstract

The abuse of new psychoactive substances (NPS) has been dramatically increasing all around the world since the late 2000s. The availability of hundreds of NPS in the past decade is challenging for both public health and global drug policies. A 39-year-old woman, known as a multidrug addict, was murdered by her partner by ligature strangulation. A comprehensive toxicological screening by gas chromatography and ultra-high performance liquid chromatography with tandem mass spectrometry revealed the simultaneous presence of ethanol (1.37 g/L), diazepam (157 ng/mL) and nordiazepam (204 ng/mL), cocaine (25 ng/mL) and benzoylecgonine (544 ng/mL), and (3-methoxy-(1-(1-phenylcyclohexyl)piperidine) or 3-MeO-PCP, a dissociative hallucinogen anesthetic drug. Concentrations of 3-MeO-PCP were 63, 64, and 94 ng/mL in femoral blood, bile, and urine, respectively. Hair tested also positive for 3-MeO-PCP on 3 × 2-cm segments at 731, 893, and 846 pg/mg, indicating long-term abuse of the drug. This seems to be the first ever reported hair concentrations. Major impairment of the victim, including visual hallucinations and alteration of behavior, was attributed to the mixture of all the drugs, with a major contribution of 3-MeO-PCP. The toxicological findings were compared to the few reports available in the medical literature.

Published

2019

14. Syntheses, analytical and pharmacological characterizations of the 'legal high' 4-[1-(3-methoxyphenyl)cyclohexyl]morpholine (3-MeO-PCMo) and analogues.

Author

Colestock T, Wallach J, Mansi M, Filemban N, Morris H, Elliott SP, Westphal F, Brandt SD, and Adejare A

Subjects

Anesthetics, Dissociative metabolism, Animals, Humans, Ketamine chemistry, Phencyclidine analysis, Phencyclidine chemical synthesis, Phencyclidine pharmacology, Piperidines chemistry, Rats, Anesthetics, Dissociative chemistry, Ketamine pharmacology, Morpholines analysis, Morpholines chemical synthesis, Morpholines pharmacology, Phencyclidine analogs & derivatives, Piperidines pharmacology, Receptors, N-Methyl-D-Aspartate chemistry, Receptors, N-Methyl-D-Aspartate metabolism

Abstract

New psychoactive substances (NPS) are commonly referred to as 'research chemicals', 'designer drugs' or 'legal highs'. One NPS class is represented by dissociative anesthetics, which include analogues of the arylcyclohexylamine phencyclidine (PCP), ketamine and diphenidine. A recent addition to the NPS market was 4-[1-(3-methoxyphenyl)cyclohexyl]morpholine (3-MeO-PCMo), a morpholine analogue of 3-MeO-PCP. Although suspected to have dissociative effects in users, information about its pharmacological profile is not available. From clinical and forensic perspectives, detailed analytical data are needed for identification, especially when facing the presence of positional isomers, as these are frequently unavailable commercially. This study presents the analytical and pharmacological characterization of 3-MeO-PCMo along with five additional analogues, namely the 2- and 4-MeO-PCMo isomers, 3,4-methylenedioxy-PCMo (3,4-MD-PCMo), 3-Me-PCMo and PCMo. All six arylcyclohexylmorpholines were synthesized and characterized using chromatographic, mass spectrometric and spectroscopic techniques. The three positional isomers could be differentiated and the identity of 3-MeO-PCMo obtained from an internet vendor was verified. All six compounds were also evaluated for affinity at 46 central nervous system receptors including the N-methyl-d-aspartate receptor (NMDAR), an important target for dissociative anesthetics such as PCP and ketamine. In vitro binding studies using (+)-[3- 3 H]-MK-801 in rat forebrain preparations revealed moderate affinity for NMDAR in the rank order of 3-Me >3-MeO > PCMo >3,4-MD > 2-MeO > 4-MeO-PCMo. 3-MeO-PCMo was found to have moderate affinity for NMDAR comparable to that of ketamine, and had an approximate 12-fold lower affinity than PCP. These results support the anecdotal reports of dissociative effects from 3-MeO-PCMo in humans., (Copyright © 2017 John Wiley & Sons, Ltd.)

Published

2018

15. Two Fatal Intoxications Involving 3-Methoxyphencyclidine.

Author

Mitchell-Mata C, Thomas B, Peterson B, and Couper F

Subjects

Drug Overdose mortality, Humans, Illicit Drugs, Phencyclidine blood, Phencyclidine poisoning, Psychotropic Drugs blood, Washington, Drug Overdose diagnosis, Phencyclidine analogs & derivatives, Psychotropic Drugs poisoning, Substance Abuse Detection methods

Abstract

3- and 4-methoxyphencyclidine (3-MeO-PCP, 4-MeO-PCP), structural analogs of phencyclidine (PCP), were among the first legal PCP alternatives to show up on the novel psychoactive substances (NPS) market in Europe in the 2000s. Their structural similarities to PCP and ketamine likely contribute to their demonstrated dissociative anesthetic effects. Limited information exists in the literature about toxic and lethal concentrations of these drugs in biological samples. This case report presents the first two death cases in Washington State in which 3-MeO-PCP was identified. Alkaline drug screen analysis by gas chromatography-mass spectrometry (GC-MS) revealed a peak with a retention time similar to PCP and base peak of m/z 230. Certified reference materials for 3-and 4-MeO-PCP were obtained and the isomers were able to be distinguished based on different retention times and mass spectra. A quantitative GC-MS method was developed and validated for casework, utilizing a dynamic range of 10-1,000 ng/mL and a limit of detection of 1 ng/mL. Postmortem (peripheral/central) blood samples were analyzed using this method and the resulting concentrations were 0.63 and 3.2 mg/L of 3-MeO-PCP. Methamphetamine (0.11 mg/L) was additionally detected in the blood of one of the decedents; while the second decedent was additionally positive for ethanol (0.047 g/100 mL), bupropion (1.8 mg/L), delorazepam, paroxetine and mitragynine. The results presented in this case report are higher than previously reported concentrations in fatal cases, but the presence of polysubstance abuse is consistent with previously reported NPS intoxications. Both of these individuals were in drug rehabilitation facilities prior to their deaths; however, users continue to be drawn to 3-MeO-PCP due to its dissociative effects and its accessibility on the internet., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2017

16. A non-fatal intoxication and seven deaths involving the dissociative drug 3-MeO-PCP.

Author

Johansson A, Lindstedt D, Roman M, Thelander G, Nielsen EI, Lennborn U, Sandler H, Rubertsson S, Ahlner J, Kronstrand R, and Kugelberg FC

Subjects

Adult, Akathisia, Drug-Induced, Catatonia chemically induced, Chromatography, Liquid, Designer Drugs analysis, Female, Half-Life, Hallucinogens analysis, Humans, Hypertension chemically induced, Male, Phencyclidine adverse effects, Phencyclidine analysis, Phencyclidine poisoning, Substance-Related Disorders diagnosis, Tachycardia chemically induced, Tachypnea chemically induced, Tandem Mass Spectrometry, Young Adult, Designer Drugs adverse effects, Designer Drugs poisoning, Hallucinogens adverse effects, Hallucinogens poisoning, Phencyclidine analogs & derivatives

Abstract

Introduction: 3-methoxyphencyclidine (3-MeO-PCP) appeared on the illicit drug market in 2011 and is an analogue of phencyclidine, which exhibits anesthetic, analgesic and hallucinogenic properties. In this paper, we report data from a non-fatal intoxication and seven deaths involving 3-MeO-PCP in Sweden during the period March 2014 until June 2016., Case Descriptions: The non-fatal intoxication case, a 19-year-old male with drug problems and a medical history of depression, was found awake but tachycardic, hypertensive, tachypnoeic and catatonic at home. After being hospitalized, his condition worsened as he developed a fever and lactic acidosis concomitant with psychomotor agitation and hallucinations. After 22h of intensive care, the patient had made a complete recovery. During his hospitalization, a total of four blood samples were collected at different time points. The seven autopsy cases, six males and one female, were all in their twenties to thirties with psychiatric problems and/or an ongoing drug abuse., Methods: 3-MeO-PCP was identified with liquid chromatography (LC)/time-of-flight technology and quantified using LC-tandem mass spectrometry., Results: In the clinical case, the concentration of 3-MeO-PCP was 0.14μg/g at admission, 0.08μg/g 2.5h after admission, 0.06μg/g 5h after admission and 0.04μg/g 17h after admission. The half-life of 3-MeO-PCP was estimated to 11h. In the autopsy cases, femoral blood concentrations ranged from 0.05μg/g to 0.38μg/g. 3-MeO-PCP was the sole finding in the case with the highest concentration and the cause of death was established as intoxication with 3-MeO-PCP. In the remaining six autopsy cases, other medications and drugs of abuse were present as well., Conclusion: Despite being scheduled in January 2015, 3-MeO-PCP continues to be abused in Sweden. Exposure to 3-MeO-PCP may cause severe adverse events and even death, especially if the user does not receive life-supporting treatment., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

17. A Case of Unusual Drug Screening Results.

Author

Chang BN and Smith MP

Subjects

Adult, Creatine Kinase blood, Delirium chemically induced, Delirium diagnosis, Delirium urine, Designer Drugs analysis, Excitatory Amino Acid Antagonists urine, Gas Chromatography-Mass Spectrometry, Hallucinogens urine, Humans, Male, Phencyclidine poisoning, Phencyclidine urine, Phencyclidine Abuse blood, Phencyclidine Abuse physiopathology, Receptors, N-Methyl-D-Aspartate antagonists & inhibitors, Troponin I blood, Designer Drugs poisoning, Excitatory Amino Acid Antagonists poisoning, Hallucinogens poisoning, Phencyclidine analogs & derivatives, Phencyclidine Abuse diagnosis, Phencyclidine Abuse urine, Substance Abuse Detection

Published

2017

18. 3-MeO-PCP intoxication in two young men: First in vivo detection in Italy.

Author

Bertol E, Pascali J, Palumbo D, Catalani V, Di Milia MG, Fioravanti A, Mari F, and Vaiano F

Subjects

Acidosis, Respiratory chemically induced, Anisocoria chemically induced, Blood Alcohol Content, Chromatography, Liquid, Coma chemically induced, Delirium chemically induced, Designer Drugs analysis, Gas Chromatography-Mass Spectrometry, Hallucinogens analysis, Humans, Hypothermia chemically induced, Italy, Male, Mydriasis chemically induced, Phencyclidine adverse effects, Phencyclidine analysis, Tandem Mass Spectrometry, Young Adult, Designer Drugs adverse effects, Hallucinogens adverse effects, Phencyclidine analogs & derivatives

Abstract

3-MeO-PCP or 3-methoxyphencyclidine is a derivative of phencyclidine. It acts as a dissociative anesthetic and it has allegedly hallucinogenic and sedative effects. There are almost no documented intoxication cases and references about its pharmacology and toxicity in literature. This study presents two concomitant intoxication cases due to consumption of 3-MeO-PCP and alcohol. A 19 (A) and a 21 years old (B) men were brought to Santa Maria Nuova Hospital in a comatose state (Glasgow score 3). They showed respiratory acidosis, right anisocoria with mydriatic pupils and hypothermia. Toxicological screening was negative. They were intubated for 7-8h. Almost 24h after hospitalization they were still in a delirious and agitated status. The subjects declared a high alcohol consumption and ingestion of unknown pills. Blood and urine were collected upon their arrival to the Emergency Department and sent to our Forensic Toxicology Division. Blood alcohol content was 2.0g/L for subject A and 1,7g/L for subject B. The specimens were analyzed by means of GC-MS, revealing the presence of 3-MeO-PCP. A confirmation and quantification was carried out by means of a new and fully validated liquid chromatography-tandem mass spectrometry (LC-MS/MS) method for new psychoactive substances (NPS) detection. The analysis was performed adding acetonitrile to the samples, the supernatant was dried and reconstituted with methanol. Mephedrone-D3 was used as internal standard. Acquisition was performed through multiple reaction monitoring (MRM) dynamic mode. The MRM transitions used for quantification of 3-MeO-PCP were: m/z 274→86, 121. 3-MeO-PCP was quantified in all the biological samples at the following concentrations: 350.0 (blood) and 6109.2 (urine) ng/mL for A; 180.1 (blood) and 3003.6 (urine) ng/mL for B. Taking into account the analytical results, we can suppose that the manifested symptoms were due to the consumption of 3-MeO-PCP in synergy with alcohol. Our report is the first case of 3-MeO-PCP intoxication in Italy and one of the few documented all over the world. For this reason, this case represents a significant worrisome alarm about the spread of this substance. Here we want to highlight the importance of having an effective and broad-spectrum analytical method in order to face the NPS issue., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2017

19. Two Cases of Non-fatal Intoxication with a Novel Street Hallucinogen: 3-Methoxy-Phencyclidine.

Author

Zidkova M, Hlozek T, Balik M, Kopecky O, Tesinsky P, Svanda J, and Balikova MA

Subjects

Chromatography, Liquid, Europe, Hallucinogens urine, Humans, Illicit Drugs urine, Phencyclidine toxicity, Phencyclidine urine, Substance Abuse Detection, Hallucinogens toxicity, Illicit Drugs toxicity, Phencyclidine analogs & derivatives

Abstract

3-Methoxy-phencyclidine (3-MeO-PCP) is a structural derivative of the dissociative hallucinogen phencyclidine (PCP). Although PCP toxicity is well documented, little is known about this new psychoactive substance despite being available on the black market even in central Europe. The objective of this case report is to present clinical and laboratory data of analytically confirmed non-fatal intoxication of two subjects with 3-MeO-PCP. A preliminary assessment of potential metabolites excreted into urine was enabled using the liquid chromatography high resolution mass spectrometric method., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2017

20. New Psychoactive Substances 3-Methoxyphencyclidine (3-MeO-PCP) and 3-Methoxyrolicyclidine (3-MeO-PCPy): Metabolic Fate Elucidated with Rat Urine and Human Liver Preparations and their Detectability in Urine by GC-MS, "LC-(High Resolution)-MSn" and "LC-(High Resolution)-MS/MS".

Author

A Michely JA, Manier SK, Caspar AT, Brandt SD, Wallach J, and Maurer HH

Subjects

Animals, Cytochrome P-450 Enzyme System metabolism, Female, Humans, Liver chemistry, Male, Metabolic Networks and Pathways drug effects, Metabolic Networks and Pathways physiology, Microsomes, Liver physiology, Phencyclidine metabolism, Phencyclidine urine, Psychotropic Drugs metabolism, Psychotropic Drugs urine, Rats, Rats, Wistar, Time Factors, Chromatography, Liquid, Gas Chromatography-Mass Spectrometry, Liver metabolism, Phencyclidine analogs & derivatives, Urine chemistry

Abstract

Background: 3-Methoxyphencyclidine (3-MeO-PCP) and 3-methoxyrolicyclidine (3-MeOPCPy) are two new psychoactive substances (NPS). The aims of the present study were the elucidation of their metabolic fate in rat and pooled human liver microsomes (pHLM), the identification of the cytochrome P450 (CYP) isoenzymes involved, and the detectability using standard urine screening approaches (SUSA) after intake of common users' doses using gas chromatography-mass spectrometry (GC-MS), liquid chromatography-multi-stage mass spectrometry (LC-MSn), and liquid chromatography-high-resolution tandem mass spectrometry (LC-HR-MS/MS)., Methods: For metabolism studies, rat urine samples were treated by solid phase extraction or simple precipitation with or without previous enzymatic conjugate cleavage. After analyses via LC-HR-MSn, the phase I and II metabolites were identified., Results: Both drugs showed multiple aliphatic hydroxylations at the cyclohexyl ring and the heterocyclic ring, single aromatic hydroxylation, carboxylation after ring opening, O-demethylation, and glucuronidation. The transferability from rat to human was investigated by pHLM incubations, where Odemethylation and hydroxylation were observed. The involvement of the individual CYP enzymes in the initial metabolic steps was investigated after single CYP incubations. For 3-MeO-PCP, CYP 2B6 was responsible for aliphatic hydroxylations and CYP 2C19 and CYP 2D6 for O-demethylation. For 3-MeO-PCPy, aliphatic hydroxylation was again catalyzed by CYP 2B6 and O-demethylation by CYP 2C9 and CYP 2D6 Conclusions: As only polymorphically expressed enzymes were involved, pharmacogenomic variations might occur, but clinical data are needed to confirm the relevance. The detectability studies showed that the authors' SUSAs were suitable for monitoring the intake of both drugs using the identified metabolites., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2017

21. Development of a Specific Substrate-Inhibitor Panel (Liver-on-a-Chip) for Evaluation of Cytochrome P450 Activity.

Author

Zakhariants AA, Burmistrova OA, Shkurnikov MY, Poloznikov AA, and Sakharov DA

Subjects

Bupropion metabolism, Chromatography, High Pressure Liquid, Cytochrome P-450 CYP2B6 analysis, Cytochrome P-450 CYP2C19 analysis, Cytochrome P-450 CYP2C9 analysis, Cytochrome P-450 CYP3A analysis, Cytochrome P-450 Enzyme Inhibitors pharmacology, Humans, Ketoconazole pharmacology, Liver drug effects, Liver enzymology, Mass Spectrometry, Mephenytoin analogs & derivatives, Mephenytoin pharmacology, Microsomes, Liver drug effects, Microsomes, Liver enzymology, Omeprazole metabolism, Phencyclidine analogs & derivatives, Phencyclidine pharmacology, Substrate Specificity, Sulfaphenazole pharmacology, Testosterone metabolism, Tolbutamide metabolism, Cytochrome P-450 CYP2B6 metabolism, Cytochrome P-450 CYP2C19 metabolism, Cytochrome P-450 CYP2C9 metabolism, Cytochrome P-450 CYP3A metabolism, Lab-On-A-Chip Devices

Abstract

We developed a cytochrome P450 substrate-inhibitor panel for preclinical in vitro evaluation of drugs in a 3D histotypical microfluidic cell model of human liver (liver-on-a-chip technology). The concentrations of substrates and inhibitors were optimized to ensure reliable detection of the principal metabolites by HPLC-mass-spectroscopy. The selected specific substrate-inhibitor pairs, namely bupropion/2-phenyl-2-(1-piperidinyl)propane) for evaluation of CYP2B6B activity, tolbutamide/sulfaphenazole for CYP2C9, omeprazole/(+)-N-benzylnirvanol for CYP2C19, and testosterone/ketoconazole for CYP3A4, enable reliable evaluation of the drug metabolism pathway. In contrast to animal models characterized by species-specific expression profile and activity of cytochrome P450 isoforms, our in vitro model reflects the metabolism of human hepatocytes in vivo.

Published

2016

22. "Trip-Sitting" in the Black Hole: A Netnographic Study of Dissociation and Indigenous Harm Reduction.

Author

Hearne E and Van Hout MC

Subjects

Cyclohexanones administration & dosage, Cyclohexanones adverse effects, Cyclohexylamines administration & dosage, Cyclohexylamines adverse effects, Designer Drugs adverse effects, Designer Drugs chemistry, Harm Reduction, Humans, Illicit Drugs chemistry, Phencyclidine administration & dosage, Phencyclidine adverse effects, Phencyclidine analogs & derivatives, Piperidines administration & dosage, Piperidines adverse effects, Substance-Related Disorders prevention & control, Designer Drugs administration & dosage, Illicit Drugs adverse effects, Substance-Related Disorders epidemiology

Abstract

An array of dissociative novel psychoactive substances, including "methoxetamine," "3-MeO-PCP," and "methoxphenidine," have emerged as substitutes for the illicit substance "ketamine." A netographic research methodology aimed to describe online, dissociative novel psychoactive substance users' perceptions of risk, informed knowledge around use, and indigenous harm-reduction practices as advocated within online drug fora, so as to provide credible information which can be used to inform public online health education and drug prevention. Systematic Internet searches were performed using the terms "synthetic dissociative," "methoxetamine," "methoxphenidine," "diphenidine," "3-MeO-PCP," "4-MeO-PCP," "2-MDP," and "dissociative research chemical" in combination with "forum." Following screening of 3,476 forum threads with removal of duplicates and exclusion criteria, 90 user trip reports and 115 fora threads from seven drug fora websites were analyzed by conducting content analysis. Five themes emerged with 43 categories. The findings illustrated how forum activity within the cyber drug user community disseminated and exchanged "communal folk pharmacology" relating to the use of dissociative novel psychoactive substances. Further research and consistent monitoring of Internet drug fora are advised to explore variations in harm-reduction tactics throughout dissociative NPS populations, and to consider how existing harm-reduction initiatives are influencing these hard-to-reach groups.

Published

2016

23. Fatal Intoxication Involving 3-MeO-PCP: A Case Report and Validated Method.

Author

Bakota E, Arndt C, Romoser AA, and Wilson SK

Subjects

Adult, Drug Overdose blood, Enzyme-Linked Immunosorbent Assay, Fatal Outcome, Forensic Toxicology, Humans, Male, Phencyclidine blood, Phencyclidine poisoning, Drug Overdose diagnosis, Phencyclidine analogs & derivatives, Substance Abuse Detection methods

Abstract

We present in this case report a validated method for accurate quantitative analysis of 3-methoxy phencyclidine (3-MeO-PCP) to determine postmortem blood concentrations of this PCP analog. A 29-year-old male with a history of illicit drug use was found unresponsive in his bed with a bag of white powder next to him. Resuscitation efforts were unsuccessful and the individual was pronounced dead 9 minutes after arrival to the hospital. Initial ELISA screening suggested the presence of PCP in the decedent's blood. However, confirmatory testing revealed no detectable PCP. Instead, a large peak corresponding to a m/z 274.218 species with retention time similar to PCP was present on a LC-TOF-MS drug screen, suggesting a possible PCP analog. This mass corresponds specifically to a methoxy-PCP analog, several of which are available for purchase online. Standards for 3-MeO-PCP and 4-MeO-PCP were obtained and injected on the same instrument. Although the 3- and 4-MeO-PCP analogs have identical masses and retention times, they are still distinguishable through their mass spectra. The peak from the decedent's sample matched both the mass spectrum and the retention time of 3-MeO-PCP. A quantitative LC-MS-MS method was subsequently developed and validated for casework. Analysis using this method revealed a concentration of 139 ± 41 µg/L 3-MeO-PCP in the decedent's blood. Diphenhydramine (4.1 ± 0.7 mg/L), marijuana metabolite (presumptive positive, confirmation not performed) and a small amount of amphetamine (<0.10 mg/L) were also found in the decedent's blood. The cause of death was determined to be combined 3-MeO-PCP, diphenhydramine and amphetamine toxicity. The manner of death was certified as an accident., (© The Author 2016. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2016

24. Phencyclidine analog use in Sweden--intoxication cases involving 3-MeO-PCP and 4-MeO-PCP from the STRIDA project.

Author

Bäckberg M, Beck O, and Helander A

Subjects

Adolescent, Adult, Biomarkers blood, Biomarkers urine, Chromatography, Liquid, Drug Overdose, Female, Hospitalization, Humans, Male, Middle Aged, Phencyclidine blood, Phencyclidine urine, Phencyclidine Abuse diagnosis, Phencyclidine Abuse physiopathology, Phencyclidine Abuse therapy, Poison Control Centers, Predictive Value of Tests, Severity of Illness Index, Substance Abuse Detection methods, Sweden epidemiology, Tandem Mass Spectrometry, Time Factors, Young Adult, Phencyclidine analogs & derivatives, Phencyclidine poisoning, Phencyclidine Abuse epidemiology

Abstract

Background: 3-Methoxy-phencyclidine (3-MeO-PCP) and 4-methoxy-phencyclidine (4-MeO-PCP) are analogs of and drug substitutes for the dissociative substance PCP ("Angel dust"), a recreational drug that was most popular in the 1970s. In Sweden, use of methoxylated PCP analogs was noted starting in mid-2013, according to statistics from the Poisons Information Centre. The objective of this case series was to present clinical and bioanalytical data from analytically confirmed non-fatal intoxications associated with 3-MeO-PCP and/or 4-MeO-PCP within the STRIDA project., Study Design: Observational case series of consecutive patients with self-reported or suspected exposure to new psychoactive substances (NPS) and who require hospital care., Patients and Methods: Blood and urine samples were collected from intoxicated patients presenting at emergency departments (ED) or intensive care units (ICU) all over Sweden. NPS analysis was performed by multicomponent liquid chromatographic-tandem mass spectrometric (LC-MS/MS) and LC-high-resolution MS (LC-HRMS) methods. Data on clinical features were collected during Poisons Information Centre consultations and retrieved from medical records., Results: The Poisons Information Centre registered its first call related to methoxylated PCP analogs in July 2013, while analytically confirmed cases first appeared in October 2013. From July 2013 to March 2015, 1243 cases of suspected NPS intoxication originating from ED or ICU were enrolled in the STRIDA project. During the 21-month period, 56 (4.5%) patients tested positive for 3-MeO-PCP and 11 (0.9%) for 4-MeO-PCP; 8 of these cases involved both substances. The 59 patients were aged 14-55 (median: 26) years and 51 (86%) were men. Co-exposure to other NPSs and/or classical drugs of abuse was common with only 7 cases (12%) indicated to be 3-MeO-PCP single-substance intoxications; prominent clinical signs seen in the latter cases were hypertension (systolic blood pressure ≥ 140 mmHg; 7 cases), tachycardia (≥ 100/min; 5 cases), and altered mental status (4 cases) including confusion, disorientation, dissociation, and/or hallucinations. Mixed-drug users displayed not only the same clinical features, but also more sympathomimetic effects including agitation (38%) and dilated pupils (33%). Patients testing positive for 3-/4-MeO-PCP were typically under medical care for 1-2 days (85%), and 37% of all cases were graded as severe intoxications (Poisoning Severity Score 3). Besides standard supportive therapy, 49% of the patients were treated with benzodiazepines and/or propofol., Conclusion: Laboratory analysis constitutes an important basis for the assessment of NPS hazard and availability. The adverse effects noted in cases of acute intoxications involving 3- and/or 4-MeO-PCP resembled those of other dissociatives such as PCP, ketamine, and methoxetamine. However, similar to intoxications involving other NPS, poly-substance use was found to be common.

Published

2015

25. The evolving high: new designer drugs of abuse.

Author

Pourmand A, Armstrong P, Mazer-Amirshahi M, and Shokoohi H

Subjects

Amphetamine-Related Disorders diagnosis, Amphetamine-Related Disorders therapy, Amphetamines chemical synthesis, Analgesics, Opioid chemical synthesis, Animals, Designer Drugs chemical synthesis, Humans, Opioid-Related Disorders diagnosis, Opioid-Related Disorders therapy, Phencyclidine analogs & derivatives, Phencyclidine chemical synthesis, Phencyclidine Abuse diagnosis, Phencyclidine Abuse therapy, Poisoning epidemiology, Poisoning therapy, Risk Factors, Amphetamine-Related Disorders epidemiology, Amphetamines poisoning, Analgesics, Opioid poisoning, Designer Drugs poisoning, Opioid-Related Disorders epidemiology, Phencyclidine poisoning, Phencyclidine Abuse epidemiology

Abstract

Over the past decade, emerging drugs of abuse and synthetic derivatives of more traditional agents have flooded the market. While Europe was the first to experience a surge in the use of drugs such as synthetic cathinones and cannabinoids, poison centers throughout the United States have seen a dramatic rise in calls related to these new designer drugs of abuse. In the majority of cases, care is largely supportive but significant medical and traumatic complications may occur. Providers must be aware of the ever-changing trends in abuse, so that they may optimally care for poisoned patients., (© The Author(s) 2014.)

Published

2014

26. Preparation and analytical characterization of 1-(1-phenylcyclohexyl)piperidine (PCP) and 1-(1-phenylcyclohexyl)pyrrolidine (PCPy) analogues.

Author

Wallach J, De Paoli G, Adejare A, and Brandt SD

Subjects

Chromatography, Gas, Illicit Drugs chemical synthesis, Magnetic Resonance Spectroscopy, Mass Spectrometry, Phencyclidine chemical synthesis, Psychotropic Drugs chemical synthesis, Substance Abuse Detection, Illicit Drugs analysis, Phencyclidine analogs & derivatives, Phencyclidine analysis, Psychotropic Drugs analysis

Abstract

Classic examples of psychoactive arylcycloalkylamines include ketamine and 1-(1-phenylcyclohexyl)piperidine (PCP) and many others serve as important structural templates for neuropharmacological research. The recent emergence of PCP analogues that can be obtained from internet retailers requires the implementation of appropriate monitoring strategies for harm reduction purposes. Access to analytical data plays a key part when encountering these substances, especially if reference material is not available. The present study describes the synthesis of three substituted 1-(1-phenylcyclohexyl)piperidines, (3-MeO-, 4-MeO- and 3-Me-PCP) and three substituted 1-(1-phenylcyclohexyl)pyrrolidine analogues (3-MeO-, 4-MeO- and 3-Me-PCPy). Analytical characterizations of all six arylcyclohexylamines and their primary 1-phenylcyclohexanamine intermediates included gas chromatography ion trap electron- and chemical ionization and high resolution mass spectrometry, liquid chromatography electrospray hybrid triple-quadrupole linear ion trap tandem mass spectrometry, infrared, diode array detection and (1) H and (13) C nuclear magnetic resonance (NMR) spectroscopy. Solvent (CDCl3 vs. d6 -DMSO) and protonation effects (free bases vs hydrochloride salts) were studied in order to investigate the impact on shifts and splitting patterns, for example, when attempting to assign separate axial and equatorial proton chemical shifts of NMR spectra. Differentiation between the isomeric 3-MeO-/4-MeO-PCP and PCPy analogues was feasible under mass spectral conditions. Gas chromatography analysis appeared to induce notable degradation of the 4-MeO-substituted analytes, especially when dealing with the HCl salts which led to the detection of the substituted 1-phenylcyclohex-1-ene nucleus. This phenomenon was observed to be less pronounced with the 3-MeO isomers, possibly due to the resonance properties of the para-methoxy group followed by more facile elimination of the amine., (Copyright © 2013 John Wiley & Sons, Ltd.)

Published

2014

27. Tissue factor/factor VIIa induces cell survival and gene transcription by transactivation of the insulin-like growth factor 1 receptor.

Author

Åberg M, Eriksson O, Mokhtari D, and Siegbahn A

Subjects

Apoptosis drug effects, Blood Coagulation drug effects, Blood Coagulation genetics, Cell Line, Tumor, Cell Survival, Cytoprotection drug effects, Cytoprotection genetics, Epithelial Cells drug effects, Humans, Monocytes drug effects, Phencyclidine analogs & derivatives, Phencyclidine pharmacology, Protein Binding, RNA, Small Interfering genetics, Receptor Cross-Talk, Receptor, IGF Type 1 antagonists & inhibitors, Receptor, IGF Type 1 genetics, Signal Transduction drug effects, Signal Transduction genetics, TNF-Related Apoptosis-Inducing Ligand metabolism, Transcriptional Activation drug effects, Tumor Necrosis Factor-alpha metabolism, Tyrphostins pharmacology, Epithelial Cells physiology, Factor VIIa metabolism, Monocytes physiology, Receptor, IGF Type 1 metabolism, Thromboplastin metabolism

Abstract

The insulin-like growth factor 1 receptor (IGF-1R) is known to promote survival and has also been implicated in the pathogenesis of several disease states, including cardiovascular disorders and cancer. Recently, we showed that binding of coagulation factor VIIa (FVIIa) to its receptor tissue factor (TF) protects cancer cells from TNF-related apoptosis inducing ligand (TRAIL)-induced apoptosis. Here we present evidence that this biological function of TF/FVIIa is dependent on the IGF-1R. IGF-1R inhibitors AG1024 and PPP as well as siRNA-mediated downregulation of IGF-1R, abolished the TF/FVIIa-mediated protection against TRAIL-induced apoptosis. Moreover, FVIIa rapidly induced a time- and concentration-dependent tyrosine phosphorylation of the IGF-1R in MDA-MB-231 breast cancer cells and in primary human monocytes, an event that was accompanied by IGF-1R chromatin binding and gene transcription. We hereby present novel evidence of a cross-talk between the coagulation and IGF-1R signalling systems, and propose that the IGF-1R is a key player in mediating TF/FVIIa-induced cell survival.

Published

2014

28. Paliperidone for the treatment of ketamine-induced psychosis: a case report.

Author

Zuccoli ML, Muscella A, Fucile C, Carrozzino R, Mattioli F, Martelli A, and Orengo S

Subjects

Adult, Anesthetics, Dissociative adverse effects, Anesthetics, Dissociative pharmacology, Antipsychotic Agents administration & dosage, Hospitalization, Humans, Male, Paliperidone Palmitate, Psychiatric Status Rating Scales, Treatment Outcome, Isoxazoles administration & dosage, Ketamine adverse effects, Ketamine pharmacology, Phencyclidine analogs & derivatives, Phencyclidine Abuse complications, Phencyclidine Abuse diagnosis, Phencyclidine Abuse psychology, Phencyclidine Abuse therapy, Psychoses, Substance-Induced diagnosis, Psychoses, Substance-Induced etiology, Psychoses, Substance-Induced psychology, Psychoses, Substance-Induced therapy, Pyrimidines administration & dosage

Abstract

Ketamine is an anaesthetic and analgesic drug synthesized in the 1960s from phencyclidine. The recreational use of ketamine increased among the dance culture of techno and house music, in particular in clubs, discotheques, and rave parties. The psychotropic effects of ketamine are now well known and they range from dissociation to positive, negative, and cognitive schizophrenia-like symptoms. We report a case of a chronic oral consumption of ketamine which induced agitation, behavioral abnormalities, and loss of contact with reality in a poly-drug abuser; these symptoms persisted more than two weeks after the drug consumption had stopped. Antipsychotic treatment with paliperidone led to a successful management of the psychosis, getting a complete resolution of the clinical picture. Paliperidone has proven to be very effective in the treatment of ketamine-induced disorders. Moreover, the pharmacological action and metabolism of paliperidone are poorly dependent from the activity of liver enzymes, so that it seems to be one of the best second generation antipsychotics for the treatment of smokers and alcohol abusers.

Published

2014

29. Synthesis and pain perception of new analogues of phencyclidine in NMRI male mice.

Author

Ahmadi A, Khalili M, Marami S, Ghadiri A, and Nahri-Niknafs B

Subjects

Analgesics chemistry, Animals, Male, Mice, Phencyclidine chemical synthesis, Phencyclidine chemistry, Analgesics chemical synthesis, Analgesics therapeutic use, Pain drug therapy, Phencyclidine analogs & derivatives, Phencyclidine therapeutic use

Abstract

Phencyclidine (PCP, I) and many of its derivatives have demonstrated many pharmacological effects. They interact with a number of neurotransmitter systems within the central nervous system. For example, Phencyclidine is a noncompetitive antagonist of the N-methyl-d-aspartate (NMDA) subtype of the glutamate receptor, and it causes the release and inhibits the reuptake of monoaminergic neurotransmitters, including dopamine, serotonin and norepinephrine. In this study, new thienyl (TCP, II), as well as benzothiophen (BTCP, III) derivatives (IV-VII) were synthesized. The acute and chronic pain activities of these drugs were studied using the tail immersion and formalin tests on mice and the results were compared with PCP, TCP and control groups at dosage of 10 mg/kg. The results indicated that the drug VII produced more analgesic effects on acute chemical pain in formalin test compared with other drugs. In addition, this analgesic effect was remarkably seen for drugs II, VI and VII in chronic pain in the mentioned test in comparison with other drugs. Also, the results showed that acute thermal pain could be diminished by drugs VI, II and I compared with other drugs in tail immersion test. It can be concluded that more analgesic effects of new BTCP analogues (VI and VII) may be concerned with antinociception activities of benzothiophene group and also with binding to cocaine site on the dopamine transporter receptor which seems to be more potent than PCP receptor in decreasing pain.

Published

2014

30. Is methoxydine a new rapid acting antidepressant for the treatment of depression in alcoholics?

Author

Coppola M and Mondola R

Subjects

Depression complications, Humans, Models, Theoretical, Phencyclidine therapeutic use, Alcoholism complications, Antidepressive Agents therapeutic use, Depression drug therapy, Phencyclidine analogs & derivatives

Abstract

Methoxydine is a dissociative anaesthetic belonging to the arylcyclohexylamine class. This substance shows pharmacodynamic similarities with ketamine, a medication with demonstrated rapid-acting antidepressant effects. Like ketamine, results of binding assays have shown that methoxydine is an uncompetitive antagonist of NMDA receptor approximately as potent as ketamine, but less potent than PCP. Furthermore, unlike ketamine, it acts as a dopamine, serotonin, and noradrenaline reuptake inhibitor as well as an agonist at sigma-1, sigma-2, and opioid receptors. The hypothesis is that methoxydine can produce rapid antidepressant effects in depressed patients with high risk of suicide, including depressed alcoholics., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

31. Telomerase inhibitors from cyanobacteria: isolation and synthesis of sulfoquinovosyl diacylglycerols from Microcystis aeruguinosa PCC 7806.

Author

Makhlouf Brahmi M, Portmann C, D'Ambrosio D, Woods TM, Banfi D, Reichenbach P, Da Silva L, Baudat E, Turcatti G, Lingner J, and Gademann K

Subjects

Diglycerides chemistry, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Glycolipids chemistry, Phencyclidine analogs & derivatives, Structure-Activity Relationship, Tandem Mass Spectrometry, Telomerase metabolism, Diglycerides chemical synthesis, Glycolipids chemical synthesis, Microcystis metabolism, Telomerase antagonists & inhibitors

Abstract

By using the Telospot assay, 27 different extracts of cyanobacteria were evaluated for telomerase inhibition. All extracts showed varying, but significant activity. We selected Microcystis aeruguinosa PCC 7806 to identify the active compound and a bioassay guided fractionation led us to isolate mixtures of sulfoquinovosyl diacylglycerols (SQDGs), which were identified by 2D NMR and MS/MS experiments. Pure SQDG derivatives were then synthesized. The IC(50) values of pure synthetic sulfoquinovosyl dipalmitoylglycerol and the monopalmitoylated derivative against telomerase were determined to be 17 and 40 μM, respectively. A structure-activity relationship study allowed the identification of compounds with modified lipophilic acyl groups that display improved activity., (Copyright © 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2013

32. The ketamine analogue methoxetamine and 3- and 4-methoxy analogues of phencyclidine are high affinity and selective ligands for the glutamate NMDA receptor.

Author

Roth BL, Gibbons S, Arunotayanun W, Huang XP, Setola V, Treble R, and Iversen L

Subjects

Drug Evaluation, Preclinical methods, Humans, Ketamine chemistry, Ketamine metabolism, Ketamine pharmacology, Molecular Structure, National Institute of Mental Health (U.S.), Phencyclidine chemistry, Phencyclidine metabolism, Phencyclidine pharmacology, Radioligand Assay, Receptors, sigma metabolism, Serotonin Plasma Membrane Transport Proteins metabolism, United States, Cyclohexanones metabolism, Cyclohexylamines metabolism, Ketamine analogs & derivatives, Phencyclidine analogs & derivatives, Receptors, N-Methyl-D-Aspartate metabolism

Abstract

In this paper we determined the pharmacological profiles of novel ketamine and phencyclidine analogues currently used as 'designer drugs' and compared them to the parent substances via the resources of the National Institute of Mental Health Psychoactive Drug Screening Program. The ketamine analogues methoxetamine ((RS)-2-(ethylamino)-2-(3-methoxyphenyl)cyclohexanone) and 3-MeO-PCE (N-ethyl-1-(3-methoxyphenyl)cyclohexanamine) and the 3- and 4-methoxy analogues of phencyclidine, (1-[1-(3-methoxyphenyl)cyclohexyl]piperidine and 1-[1-(4-methoxyphenyl)cyclohexyl]piperidine), were all high affinity ligands for the PCP-site on the glutamate NMDA receptor. In addition methoxetamine and PCP and its analogues displayed appreciable affinities for the serotonin transporter, whilst the PCP analogues exhibited high affinities for sigma receptors. Antagonism of the NMDA receptor is thought to be the key pharmacological feature underlying the actions of dissociative anaesthetics. The novel ketamine and PCP analogues had significant affinities for the NMDA receptor in radioligand binding assays, which may explain their psychotomimetic effects in human users. Additional actions on other targets could be important for delineating side-effects.

Published

2013

33. Effect of phencyclidine derivatives on anxiety-like behavior using an elevated-plus maze test in mice.

Author

Hajikhani R, Ahmadi A, Naderi N, Yaghoobi K, Shirazizand Z, Rezaee NM, and Niknafs BN

Subjects

Animals, Anti-Anxiety Agents administration & dosage, Anti-Anxiety Agents chemistry, Anxiety psychology, Disease Models, Animal, Hydrophobic and Hydrophilic Interactions, Injections, Intraperitoneal, Male, Mice, Molecular Structure, Motor Activity drug effects, Phencyclidine administration & dosage, Phencyclidine analogs & derivatives, Phencyclidine chemistry, Structure-Activity Relationship, Anti-Anxiety Agents pharmacology, Anxiety drug therapy, Behavior, Animal drug effects, Maze Learning drug effects, Phencyclidine pharmacology

Abstract

Objectives: The study attempted to investigate the anti-anxiety activities of Phencyclidine (1-(1-phenylcyclohexyl) piperidine, PCP, I) and some of its derivatives (M, F, L, B, S, P) with the elevated-plus maze (EPM) Test., Material and Methods: Phencyclidine and its derivatives (M, F, L, B, S, P) were administrated intraperitoneally (i.p.) at a dose of 10 mg/kg to male mice. Anxiety-like behaviors were assessed using the elevated-plus maze test., Results: EPM results revealed an increase in open arms time spent after applying PCP and M, L, P, and B compounds at the administered dosage. Moreover, an increase in the number of open arm entries was observed with M, P, and B compounds. The P, B and S compounds increased the locomotion of animals, too, which might be considered as the side effect to the compounds., Conclusions: Considering the elevated-plus maze results, it was concluded that M and L compounds could be considered as a potential anxiolytic with less side effects due to a probable high electron donation of the methoxy group, as well as the hydrophilic properties of hydroxyl groups on these compounds.

Published

2012

34. Designer drugs: a medicinal chemistry perspective.

Author

Carroll FI, Lewin AH, Mascarella SW, Seltzman HH, and Reddy PA

Subjects

Amphetamines chemistry, Amphetamines pharmacology, Analgesics, Opioid chemistry, Analgesics, Opioid pharmacology, Animals, Cannabinoids chemistry, Cannabinoids pharmacology, Chemistry, Pharmaceutical ethics, Designer Drugs pharmacology, Drug and Narcotic Control legislation & jurisprudence, Humans, Illicit Drugs legislation & jurisprudence, Illicit Drugs pharmacology, Phencyclidine analogs & derivatives, Phencyclidine chemistry, Phencyclidine pharmacology, Scientific Misconduct, United States, Designer Drugs chemistry, Drug Design, Illicit Drugs chemistry

Abstract

There are numerous medicinal chemistry reports in the literature describing the pharmacological properties of thousands of narcotics, stimulants, hallucinogens, sedative-hypnotic drugs, cannabinoids, and other psychoactive substances as well as synthetic methods for their preparations. This information, while essential for the advancement of science, has been used by clandestine chemists to manufacture and market an endless variety of analogs of so-called designer drugs. In this review, we describe how clandestine chemists used the principles of medicinal chemistry to design molecules, referred to as designer drugs, that elicit the effects of opioids, amphetamine and analogs, cannabinoids, and phencyclidine analogs while circumventing the law., (© 2012 New York Academy of Sciences.)

Published

2012

35. Out with the old, in with the new? Case reports of the clinical features and acute management of two novel designer drugs.

Author

Misselbrook GP and Hamilton EJ

Subjects

Adult, Drug Overdose etiology, Drug Overdose therapy, Emergency Service, Hospital, Emergency Treatment methods, Follow-Up Studies, Humans, Incidence, Male, Middle Aged, Neurotoxicity Syndromes therapy, Phencyclidine poisoning, Risk Assessment, Substance-Related Disorders therapy, Treatment Outcome, Cyclohexanones poisoning, Cyclohexylamines poisoning, Designer Drugs poisoning, Illicit Drugs poisoning, Neurotoxicity Syndromes etiology, Phencyclidine analogs & derivatives, Substance-Related Disorders complications

Abstract

Methoxydine (4-MeO-PCP) and Methoxetamine (3-MeO-2-Oxo-PCE) are both commercially produced designer drugs with structural and biochemical similarities to phencyclidine (PCP). Although phencyclidine toxicity is well documented, its recreational use in present times is rare. With the advent of new designer drugs being available widely through internet sites, Acute Physicians should be aware of the clinical features and management of these potential toxins. We present a case of methoxydine ingestion (which to our knowledge has not been previously documented in any medical journals) and a case of methoxetamine ingestion, and discuss their history, contrasting clinical features and acute management.

Published

2012

36. Synthesis and antinociceptive behaviors of new methyl and hydroxyl derivatives of phencyclidine.

Author

Ahmadi A, Kermani M, Naderi N, Hajikhani R, Rezaee NM, Javadi M, and Niknafs BN

Subjects

Analgesics chemistry, Animals, Pain Measurement, Phencyclidine analogs & derivatives, Phencyclidine chemical synthesis, Structure-Activity Relationship, Analgesics chemical synthesis, Phencyclidine pharmacology, Visceral Pain drug therapy

Abstract

Phencyclidine (I) and its derivatives show such pharmacological behaviors as analgesic, anticonsulvant, anti-anxiety and antidepressant, while interacting with central nervous system. In this study, new methyl and hydroxyl derivatives of PCP were synthesized and their antinociceptive behaviors in animals were examined by measuring the number of writhing in a writhing test of visceral pain and the pain scores in Formalin test. Compared to control and PCP groups, findings in experimental groups indicated the new synthesized analogues (compounds II, III and V, 10 mg/kg) of PCP were able to produce more analgesic effects in formalin and writhing tests, especially for compound V. It was concluded that the new synthesized derivatives of PCP could substantially and respectively diminish acute and chronic pains.

Published

2012

37. Afobazole modulates neuronal response to ischemia and acidosis via activation of sigma-1 receptors.

Author

Cuevas J, Behensky A, Deng W, and Katnik C

Subjects

Acidosis pathology, Animals, Brain Ischemia pathology, Calcium metabolism, Cell Survival drug effects, Cerebral Cortex cytology, Cerebral Cortex drug effects, Ethylenediamines pharmacology, Female, Guanidines pharmacology, Indicators and Reagents, L-Lactate Dehydrogenase metabolism, Membrane Potentials drug effects, Narcotics pharmacology, Neurons pathology, Patch-Clamp Techniques, Pentazocine pharmacology, Phencyclidine analogs & derivatives, Phencyclidine pharmacology, Piperazines pharmacology, Pregnancy, Rats, Receptors, sigma antagonists & inhibitors, Sigma-1 Receptor, Acidosis metabolism, Anti-Anxiety Agents pharmacology, Benzimidazoles pharmacology, Brain Ischemia metabolism, Morpholines pharmacology, Neurons metabolism, Receptors, sigma agonists

Abstract

Afobazole is an anxiolytic medication that has been previously shown to be neuroprotective both in vitro and in vivo. However, the mechanism(s) by which afobazole can enhance neuronal survival remain poorly understood. Experiments were carried out to determine whether afobazole can decrease intracellular calcium overload associated with ischemia and acidosis and whether the effects of afobazole are mediated via interaction of the compound with σ receptors. Fluorometric Ca(2+) imaging was used to resolve how application of afobazole affects intracellular Ca(2+) handling in cortical neurons. Application of afobazole significantly depressed, in a concentration-dependent and reversible manner, the intracellular Ca(2+) overload resulting from in vitro ischemia and acidosis. The IC(50) for afobazole inhibition of ischemia-evoked intracellular Ca(2+) overload was considerably less than that for the inhibition of [Ca(2+)](i) increases induced by acidosis. However, afobazole maximally inhibited only 70% of the ischemia-evoked intracellular Ca(2+) overload but effectively abolished intracellular Ca(2+) increases produced by acidosis. The effects of afobazole on ischemia- and acidosis-induced intracellular Ca(2+) dysregulation were inhibited by preincubating the neurons in the irreversible, pan-selective σ-receptor antagonist, metaphit. Moreover, the effects of afobazole on intracellular Ca(2+) increases triggered by acidosis and ischemia were blocked by the selective σ-1-receptor antagonists, BD 1063 and BD 1047, respectively. Experiments examining the effects of afobazole on neuronal survival in response to ischemia showed that afobazole was neuroprotective. Taken together, these data suggest that afobazole regulates intracellular Ca(2+) overload during ischemia and acidosis via activation of σ-1 receptors. This mechanism is probably responsible for afobazole-mediated neuroprotection.

Published

2011

38. Novel analogues of ketamine and phencyclidine as NMDA receptor antagonists.

Author

Zarantonello P, Bettini E, Paio A, Simoncelli C, Terreni S, and Cardullo F

Subjects

Ketamine analogs & derivatives, Phencyclidine analogs & derivatives, Ketamine pharmacology, Phencyclidine pharmacology, Receptors, N-Methyl-D-Aspartate antagonists & inhibitors

Abstract

The identification of structurally novel analogues of ketamine and phencyclidine (PCP), as NMDA receptor antagonists, with low to moderate potency at GluN2A and GluN2B receptors is discussed. In particular, some examples, such as compounds 6 and 10, shows decreased calculated lipophilicity, when compared to PCP, while retaining moderate activity. Moreover, the germinal aryl amino substituted lactam ring, as exemplified in compounds 7-10 and 11-13, constitutes a novel scaffold with potential application in the design of biologically active compounds., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

39. New morpholine analogues of phencyclidine: chemical synthesis and pain perception in rats.

Author

Ahmadi A, Khalili M, Hajikhani R, and Naserbakht M

Subjects

Analgesics chemical synthesis, Analgesics chemistry, Analgesics pharmacology, Animals, Female, Models, Animal, Pain Measurement, Phencyclidine chemical synthesis, Phencyclidine pharmacology, Rats, Structure-Activity Relationship, Pain Perception drug effects, Phencyclidine analogs & derivatives

Abstract

Phencyclidine (PCP, I) and most its derivatives have demonstrated some pharmacological effects. Accordingly, in this study, the new methoxy (III) and hydroxy-methyl (IV) morpholine PCP derivatives were synthesized. The acute and chronic pain activities of these drugs (III, IV) were investigated by tail immersion and formalin tests on rats and the results were compared with those in PCP, PCM (PCP-morpholine, II), and methyl-PCM (V). Findings indicated that III (6 mg/kg, i.p.) generates more analgesic effects in tail immersion test in comparison with I and II in 20, 40, 45 and 55 min post-injection. These effects were observed in 10, 20, 40, 45 and 50 min after the application of IV (at the same dosage). This analgesic effect was markedly seen in 20, 40, 45 and 50 min after compound IV's application in comparison with the drugs (I-V). In formalin test analysis, the acute chemical pain (Phase I) could not be affected by any drugs (I-V) while chronic formalin pain would be diminished by these new synthesized drugs (III and IV), especially in late Phase II, compared to I and II at the dosage of 6 mg/kg. It is, therefore, concluded that these new synthesized PCP derivates including methoxy-PCM (III) and hydroxy-methyl-PCM (IV) could substantially and respectively diminish acute thermal and chronic chemical pains., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2011

40. Synthesis and analgesic effects of new pyrrole derivatives of phencyclidine in mice.

Author

Ahmadi A, Solati J, Hajikhani R, and Pakzad S

Subjects

Analgesics toxicity, Animals, Chronic Disease, Dimethyl Sulfoxide, Formaldehyde, Hot Temperature, Indicators and Reagents, Methylation, Mice, Pain Measurement drug effects, Phencyclidine chemical synthesis, Pyrroles toxicity, Structure-Activity Relationship, Analgesics chemical synthesis, Analgesics pharmacology, Phencyclidine analogs & derivatives, Phencyclidine pharmacology, Pyrroles chemical synthesis, Pyrroles pharmacology

Abstract

Phencyclidine (1-(1-phenylcyclohexyl)piperidine, CAS 956-90-1, PCP, I) and many of its analogues have shown some pharmacological effects. In this study, new pyrrole derivatives of I (1-(1-phenylcyclohexyl)pyrrole, II and 1-[1-(4-methylphenyl)(cyclohexyl)]pyrrole, III) and their intermediates were synthesized and the acute and chronic pains were examined on mice using tail immersion (as a model of acute thermal pain) and formalin (as a model of acute and chronic chemical pain) tests and the results were compared with the PCP and control groups. The results indicated that III generated higher analgesic effects in the tail immersion test compared to the PCP and control (dimethyl sulfoxide, DMSO) groups, demonstrating a marked and significant increase in tail immersion latency, but this effect was not observed for II in the dose of 1 mg/kg. The formalin test showed that III was effective in acute chemical pain (phase I, 0-5 min after injection), but was not effective for II at the same dosage compared to the PCP and control groups. Also chronic pain will be significantly attenuated by III but II was not effective as compared to the other groups. It is concluded that substitution of the aromatic pyrrole ring instead of piperidine in the PCP molecule will not be effective alone in tail immersion and formalin tests but the addition of a methyl group (with high electron donating and dipole moments) on the phenyl group plus substitution of the aromatic pyrrole ring can be effective in acute and chronic pain compared to the PCP and control groups.

Published

2011

41. Synthesis and determination of acute and chronic pain activities of 1-[1-(4-methylphenyl) (cyclohexyl)] morpholine as a new phencyclidine derivative in rats.

Author

Ahmadi A, Khalili M, Hajikhani R, and Naserbakht M

Subjects

Acute Disease, Analgesics, Non-Narcotic chemical synthesis, Animals, Chronic Disease, Excitatory Amino Acid Antagonists chemical synthesis, Female, Formaldehyde, Immersion, Indicators and Reagents, Pain Measurement drug effects, Phencyclidine chemical synthesis, Rats, Analgesics, Non-Narcotic pharmacology, Excitatory Amino Acid Antagonists pharmacology, Morpholines chemical synthesis, Morpholines pharmacology, Pain drug therapy, Phencyclidine analogs & derivatives, Phencyclidine pharmacology

Abstract

Phencyclidine (1-(1-phenylcyclohexyl)piperidine, CAS 77-10-1, PCP, I) and many of its analogues have been synthesized and their pharmacological properties studied. In this research, new methyl morpholine derivative of phencyclidine (1-[1-(4-methylphenyl) (cyclohexyl)]morpholine, Methyl-PCM, III) was synthesized and the acute and chronic pain activities were studied using tail immersion and formalin tests on rats and compared to PCP and PCM (1-(1-phenylcyclohexyl)morpholine, CAS 2201-40-3, PCP-morpholine, II). The results Indicated that Methyl-PCM (III, 6 mg/kg, i.p) produces more analgesic effects in tail immersion test (as a model of acute thermal pain) in comparison with the PCP, PCM and control groups. Meanwhile, this analgesic effect was markedly shown 5-15 min after the compound III application. In formalin test analysis, the acute pain (phase I) could not be affected by any drugs, but the chronic formalin pain (phase II) could be diminished by PCM and especially compound III. The chronic analgesic effect of Methyl-PCM was markedly shown in the late phase of chronic pain.

Published

2011

42. 1,2-ethane bis-1-amino-4-benzamidine is active against several brain insult and seizure challenges through anti-NMDA mechanisms targeting the 3H-TCP binding site and antioxidant action.

Author

Vamecq J, Maurois P, Pages N, Bac P, Stables JP, Gressens P, Stanicki D, and Vanden Eynde JJ

Subjects

Animals, Anticonvulsants chemistry, Anticonvulsants pharmacology, Anticonvulsants therapeutic use, Anticonvulsants toxicity, Antioxidants, Benzamidines chemical synthesis, Benzamidines therapeutic use, Benzamidines toxicity, Binding Sites drug effects, Body Temperature drug effects, Brain metabolism, Mice, Models, Molecular, Molecular Conformation, Motor Activity drug effects, N-Methylaspartate metabolism, N-Methylaspartate pharmacology, Neuroprotective Agents chemistry, Neuroprotective Agents pharmacology, Neuroprotective Agents therapeutic use, Neuroprotective Agents toxicity, Phencyclidine chemistry, Phencyclidine metabolism, Receptors, N-Methyl-D-Aspartate metabolism, Seizures chemically induced, Seizures metabolism, Seizures physiopathology, Benzamidines pharmacology, Brain drug effects, N-Methylaspartate antagonists & inhibitors, Phencyclidine analogs & derivatives, Seizures drug therapy

Abstract

Five bis-benzamidines were screened towards murine magnesium deficiency-dependent audiogenic seizures, unravelling two compounds with efficacious doses 50 (ED(50)) less than 10mg/kg. They were also screened against maximal electroshock and subcutaneous pentylenetetrazole-induced seizures, and explored for superoxide -scavenging activity. 1,2-Ethane bis-1-amino-4-benzamidine (EBAB) was selected and evaluated in 6 Hz seizure test (ED(50)=49 mg/kg) and at 4 microg/kg in focal cerebral ibotenate poisoning in pups (sizes of both white and grey matter wounds were halved). EBAB was further tested on NMDA-induced seizures in mice (ED(50)=6 mg/kg) and on (3)H-TC -binding to a rodent cerebral preparation (IC(50)=1.4 microM). Taken as a whole, present data emphasise the suitability of bis-benzamidines as templates for designing brain protective compounds., (Copyright (c) 2010 Elsevier Masson SAS. All rights reserved.)

Published

2010

43. Relationship between color and pigment production in two stone biofilm-forming cyanobacteria (Nostoc sp. PCC 9104 and Nostoc sp. PCC 9025).

Author

Sanmartín P, Aira N, Devesa-Rey R, Silva B, and Prieto B

Subjects

Biofilms, Carotenoids genetics, Chlorophyll, Chlorophyll A, Color, Nostoc genetics, Phencyclidine analogs & derivatives, Pheochromocytoma genetics, Phycocyanin genetics, Proteins genetics, Cyanobacteria genetics, Cyanobacteria metabolism, Light, Nitrogen metabolism, Nostoc metabolism

Abstract

Previous studies have provided evidence that color measurements enable on site quantification of superficial biofilms, thereby avoiding the need for sampling. In the present study, the efficiency of color measurements to evaluate to what extent pigment production is affected by environmental parameters such as light intensity, combined nitrogen and nutrient availability, was tested with two cyanobacteria, Nostoc sp. strains PCC 9104 and PCC 9025, which form biofilms on stone. Both strains were acclimated, in aerated batch cultures for 2 weeks, to three different culture media: BG-11, BG-11(0), and BG-11(0)/10 at either high or low light intensity. The content of chlorophyll a, carotenoids, and phycocyanins was measured throughout the experiment, together with variations in the color of the cyanobacteria, which were represented in the CIELAB color space. The results confirmed that the CIELAB color parameters are correlated with pigment content in such a way that variations in the latter are reflected as variations in color.

Published

2010

44. Qualitative GC-MS assessment of TCP and TAMORF elimination in rats.

Author

Petek MJ, Vrdoljak AL, and Mrsić G

Subjects

Adamantane pharmacokinetics, Adamantane urine, Animals, Male, Morpholines urine, Organophosphate Poisoning, Phencyclidine analogs & derivatives, Piperidines urine, Rats, Rats, Wistar, Thiophenes urine, Adamantane analogs & derivatives, Gas Chromatography-Mass Spectrometry, Morpholines pharmacokinetics, Piperidines pharmacokinetics, Thiophenes pharmacokinetics

Abstract

Nerve agents are highly toxic organophosphorus (OP) compounds. They inhibit acetylcholinesterase (AChE), an enzyme that hydrolyses acetycholine (ACh) in the nervous system. Pathophysiological changes caused by OP poisonings are primarily the consequence of surplus ACh on cholinergic receptors and in the central nervous system. Standard treatment of OP poisoning includes combined administration of carbamates, atropine, oximes and anticonvulsants. In order to improve therapy, new compounds have been synthesised and tested. Tenocyclidine (TCP) and its adamantane derivative 1-[2-(2-thienyl)-2-adamantyl] morpholine (TAMORF) have shown interesting properties against soman poisoning. In this study, we developed a qualitative GC-MS method to measure elimination of TCP and TAMORF through rat urine in order to learn more about the mechanisms through which TCP protects an organism from OP poisoning and to determine the duration of this protective effect. GC-MS showed that six hours after treatment with TCP, rat urine contained only its metabolite 1-thienylcyclohexene, while urine of rats treated with TAMORF contained both TAMORF and its metabolites.

Published

2010

45. Synthesis and determination of acute and chronic pain activities of 1-[1-(3-methylphenyl) (tetralyl)]piperidine as a new derivative of phencyclidine via tail immersion and formalin tests.

Author

Ahmadi A, Khalili M, Mihandoust F, and Barghi L

Subjects

Acute Disease, Analgesics chemistry, Anesthetics, Dissociative pharmacology, Animals, Chronic Disease, Female, Immersion, Ketamine pharmacology, Phencyclidine chemistry, Rats, Rats, Wistar, Analgesics chemical synthesis, Analgesics pharmacology, Formaldehyde, Pain Measurement drug effects, Phencyclidine analogs & derivatives, Phencyclidine chemical synthesis, Phencyclidine pharmacology

Abstract

Phencyclidine (1-(1-phenylcyclohexyl)piperidine, CAS 956-90-1, PCP, 1) and ketamine (2-O-chlorophenyl-2-methylaminocyclohexan, CAS 1867-66-9, II) revealed some analgesic effects. Some of their derivatives have been synthesized for biological properties studies. Utilizing 1-tetralone as a starting material, 1-[1-(3-methylphenyl)(tetralyl)]piperidine, (PCP-CH3-tetralyl, III) was synthesized and its analgesic effects were studied on rats via tail immersion (as a model of acute thermal pain) and formalin (as a model of acute chemical and chronic pain) tests and compared with those of ketamine and PCP. The results indicated a marked anti-nociception 2-25 min after ketamine injection, but this analgesic effect lasted for 40 min following PCP-CH3-tetralyl application in the tail immersion test. However, the data obtained from the formalin test showed that chronic pain could be significantly attenuated by ketamine, PCP and PCP-CH3-tetralyl.

Published

2010

46. Early candidacy for differentiation into heterocysts in the filamentous cyanobacterium Anabaena sp. PCC 7120.

Author

Toyoshima M, Sasaki NV, Fujiwara M, Ehira S, Ohmori M, and Sato N

Subjects

Amino Acid Sequence, Anabaena genetics, Anabaena metabolism, Bacterial Proteins genetics, Bacterial Proteins metabolism, Bacterial Proteins physiology, Culture Media metabolism, Fluorescence, Gene Deletion, Gene Dosage, Gene Expression Regulation, Bacterial, Gene Expression Regulation, Developmental, Gene Silencing, Genes, Bacterial, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Microscopy, Fluorescence, Models, Biological, Multigene Family, Mutation, Nitrogen metabolism, Nitrogen Fixation genetics, Phencyclidine analogs & derivatives, Phencyclidine metabolism, Promoter Regions, Genetic, Sequence Alignment, Anabaena cytology

Abstract

The filamentous cyanobacterium Anabaena sp. PCC 7120 fixes dinitrogen facultatively. Upon depletion of combined nitrogen, about 10% of vegetative cells within the filaments differentiate terminally into nitrogen-fixing cells. The heterocyst has been studied as a model system of prokaryotic cell differentiation, with major focus on signal transduction and pattern formation. The fate of heterocyst differentiation is determined at about the eighth hour of induction (point of no return), well before conspicuous morphological or metabolic changes occur. However, little is known about how the initial heterocysts are selected after the induction by nitrogen deprivation. To address this question, we followed the fate of every cells on agar plates after nitrogen deprivation with an interval of 4 h. About 10% of heterocysts were formed without prior division after the start of nitrogen deprivation. The intensity of fluorescence of GFP in the transformants of hetR-gfp increased markedly in the future heterocysts at the fourth hour with respect to other cells. We also noted that the growing filaments consisted of clusters of four consecutive cells that we call quartets. About 75% of initial heterocysts originated from either of the two outer cells of quartets at the start of nitrogen deprivation. These results suggest that the future heterocysts are loosely selected at early times after the start of nitrogen deprivation, before the commitment. Such early candidacy could be explained by different properties of the outer and inner cells of a quartet, but the molecular nature of candidacy remains to be uncovered.

Published

2010

47. Synthesis and analgesic effects of 1-[1-(2-methylphenyl)(cyclohexyl)]-3-piperidinol as a new derivative of phencyclidine in mice.

Author

Ahmadi A, Solati J, Hajikhani R, Onagh M, and Javadi M

Subjects

Acute Disease, Analgesics chemistry, Animals, Chronic Disease, Formaldehyde, Immersion physiopathology, Indicators and Reagents, Mice, Pain Measurement drug effects, Phencyclidine chemistry, Solubility, Structure-Activity Relationship, Tail, Analgesics pharmacology, Phencyclidine analogs & derivatives, Phencyclidine pharmacology

Abstract

Phencyclidine (1-(1-phenylcyclohexyl) piperidine, CAS 956-90-1, PCP, I) and its derivatives have shown many analgesic effects. In this research, a new derivative of PCP (1-[1-(2-methylphenyl) (cyclohexyl)l3-piperidinol, PD, II) was synthesized and its analgesic (acute and chronic pains) effects were examined on rats using tail immersion (as a model of acute thermal pain) and formalin (as a model of acute and chronic chemical pain) tests and the results are compared to PCP and control groups. The results indicated that II produces higher analgesic effects in the tail immersion test compared to the PCP and control groups, with a marked and significant increase in tail immersion latency for the doses 1, 5 and 10 mg/kg. The formalin test showed that PD (II) is not effective in acute chemical pain (phase I, 0-5 min after injection) in all doses but chronic pain (initial-phase II, 15-40 min after injection) is significantly attenuated by this compound compared to PCP and saline (control) in dosesof 5 and 10 mg/kg. It is concluded that II is effective in acute thermal (in all doses) and chronic (doses of 5 and 10 mg/kg) pains; however, it is not effective in acute chemical pain compared to PCP and control.

Published

2010

48. Inhibition of the histone demethylase LSD1 blocks alpha-herpesvirus lytic replication and reactivation from latency.

Author

Liang Y, Vogel JL, Narayanan A, Peng H, and Kristie TM

Subjects

Animals, Cell Line, Transformed, Chromatin Immunoprecipitation methods, DNA Replication drug effects, DNA Replication physiology, Enzyme Activation drug effects, Ganglia cytology, Gene Expression Regulation, Viral drug effects, Gene Expression Regulation, Viral physiology, Green Fluorescent Proteins genetics, Herpesvirus 3, Human physiology, Histone Demethylases genetics, Histone Methyltransferases, Histone-Lysine N-Methyltransferase, Host Cell Factor C1 metabolism, Humans, Lysine metabolism, Mice, Monoamine Oxidase Inhibitors pharmacology, Mutation genetics, Neurons drug effects, Neurons metabolism, Pargyline pharmacology, Phencyclidine analogs & derivatives, Piperidines pharmacology, Promoter Regions, Genetic drug effects, Promoter Regions, Genetic physiology, RNA, Small Interfering metabolism, RNA, Small Interfering pharmacology, Reaction Time drug effects, Simplexvirus physiology, Thiophenes pharmacology, Time Factors, Transfection methods, Virus Replication drug effects, Herpesvirus 1, Human physiology, Histone Demethylases antagonists & inhibitors, Histone Demethylases metabolism, Virus Replication physiology

Abstract

Reversible methylation of histone tails serves as either a positive signal recognized by transcriptional assemblies or a negative signal that result in repression. Invading viral pathogens that depend upon the host cell's transcriptional apparatus are also subject to the regulatory impact of chromatin assembly and modifications. Here we show that infection by the alpha-herpesviruses, herpes simplex virus (HSV) and varicella zoster virus (VZV), results in the rapid accumulation of chromatin bearing repressive histone H3 Lys9 methylation. To enable expression of viral immediate early (IE) genes, both viruses use the cellular transcriptional coactivator host cell factor-1 (HCF-1) to recruit the lysine-specific demethylase-1 (LSD1) to the viral immediate early promoters. Depletion of LSD1 or inhibition of its activity with monoamine oxidase inhibitors (MAOIs) results in the accumulation of repressive chromatin and a block to viral gene expression. As HCF-1 is a component of the Set1 and MLL1 histone H3 Lys4 methyltransferase complexes, it thus coordinates modulation of repressive H3 Lys9 methylation levels with addition of activating H3 Lys4 trimethylation marks. Strikingly, MAOIs also block the reactivation of HSV from latency in sensory neurons, indicating that the HCF-1 complex is a crucial component of the reactivation mechanism. The results support pharmaceutical control of histone modifying enzymes as a strategy for controlling herpesvirus infections.

Published

2009

49. Synthesis and evaluation of 1-(1-(Benzo[b]thiophen-2-yl)cyclohexyl)piperidine (BTCP) analogues as inhibitors of trypanothione reductase.

Author

Patterson S, Jones DC, Shanks EJ, Frearson JA, Gilbert IH, Wyatt PG, and Fairlamb AH

Subjects

Animals, Cell Line, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Humans, NADH, NADPH Oxidoreductases metabolism, Phencyclidine chemical synthesis, Phencyclidine pharmacology, Piperidines chemistry, Piperidines pharmacology, Structure-Activity Relationship, Thiophenes chemistry, Thiophenes pharmacology, Trypanocidal Agents chemistry, Trypanocidal Agents pharmacology, Trypanosoma brucei brucei drug effects, Trypanosoma brucei brucei enzymology, Enzyme Inhibitors chemical synthesis, NADH, NADPH Oxidoreductases antagonists & inhibitors, Phencyclidine analogs & derivatives, Piperidines chemical synthesis, Thiophenes chemical synthesis, Trypanocidal Agents chemical synthesis

Abstract

Thirty two analogues of phencyclidine were synthesised and tested as inhibitors of trypanothione reductase (TryR), a potential drug target in trypanosome and leishmania parasites. The lead compound BTCP (1, 1-(1-benzo[b]thiophen-2-yl-cyclohexyl) piperidine) was found to be a competitive inhibitor of the enzyme (K(i)=1 microM) and biologically active against bloodstream T. brucei (EC(50)=10 microM), but with poor selectivity against mammalian MRC5 cells (EC(50)=29 microM). Analogues with improved enzymatic and biological activity were obtained. The structure-activity relationships of this novel series are discussed.

Published

2009

50. High specific activity tritiation of TCP and BTCP.

Author

Hainley C, Hurt S, True D, and Filer CN

Subjects

Isotope Labeling methods, Phencyclidine analysis, Phencyclidine chemical synthesis, Phencyclidine analogs & derivatives, Tritium

Abstract

Methods are described to synthesize and characterize tritium labelled TCP and BTCP at high specific activity.

Published

2009