PCP: Difference between revisions
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It was marketed in the 1950s as an anesthetic pharmaceutical drug but was taken off the market in 1965 due to the high prevalence of dissociating and [[hallucinogenic]] side effects it produced. Afterward, a similar structurally related compound named [[ketamine]] was discovered by Parke-Davis researchers as a better-tolerated derivative for use as an anesthetic pharmaceutical drug. | It was marketed in the 1950s as an anesthetic pharmaceutical drug but was taken off the market in 1965 due to the high prevalence of dissociating and [[hallucinogenic]] side effects it produced. Afterward, a similar structurally related compound named [[ketamine]] was discovered by Parke-Davis researchers as a better-tolerated derivative for use as an anesthetic pharmaceutical drug. | ||
PCP emerged as a recreational drug in mid-1967, under the name "The Peace Pill".<ref>"Peace Pill". Microgram. Bureau of Drug Abuse Control. Jan 1968. 1(3):p1 (Erowid.org) | https://erowid.org/library/periodicals/microgram/microgram_1968_01_v01n03.pdf</ref><ref>"Sweet Streetfact's Lowdown on Low Dope Highs!". Berkeley Tribe, September 10-16, 1971. p12 (Independent Voices) | | PCP emerged as a recreational drug in mid-1967, under the name "The Peace Pill".<ref>"Peace Pill". Microgram. Bureau of Drug Abuse Control. Jan 1968. 1(3):p1 (Erowid.org) | https://erowid.org/library/periodicals/microgram/microgram_1968_01_v01n03.pdf</ref><ref>"Sweet Streetfact's Lowdown on Low Dope Highs!". Berkeley Tribe, September 10-16, 1971. p12 (Independent Voices) | https://www.jstor.org/stable/community.28033860?seq=12</ref> Since this time, a number of synthetic derivatives of PCP have been sold as dissociative drugs for both recreational and non-medical use.<ref name="morris">From PCP to MXE: a comprehensive review of the non-medical use of dissociative drugs (PubMed.gov / NCBI) | https://www.ncbi.nlm.nih.gov/pubmed/24678061</ref> As an established "street drug", PCP is associated with compulsive abuse.<ref>Malenka RC, Nestler EJ, Hyman SE (2009). "Chapter 15: Reinforcement and Addictive Disorders". In Sydor A, Brown RY. Molecular Neuropharmacology: A Foundation for Clinical Neuroscience (2nd ed.). New York: McGraw-Hill Medical. pp. 374–375. ISBN 9780071481274. </ref><ref name="morris" /> | ||
As a recreational substance, PCP may be ingested [[orally]], [[Routes of administration#Smoking|smoked]], [[insufflated]] or via [[Routes of administration#Injection|injection]].<ref>NIDA. (2016, January 11). Hallucinogens. Retrieved from https://www.drugabuse.gov/publications/drugfacts/hallucinogens on 2017, October 29 | http://drugabuse.gov/infofacts/hallucinogens.html</ref> Due to its potent dissociative and stimulant effects, known habit-forming properties as well as an established toxicity profile, it is strongly recommended that one use proper [[Responsible drug use|harm reduction practices]] if choosing to use this substance. | As a recreational substance, PCP may be ingested [[orally]], [[Routes of administration#Smoking|smoked]], [[insufflated]] or via [[Routes of administration#Injection|injection]].<ref>NIDA. (2016, January 11). Hallucinogens. Retrieved from https://www.drugabuse.gov/publications/drugfacts/hallucinogens on 2017, October 29 | http://drugabuse.gov/infofacts/hallucinogens.html</ref> Due to its potent dissociative and stimulant effects, known habit-forming properties as well as an established toxicity profile, it is strongly recommended that one use proper [[Responsible drug use|harm reduction practices]] if choosing to use this substance. |