3-HO-PCE: Difference between revisions

{{Distinguish|3-HO-PCP}}

'''3-Hydroxyeticyclidine''' (commonly known as '''3-HO-PCE''') is a novel synthetic [[Psychoactive class::dissociative]] substance of the [[Chemical class::arylcyclohexylamine]] chemical class. It produces potent, dose-sensitive [[dissociative]], [[hallucinogenic]] and [[euphoric]] effects when [[Routes of administration|administered]]. Unlike its close structural analog [[3-HO-PCP]], this compound has no precedent in the scientific literature before being offered on the research chemicals market in the 2010s.<ref name="PCP2MXE">{{cite journal | vauthors=((Morris, H.)), ((Wallach, J.)) | journal=Drug Testing and Analysis | title=From PCP to MXE: a comprehensive review of the non-medical use of dissociative drugs: PCP to MXE | volume=6 | issue=7–8 | pages=614–632 | date= July 2014 | url=https://onlinelibrary.wiley.com/doi/10.1002/dta.1620 | issn=19427603 | doi=10.1002/dta.1620}}</ref>

Early discussions of this compound have revolved around whether it possesses an appreciable affinity for the [[μ-opioid]] [[receptor]] given its structural relationship to [[3-HO-PCP]], which has been shown to display affinity for the  [[μ-opioid]] [[receptor]] in animal models.<ref name="3HOPCEsar">{{cite journal | vauthors=((Kalir, A.)), ((Maayani, S.)), ((Rehavi, M.)), ((Elkavets, R.)), ((Pri-Bar, I.)), ((Buchman, O.)), ((Sokolovsky, M.)) | journal=Chemischer Informationsdienst | title=ChemInform Abstract: STRUCTURE-ACTIVITY RELATIONSHIP OF SOME PHENCYCLIDINE DERIVATIVES- IN VIVO STUDIES IN MICE | volume=9 | issue=25 | date=20 June 1978 | url=https://onlinelibrary.wiley.com/doi/10.1002/chin.197825192 | issn=00092975 | doi=10.1002/chin.197825192}}</ref> Whether it produces any of its theorized [[opioid]] effects in humans is the subject of ongoing discussion. If it does, 3-HO-PCE may pose unique risks relative to other dissociatives, particularly when it is redosed.

Following other substances of its class, particularly [[methoxetamine]] (MXE), [[phencyclidine]] (PCP), and [[3-MeO-PCE]], it is speculated to to be able to induce a state known as "[[dissociatives#Subjective effects|dissociative anesthesia]]". Early reports suggest that this state is difficult to reach relative to other [[dissociatives]], and its general effects profile has been characterized as "lying halfway between [[3-MeO-PCP]] and [[3-MeO-PCE]]."

There is a lack of data of the pharmacological properties, metabolism and toxicity of 3-HO-PCE. To date, there have been no analytical studies conducted on samples of 3-HO-PCE distributed through the grey market via independent laboratories.<ref name="PCP2MXE" /> Due to an unknown toxicity profile and likely similar habit-forming properties shared by other hydroxylanated arylcyclohexylamines, it is strongly recommended that one use proper [[harm reduction practices]] if choosing to use this substance.

 

3-HO-PCE, or 3-hydroxyeticyclidine, is a synthetic dissociative of the [[arylcyclohexylamine]] class. The structure of 3-HO-PCE is comprised of cyclohexane, a six-member saturated ring, bonded to two additional groups at R₁. One of these an ethyl chain bonded at its nitrogen group. The other ring is an aromatic phenyl ring, substituted at R₃ with a hydroxy group.  

3-HO-PCE is an analog of [[PCE]] and structurally homologous to [[3-MeO-PCE]].

While no formal studies have been conducted, 3-HO-PCE likely acts principally as an [[NMDA receptor antagonist]].<ref name="3HOPCEsar" />

 

The NMDA (N-Methyl-D-Aspartate) receptor, a specific subtype of [[glutamate]] receptor, modulates the transmission of electrical signals between neurons in the brain and spinal cord; for the signals to pass, the receptor must be open.

 

Dissociatives inhibit the normal functioning NMDA receptors by binding to and blocking them. This disruption of neural network activity leads to loss of normal cognitive and affective processing, psychomotor functioning, anesthesia.{{citation needed}}

There is ongoing speculation as to whether this compound possesses [[μ-opioid]] receptor activity due to its structural relationship to 3-HO-PCP, which has been found to have appreciable affinity as a [[μ-opioid]] [[receptor]] [[agonist]] in animal models.<ref name="3HOPCEsar" />

 

*'''[[Effect::Delusion]]'''

*'''[[Effect::Internal hallucination]]''' (''[[effect::settings, sceneries, and landscapes]]''; ''[[effect::perspective hallucinations]]'' and ''[[effect::scenarios and plots]]'')

There are currently no anecdotal reports which describe the effects of this compound within our [[experience index]]. Additional experience reports can be found here:

 

*[https://www.erowid.org/experiences/subs/exp_3HOPCE.shtml Erowid Experience Vaults: 3-HO-PCE]

{{toxicity}}

{{further|Research chemicals#Toxicity and harm potential|Responsible use #Hallucinogens}}

Early reports have characterized the chronic use of 3-HO-PCE as [[Addiction potential::moderately addictive with a moderate potential for adverse side effects such as psychosis]]. In comparison to other [[dissociatives]], 3-HO-PCE has been reported to be more potentially habit-forming than [[MXE]], [[diphenidine]], [[ephenidine]], [[DCK]], and [[ketamine]]. When addiction has developed, cravings and [[withdrawal effects]] may occur if a person suddenly stops their usage.

Tolerance to many of the effects of 3-HO-PCE is expected to develop [[Time to full tolerance::with prolonged and repeated use]]. This results in users having to administer increasingly large doses to achieve the same effects. After that, it takes about [[Time to half tolerance::4 - 7 days]] for the tolerance to be reduced to half and [[Time to zero tolerance::1 - 2 weeks]] to be back at baseline (in the absence of further consumption). 3-HO-PCE presents cross-tolerance with [[Cross-tolerance::all [[dissociative]]s]], meaning that after the consumption of 3-HO-PCE, all [[dissociatives]] will have a reduced effect.

*Users should avoid taking the drug multiple days in a row or becoming dependent/addicted to it as this seems to be the main common factor in the observed incidences of severe adverse effects.

*The recommended dosage range should not be exceeded as high doses can trigger these effects as well.

*Users should start with extremely low doses and work their way up as slowly as possible. [[Volumetric liquid dosing|Volumetric liquid dosing]] should preferably be used due to the substance's potency; most standard milligram scales cannot accurately weigh out doses below 10-15mg.<ref>3-HO-PCE (Tripsit) | https://wiki.tripsit.me/wiki/3-HO-PCE</ref>

*[[Compulsive redosing]] before one has fully sobered up is not recommended and can result in too high of a dose, which can potentially produce serious adverse physical side effects.

Due to the risk of psychosis, it is not recommended to combine this drug with other substances, especially [[stimulants]], [[psychedelics]], or other [[dissociatives]]. [https://www.google.com/ Independent research] should always be done to ensure that a combination of two or more substances is safe before consumption.

In terms of its long-term health effects when used repeatedly and excessively for extended periods of time, 3-HO-PCE is likely to exhibit similar bladder and urinary tract problems to those produced by [[ketamine]], albeit to a lesser extent. This has been speculated to be due to the fact 3-HO-PCE is far more potent than ketamine so significantly less of material needs to be consumed. Symptoms of dissociative-induced cystitis can become extremely serious and can be described as:

*'''Urinary frequency''' - Urinary frequency is the need to empty the bladder every few minutes.

*'''Hematuria''' - This is visible blood in the urine.

==Legal status==

 

*'''United Kingdom:''' 3-HO-PCE is a class B drug in the UK and is illegal to possess, produce, supply, or import. As a derivative of 1-Phenylcyclohexylamine where the amine has been replaced with a 1-piperidyl group, further substituted in the phenyl ring with a hydroxy substituent, it is covered by the arylcyclohexylamine generic clause added to the Misuse of Drugs Act by S.I. 2013/239, which came into effect on the 26th February 2013.<ref>{{Citation | title=The Misuse of Drugs Act 1971 (Amendment) Order 2013 | url=https://www.legislation.gov.uk/uksi/2013/239/introduction/made}}</ref>

 

*[https://isomerdesign.com/PiHKAL/explore.php?id=968 3-HO-PCE (Isomer Design)]

 

 

*[http://bluelight.org/vb/threads/812314-The-Big-amp-Dandy-3-HO-PCE-Thread The Big & Dandy 3-HO-PCE Thread (Bluelight)]

 

*Morris, H., & Wallach, J. (2014). From PCP to MXE: A comprehensive review of the non-medical use of dissociative drugs. Drug Testing and Analysis, 6(7–8), 614–632. https://doi.org/10.1002/dta.1620