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$8.40

Buy 3-HO-PCP Sale Online is high quality Research Chemicals. You can buy 3-ho-pcp online at wholesale price from trust supplier Top Mark Chemical

3-ho-pcp (also named ) is very similar with 2-FDCK, 3-meo-pcp.

3-Hydroxyphencyclidine (commonly known as 3-HO-PCP) is a novel dissociative substance of the arylcyclohexylamine class that produces potent dissociative, hallucinogenic and euphoric effects when administered. In addition to its primary activity as a NMDA receptor antagonist, it has been found to have appreciable affinity for the μ-opioid receptor.

3-HO-PCP was first synthesized in 1978 to investigate the structure-activity relationship of phencyclidine (PCP) derivatives. It was further explored alongside PCP in the 1980s, where it was discovered to possess μ-opioid agonist activity in animal models.

Like other substances of its class, particularly methoxetamine (MXE), phencyclidine (PCP), and 3-MeO-PCE, it is known to primarily induce a state referred to as “dissociative anesthesia”, albeit the extent to which this occurs has been reported to be highly dose-dependent and variable in its effects.[citation needed] It is unknown whether the studied opioid properties in animal models applies to humans, with some early reports suggesting that it does not.

There are also reports that suggest this compound may produce more physical side effects such as muscle soreness and flu-like symptoms during or shortly after administration. This suggests it may be uniquely more dangerous or toxic than related dissociatives, particularly at higher doses.

Today, 3-HO-PCP is almost exclusively distributed as a gray area research chemical by online vendors. Extremely little is known about its pharmacology, metabolism and toxicity in humans. Due to its sensitive dose-response, potential habit-forming properties, as well as unknown toxicity profile, it is strongly recommended that one use proper harm reduction practices if choosing to use this substance.

The physiological and toxicological properties of this compound are not known. This product is intended for forensic and research applications.

There are also reports that suggest this compound may produce more physical side effects such as muscle soreness and flu-like symptoms during or shortly after administration. This suggests it may be uniquely more dangerous or toxic than related dissociatives, particularly at higher doses.

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Buy 3-HO-PCP Sale Online UK GERMANY US AUSTRALIA

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Firstly Buy 3-HO-PCP Sale Online, Today, 3-HO-PCP is disseminate as a hazy area inquire about concoction by online merchants. Very little is known about its pharmacology, digestion and harmfulness in people.

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Reports that suggest this compound may produce more physical side effects such as muscle soreness and flu-like symptoms during.

This suggests it may be uniquely more dangerous than relate dissociatives, particularly at higher doses.

Today, 3-HO-PCP is almost exclusively distribute as a gray area research chemical by online vendors.
little is known about its pharmacology, metabolism and toxicity in humans.

Due to its sensitive dose-response, potential habit-forming properties as well as unknown toxicity profile.

It is strongly recommend that one use proper harm reduction practices if choosing to use this substance.

History Of 3-HO-PCP Sale Online

Buy 3-HO-PCP Sale Online ; 3-HO-PCP was first synthesized in 1978 to investigate the structure-activity relationship of phencyclidine derivatives.

It was further explore alongside PCP in the 1980s, where it was discover to possess μ-opioid agonist activity in animal models.

Its potential as a research chemical for human use was not suggest until 1999 when a chemist using the pseudonym John Q.

Beagle report on its significantly increase potency relative to PCP as well as its “profoundly enhance affinity for the opiate receptor” which was estimate to give it analgesic activity one order of magnitude lower than morphine.

On October 18, 2012, the Advisory Council on the Misuse of Drugs in the United Kingdom release a report about methoxetamine,

saying that the “harms of methoxetamine are commensurate with Class B of the Misuse of Drugs Act (1971)”, despite the fact that the act does not classify drugs base on harm.

The report suggests that all analogs of MXE should also become class B drugs and suggest a catch-all clause covering both existing and unresearch arylcyclohexamines, including 3-HO-PCP.

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