Introduction to Cannabis PDF
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University of Florida
Stephan C. Jahn, Ph.D.
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This document is a presentation on introduction to cannabis, covering topics such as its history, chemical composition, administration methods, absorption, and effects. It details the potential uses, risks, and controversies surrounding cannabis.
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Introduction to Cannabis Stephan C. Jahn, Ph.D. Pharmacology and Therapeutics University of Florida Cannabis Cannabis sativa Cannabis indica Cannabis ruderalis Hemp...
Introduction to Cannabis Stephan C. Jahn, Ph.D. Pharmacology and Therapeutics University of Florida Cannabis Cannabis sativa Cannabis indica Cannabis ruderalis Hemp Marijuana Hashish Cannabidiol Tetrahydrocannabinol (CBD) (THC) History Use of Cannabis fibers dates back to roughly 8,000 BC Known to be used in China, India, Egypt, and Mesopotamia First recorded medical use was in China ~5,000 years ago First recreational use also in China Cannabis appears in Hindu holy books Bhang is consumed at weddings and festivals In early 1900’s cannabis was considered “an integral part of the culture and religion of the country.” Introduced into Western medicine in the 1800s Phased out in 1900s as purified medicines took hold Control of Cannabis 1961 Single Convention on Narcotic Drugs Included cannabis with opium and others Prohibited production and supply other than for medical purposes 1971 Convention on Psychotropic Substances Generated the current “schedule” drugs Placed THC in Schedule I Other cannabinoids (i.e. CBD) were not regulated U.S., among others, broadened regulations CBD from marijuana is Schedule I CBD from hemp is legal after 2018 farms bill Chemical Makeup of Cannabis Over 100 cannabinoids THC responsible for nearly all psychoactive effects Absent in roots and seeds Present at low levels in stems Present in leaves (2-3%) High in flowers (up to 25%) Other compounds can modulate THC effects Cannabinoid content varies between strains 1960’s marijuana was 2-5% THC Current street marijuana is 12% THC Cannabinoids 11 types of cannabinoids Δ9-THC and CBD are two Δ9-THC (tetrahydrocannabinol) Only psychoactive cannabinoid Δ9-THC-acid is not psychoactive Converted to Δ9-THC during heating or combustion CBD (cannabidiol) Produces many of the same effects as THC, but not psychoactive Reduces psychoactive properties of THC Concentration in street marijuana has dropped to near 0 CBD-acid is converted to CBD during combustion 100-1,000x more potent than CBD as antiemetic Historically, all NIH supplied marijuana has been low THC, high CBD Administration Smoking Vaporizing Reduces toxin formation Eating Oral tinctures Topical Absorption Smoking Most common Bioavailability ~25%, but highly variable THC plasma Cmax in 6-10 minutes 60% after 15 minutes 20% after 30 minutes Oral (Edibles or THC pill) Bioavailability ~6% Higher when in oils THC plasma Cmax in 2-6 hours Distribution THC is highly lipophilic Quickly sequestered by organs with high blood flow THC can be measured in the blood of chronic users more than a month after cessation Metabolism Extensive metabolism in liver Primarily Cytochrome P450s Three primary metabolites 11-OH-THC Psychoactive THC-COOH and glucuronide conjugates Inactive High inter-individual variability Not sex-dependent CYP2C9 variants reduce clearance Excretion Eliminated primarily as metabolites 65% in feces 25% in urine 10-20% remaining after 5 days One low THC marijuana cigarette detectable for up to 2-5 days Weeks for chronic user Tolerance Tolerance is seen with long-term use Receptor desensitization Receptor downregulation Some receptors affected more than others Some effects show tolerance while others don’t Dosing Dosing is individualized Inhalation allows dose titration Dose until desired effects are achieved 10-20 minutes between puffs Edibles do not Leads to over-consumption 3 hours between bites Average 10-20 g per week for medical use 6-7x daily inhalation 2x daily edibles Low risk of life-threatening overdose Low concentration of receptors in life-critical brain areas (i.e. respiratory/cardiac centers) No known instances Psychotic adverse effects more common (i.e. anxiety)