Medical and Legalized Marijuana



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Medical and Legalized Marijuana From pain relief to recreational use Schoen W. Kruse, Ph.D.

Dr. White, a practicing family physician in Kansas City, MO, walks into an examination room and meets a 31 y/o female named Rachel. Rachel has a 3 year history of multiple sclerosis (MS). She was born in KC, MO and now lives in California. She has been in town visiting family and friends for the past 2 weeks. Rachel s MS is categorized as the primary progressive MS (PPMS) type, in which the disease progresses from the onset with occasional plateaus, temporary minor improvements, and acute relapses. Over the course of her disease, she has taken the immunosuppressive therapies cyclosporine, methotrexate, cyclophosphamide, interferon, and steroids.

Most of the treatments Rachel has tried have temporarily halted disease progression, but they have not resulted in long-term symptom management. As a result, Rachel has become reliant on medical marijuana for symptom management, which has offered the only consistent relief of her symptoms. Rather than fly, she drove to KC so that could bring marijuana on her trip to control her symptoms. Rachel arrives in Dr. White s office in distress because her supply of medical marijuana was exhausted by her nephew and his friends (they found the drug in her travel bag and took it and smoked it). She is suffering and is looking to Dr. White for help. Ethical Clinical Legal

Session Objectives After attending the CME session on Medical and Legalized Marijuana, you will be able to: 1. Compare and contrast the known effects of tetrahydrocannabinol (THC) and cannabidiol (CBD). 2. Identify symptoms that may be relieved by treatment with marijuana or other cannabinoids 3. Identify applicable medical marijuana laws in states in which you have a medical license.

Exogenous cannabinoids Extracted from the marijuana plant Cannabis sativa or Cannabis indica Over 100 cannabinoids have been identified in the marijuana plant Tetrahydrocannabinol (THC) Major psychoactive component in marijuana Cannabis sativa Cannabidiol (CBD) Doesn t produce any of the psychoactive effects of THC Doesn t make you high, paranoid, hallucinate Cannabis indica www.thcdigest.com/indica-vs-sativa

Receptors that bind exogenous cannabinoids CB1 receptors CNS neurons in the basal ganglia, limbic system, cerebellum, cortex Activation causes psychotropic effects, dependence, and cognitive impairment CB2 receptors Distribution predominantly in cells and tissues of the immune system (thymus, tonsils, B & T lymphocytes, macrophages, monocytes, NK cells) Expressed in microglial cells (CNS version of immune cells) during various states of inflammation Activation largely devoid of psychotropic effects Serotonin receptors, GPR-55, TRVP1 receptor, others

Effects of THC and CBD THC CB1 and CB2 receptor partial agonist Responses strongly influenced both by the expression level and signaling efficiency of CB1/CB2 receptors and by ongoing endogenous cannabinoid release CBD High potency as an antagonist of CB1/CB2 receptor agonists in CB1- and CB2- expressing cells or tissues Antagonist actions helps explain its ability to inhibit evoked immune cell migration May prevent THC from acting as agonist (hallucinogenic effects)

What are the components of marijuana? Heterogeneity in the composition of marijuana seized in California THC levels have risen consistently since the mid 1990s As the desire for marijuana with high hallucinogenic effects increased, CBD levels decreased

CBD may be the real star CBD has gained particular interest recently as a constituent in the medication Sativex, which has been found to alleviate spasticity associated with MS, cancer pain in opioid-treated patients, and marijuana withdrawal CBD is under investigation in assorted clinical trials as an anti-epileptic Preclinical studies reported that CBD elicits anticonvulsant, anti-inflammatory, and anti-tumorgenic effects. http://www.ncbi.nlm.nih.gov/pubmed

Clinical conditions with symptoms that may be relieved by treatment with marijuana or other cannabinoids

Glaucoma Marijuana can cause a transient decrease in intraocular pressure (1970s, 1980s) Other, standard treatments are currently more effective More research is needed to establish whether molecules that modulate the endocannabinoid system may not only reduce intraocular pressure but also provide a neuroprotective benefit in patients with glaucoma

Nausea Treatment of the nausea and vomiting associated with chemotherapy was one of the first medical uses of THC and other cannabinoids THC is an effective antiemetic agent in patients undergoing chemotherapy,59 but patients often state that marijuana is more effective in suppressing nausea Other, unidentified compounds in marijuana may enhance the effect of THC (as appears to be the case with THC and CBD) Paradoxically, increased vomiting (hyperemesis) has been reported with repeated marijuana use

AIDS-associated anorexia and wasting syndrome Smoked or ingested cannabis improves appetite and leads to weight gain and improved mood and quality of life among patients with AIDS However, there is no long-term or rigorous evidence of a sustained effect of cannabis on AIDS-related morbidity and mortality, with an acceptable safety profile, that would justify its incorporation into current clinical practice for patients who are receiving effective antiretroviral therapy Data from the few studies that have explored the potential therapeutic value of cannabinoids for this patient population are inconclusive

Chronic pain Marijuana has been used to relieve pain for centuries Studies have shown that cannabinoids acting through central CB1 receptors and possibly peripheral CB1 and CB2 receptors play important roles in modeling nociceptive responses in various models of pain Marijuana has been shown to be effective in ameliorating neuropathic pain at very low levels of THC (1.29%) Both marijuana and dronabinol (synthesized THC) decrease pain, but dronabinol may lead to longer-lasting reductions in pain sensitivity and lower ratings of rewarding effects

Inflammation THC and CBD have substantial anti-inflammatory effects because of their ability to induce apoptosis, inhibit cell proliferation, and suppress cytokine production CBD has attracted particular interest as an anti-inflammatory agent because of its lack of psychoactive effects Animal models have shown that CBD is a promising candidate for the treatment of rheumatoid arthritis and for inflammatory diseases of the gastrointestinal tract (e.g., ulcerative colitis and Crohn's disease)

Multiple sclerosis Nabiximols (Sativex), an oromucosal spray that delivers a mix of THC and CBD, appears to be an effective treatment for neuropathic pain, disturbed sleep, and spasticity in patients with multiple sclerosis Sativex is available in the United Kingdom, Canada, and several other countries and is currently being reviewed in phase 3 trials in the United States in order to gain approval from the Food and Drug Administration The National Multiple Sclerosis society supports the rights of people with MS to work with their MS health care providers to access marijuana for medical purposes in accordance with legal regulations in those states where such use has been approved (www.nationalmssociety.org)

Epilepsy In a recent small survey of parents (19 families) who use marijuana with a high CBD content to treat epileptic seizures in their children: 11% reported complete freedom from seizures 42% reported a reduction of more than 80% in seizure frequency 32% (6 families) reported a reduction of 25 to 60% in seizure frequency Although such reports are promising, insufficient safety and efficacy data are available on the use of cannabis botanicals for the treatment of epilepsy There is increasing evidence of the role of CBD as an antiepileptic in animal models

Clinical trials 80 total studies for cannabidiol (CBD) 132 total studies for tetrahydrocannabinol (THC) Conditions involved Epilepsy Substance abuse Pain Autoimmune diseases Demyelinating diseases Multiple sclerosis Psychiatric disorders www.clinicaltrials.gov

Level of Confidence in the Evidence for Adverse Effects of Marijuana on Health and Well-Being Compared to adverse effects from current therapy options? NEJM 370; 23. 2014

Back to our case Dr. White, a practicing family physician in Kansas City, MO, walks into an examination room and meets a 31 y/o female named Rachel. Rachel has a 3 year history of multiple sclerosis (MS). She was born in KC, MO and now lives in California. She has been in town visiting family and friends for the past 2 weeks. Rachel s MS is categorized as the primary progressive MS (PPMS) type, in which the disease progresses from the onset with occasional plateaus, temporary minor improvements, and acute relapses. Over the course of her disease, she has taken the immunosuppressive therapies cyclosporine, methotrexate, cyclophosphamide, interferon, and steroids. Most of the treatments Rachel has tried have temporarily halted disease progression, but they have not resulted in long-term symptom management. As a result, Rachel has become reliant on medical marijuana for symptom management, which has offered the only consistent relief of her symptoms. She travelled by car across the country so that she could bring marijuana on her trip to control her symptoms. Rachel arrives in Dr. White s office in distress because her supply of medical marijuana was exhausted by her nephew and his friends (they found the drug in her travel bag and took it and smoked it). She is suffering and is looking to Dr. White for help. Ethical Clinical Legal

Marijuana in the 1600-1800s American production of hemp was encouraged by the government in the 17th century for the production of rope, sails, and clothing In 1619 the Virginia Assembly passed legislation requiring every farmer to grow hemp. Hemp was allowed to be exchanged as legal tender in Pennsylvania, Virginia, and Maryland Domestic production flourished until after the Civil War, when imports and other domestic materials replaced hemp for many purposes In the late nineteenth century, marijuana became a popular ingredient in many medicinal products and was sold openly in public pharmacies www.pbs.org, 9/9/2015

Brief history of marijuana regulation 1906 Pure Food and Drug Act requiring labeling of any cannabis in OTC remedies 1930 Creation of the Federal Bureau of Narcotics 1932 Uniform State Narcotic Act encouraging state governments to control rising use of marijuana 1936 Reefer Madness propaganda film about the dangers of marijuana use 1937 Marijuana tax act criminalizing marijuana except authorized medical and industrial uses 1951-56 Boggs Act and Narcotics Control Act set mandatory sentences for marijuanarelated offenses 1968 Creation of the Bureau of Narcotics and Dangerous Drugs 1970 Controlled Substances Act eliminated mandatory federal sentences for possession of small amounts; marijuana is a Schedule I substance 1973 Creation of the Drug Enforcement Agency 1986 Anti-Drug Abuse Act institutes mandatory sentences for drug-related crimes 1996 Medical use legalized in California 2009 Memo to federal prosecutors encouraging them not to prosecute people who distribute marijuana for medical purposes in accordance with state law www.pbs.org, 9/9/2015 www.ncsl.org, 8/11/2015

Federal perspective a mixed message? Marijuana is a Schedule I substance under the Controlled Substances Act Considered to have a high potential for dependency and no accepted medical use Distribution of marijuana is a federal offense. October 2009 Obama Administration sends a memo to federal prosecutors encouraging them not to prosecute people who distribute marijuana for medical purposes in accordance with state law August 2013 USDOJ announces update to their marijuana enforcement policy USDOJ expects states like CO and WA to create "strong, state-based enforcement efforts... and will defer the right to challenge their legalization laws at this time." USDOJ reserves the right to challenge the states at any time they feel it's necessary. www.ncsl.org 8/11/2015

What is legal and what is not? National Conference of State Legislatures www.ncsl.org State medical marijuana/cannabis program laws Limited access marijuana product laws (low THC/high CBD) Links to legal documentation State vs. federal perspective Marijuana Policy Project www.mpp.org Federal and state policies Ballot initiatives

State medical marijuana/cannabis program laws 23 states, the District of Columbia and Guam now allow for comprehensive public medical marijuana and cannabis programs Comprehensive program Protection from criminal penalties for using marijuana for a medical purpose Access to marijuana through home cultivation, dispensaries or some other system that is likely to be implemented It allows a variety of strains, including those more than "low THC" It allows either smoking or vaporization of some kind of marijuana products, plant material or extract www.ncsl.org 8/11/2015

State medical marijuana/cannabis program laws State Statutory Language (year) Arizona Proposition 203 (2010) Colorado Amendment 20 (2000) California Proposition 215 (1996) SB 420 (2003) Patient Registry or ID cards Allows Dispensaries Specifies Conditions Yes Yes Yes Yes Recognizes Patients from other states State Allows for Retail Sales/Adult Use Yes Yes Yes No Amendment 64 (2012) Yes Yes (cooperatives and collectives) Michigan Proposal 1 (2008) Yes Not in state law, but localities may create ordinances to allow them and regulate them. Alaska, Connecticut, Delaware, DC, Guam, Hawaii, Illinois, Maine, Maryland, Massachusetts, Minnesota, Montana, Nevada, New Hampshire, New Jersey, New Mexico, New York, Oregon, Rhode Island, Vermont, Washington www.ncsl.org 8/11/2015 No Yes Yes

Variability from state to state Serious medical condition": Acquired immune deficiency syndrome (AIDS) Anorexia Arthritis Cachexia Cancer Chronic pain Glaucoma Migraine Severe nausea Persistent muscle spasms, including, but not limited to, spasms associated with multiple sclerosis Seizures, including, but not limited to, seizures associated with epilepsy. Any other chronic or persistent medical symptom that either: (A) Substantially limits the ability of the person to conduct one or more major life activities as defined in the Americans with Disabilities Act of 1990. (B) If not alleviated, may cause serious harm to the patient's safety or physical or mental health.

Variability from state to state Debilitating medical condition": Cancer multiple sclerosis HIV AIDS The treatment of these conditions, if the disease or the treatment results in severe, persistent, and intractable symptoms; OR a disease, medical condition, or its treatment that is chronic, debilitating, and produces severe, persistent, and one or more of the following intractable symptoms: Cachexia or wasting syndrome Severe pain Severe nausea Seizures

Limited access marijuana product laws 17 states allow use of "low THC, high cannabidiol (CBD)" products for medical reasons in limited situations or as a legal defense State Program Name and Statutory Language (year) Patient Registry or ID cards Dispensaries or Source of Product(s) Specifies Conditions Recognizes Patients from other states Definition of Products Allowed Allows for Legal Defense Allowed for Minors Missouri HB 2238 (2014) Yes Yes, creates cannabidiol oil care centers and cultivation and production facilities/laboratories. Yes, intractable epilepsy that has not responded to three or more other treatment options. No "Hemp extracts" equal or less than.3% THC and at least 5% CBD by weight. Yes Yes Alabama, Florida, Georgia, Iowa, Kentucky, Louisiana, Mississippi, North Carolina, Oklahoma, South Carolina, Tennessee, Texas, Utah, Virginia, Wisconsin, Wyoming www.ncsl.org 8/11/2015

Variability from state to state State Specifies Conditions Definition of Products Allowed Missouri Yes, intractable epilepsy that has not responded to three or more other treatment options. "Hemp extracts" equal or less than.3% THC and at least 5% CBD by weight. Alabama Yes, debilitating epileptic conditions or life-threatening seizures. Extracts that are low THC= below 3% THC Florida Georgia Yes, cancer, medical condition or seizure disorders that chronically produces symptoms that can be alleviated by low-thc products Yes, end stage cancer, ALS, MS, seizure disorders, Crohn's, mitochondrial disease, Parkinson's, Sickle Cell disease Cannabis with low THC= below.8% THC and above 10% CBD by weight Cannabis oils with low THC= below 5% THC and at least an equal amount of CDB. Iowa Yes, intractable epilepsy "Cannabidiol- a non-psychoactive cannabinoid" that contains below 3% THC, no more than 32 oz, and essentially free from plant material. Kentucky Intractable seizure disorders No, only "cannabidiol" www.ncsl.org 8/11/2015

Missouri hemp extract registration card http://www.health.mo.gov/about/proposedrules/hempextract.php

Back to our case Dr. White, a practicing family physician in Kansas City, MO, walks into an examination room and meets a 31 y/o female named Rachel. Rachel has a 3 year history of multiple sclerosis (MS). She was born in KC, MO and now lives in California. She has been in town visiting family and friends for the past 2 weeks. Rachel s MS is categorized as the primary progressive MS (PPMS) type, in which the disease progresses from the onset with occasional plateaus, temporary minor improvements, and acute relapses. Over the course of her disease, she has taken the immunosuppressive therapies cyclosporine, methotrexate, cyclophosphamide, interferon, and steroids. Most of the treatments Rachel has tried have temporarily halted disease progression, but they have not resulted in long-term symptom management. As a result, Rachel has become reliant on medical marijuana for symptom management, which has offered the only consistent relief of her symptoms. She travelled by car across the country so that she could bring marijuana on her trip to control her symptoms. Rachel arrives in Dr. White s office in distress because her supply of medical marijuana was exhausted by her nephew and his friends (they found the drug in her travel bag and took it and smoked it). She is suffering and is looking to Dr. White for help.

Session Objectives After attending the CME session on Medical and Legalized Marijuana, you will be able to: 1. Compare and contrast the known effects of tetrahydrocannabinol (THC) and cannabidiol (CBD). 2. Identify symptoms that may be relieved by treatment with marijuana or other cannabinoids 3. Identify applicable medical marijuana laws in states in which you have a medical license.

References 1. Burgdorf JR, Kilmer B, Pacula RL. Heterogeneity in the composition of marijuana seized in California. Drug Alcohol Depend. 2011 Aug 1;117(1):59-61. 2. Cabral, GA and Griffin-Thomas, L. Emerging role of the cannabinoid receptor CB2 in immune regulation: Therapeutic prospects for neuroinflammation. Expert Reviews in Molecular Medicine 11, No. 1 (2009): e3. 3. Cabral, GA, Rogers, TJ, Lichtman, AH. Turning Over a New Leaf: Cannabinoid and Endocannabinoid Modulation of Immune Function. J Neuroimmune Pharmacol. 2015; 10(2): 193 203. 4. Casarett, D. Stoned. Current Publishing. 2015. 5. National Conference of State Legislatures website (www.ncsl.org) 6. Marijuana Policy Project website (www.mpp.org) 7. Pertwee, RG. The diverse CB1 and CB2 receptor pharmacology of three plant cannabinoids: delta-9- tetrahydrocannabinol, cannabidiol, and delta-9-tetrahydrocannabivarin. British Journal of Pharmacology 153, 199-215. 2008. 8. Volkow ND, Baler RD, Compton WM, Weiss SR. Adverse health effects of marijuana use. N Engl J Med. 2014;370(23):2219 2227. 9. Whiting, PF, et. al. Cannabinoids for Medical Use: A systematic review and meta-analysis. JAMA. 2015; 313(24): 2456-2473.