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Tetrahydrocannabinol (THC)

Editor: Maureen C. Keshock Updated: 11/12/2023 9:35:36 PM

Indications

The Cannabis sativa plant produces numerous bioactive compounds with potential medical benefits, including terpenes, flavonoids, and cannabinoids. Among these, delta-9-tetrahydrocannabinol (THC) and cannabidiol (CBD) are the most extensively researched and studied compounds.[1][2] THC is responsible for the psychoactive effects associated with cannabis consumption. Historically, cannabis was predominantly utilized for recreational purposes due to its psychoactive properties. However, more recently, there has been significant interest in its potential medical applications. The U.S. Food and Drug Administration (FDA) recognizes the potential value of cannabis for medical purposes and acknowledges the necessity for research to mitigate unintended adverse outcomes.[3]

FDA-Approved Indications

FDA-approved synthetic THC preparations, including nabilone and dronabinol, have received recognition for their effectiveness in addressing chemotherapy-induced nausea and vomiting. Dronabinol has also received FDA approval for stimulating appetite in cases of acquired immune deficiency syndrome (AIDS)-related anorexia.[1][2] These 2 medications are the sole synthetic THC formulations that have obtained FDA approval in the United States. Nevertheless, the utilization of cannabis for various off-label and medical purposes has increased due to the legalization of medical cannabis in numerous states across the United States. Although many states have granted permission for medical marijuana usage, it remains classified as a Schedule 1 drug under federal standards, lacking recognized medical applications and posing a significant risk of abuse. In addition, as per the American Society of Clinical Oncology's 2017 guidelines, there is inadequate evidence to recommend THC as monotherapy for addressing chemotherapy-induced nausea and vomiting. However, in cases of breakthrough nausea and vomiting resistant to ondansetron, moderate evidence supports THC's effectiveness when used alongside standard antiemetic therapy.[4]

Off-Label Uses

Currently, various potential off-label applications of THC are subjects of ongoing research. Randomized controlled trials have indicated that synthetic THC dronabinol has the potential to enhance respiratory stability in individuals with moderate-to-severe obstructive sleep apnea (OSA).[5] However, additional research is essential to evaluate dronabinol's tolerability, safety profile, and potential implications for long-term drug usage. As a result, the American Academy of Sleep Medicine refrains from endorsing its usage for addressing OSA use.[6] Furthermore, a recent laboratory investigation indicates that THC might inhibit the proliferation of breast cancer cells.[7]

Randomized controlled trials have also demonstrated the efficacy of THC in effectively alleviating fibromyalgia and chronic neuropathic pain. However, the off-label use of the drug remains a subject of controversy and demands further comprehensive research.[8][9]

Despite the FDA approval of synthetic cannabinoids, dronabinol and nabilone, for chemotherapy-induced nausea and vomiting, research has not substantiated their efficacy as antiemetics for postoperative nausea and vomiting.[10] Currently, medical cannabis is legally accessible in over 50% of states, with 17 states allowing the utilization of products rich in CBD and low in THC for medical purposes.[11] However, this figure has the potential to increase in the coming years.

Although medical cannabis has gained legal status in numerous states, the FDA prohibits any product. This prohibition hampers its distribution, limits clinical research possibilities, and confines other potential therapeutic applications.[11]

Mechanism of Action

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Mechanism of Action

THC binds to cannabinoid receptors CB1 and CB2, which are integral components of the endogenous cannabinoid system. Although THC exhibits a weaker binding affinity for CB2 receptors, it also demonstrates a strong affinity for CB1 receptors. The expression and pathway of these receptors are still the focus of research. However, it is established that CB1 receptors are primarily expressed in the central nervous system (CNS), whereas CB2 receptors are found in the peripheral nervous system (PNS), immune cells, and various organs.[12][13] Upon interaction with THC, the CB1 receptor elicits hypolocomotion, hypothermia, catalepsy, and analgesia responses.[3]

THC's effects on emesis, appetite, and pain are attributed to its binding of CB1 receptors in the CNS, which modulate sensory, somatic, and cognitive perception.[4][2][8] In addition, CB2 and other receptors mediate THC's neuroprotective, anti-spasmodic, and anti-inflammatory effects.[3] When considering the potential benefits of THC in treating OSA, THC appears to act as an antagonist of serotonin in the PNS.[5] Serotonin plays a pivotal role in regulating respiration, and disturbances in its function can contribute to irregular breathing patterns during sleep.[14]

Administration

Available Dosage Forms and Strengths

The 2 FDA-approved synthetic THC compounds, nabilone and dronabinol, are available in various formulations and strengths for managing chemotherapy-induced nausea and vomiting, as well as for stimulating appetite in cases of AIDS-related anorexia in patients.

Nabilone is accessible in the form of oral capsules with strengths of 1 mg and 2 mg. In contrast, dronabinol is available in the form of oral capsules in strengths of 2.5 mg, 5 mg, and 10 mg, as well as offered in an oral solution form with a concentration of 5 mg/mL.

Adult Dosage

The recommended dosages for both nabilone and dronabinol are listed below.

  • Nabilone is commonly provided as an oral capsule with 1 mg and 2 mg strengths.
    • In patients with refractory nausea and vomiting due to cancer chemotherapy, the initial nabilone dosage ranges from 1 to 2 mg, administered twice daily. This dosing regimen lasts up to 48 hours following the final chemotherapy treatment. The highest permissible dosage of nabilone is 2 mg, administered to patients thrice daily.[15]
  • Dronabinol is available in 2 forms: as an oral capsule with strengths of 2.5 mg, 5 mg, and 10 mg, and as a 5 mg/mL oral solution packaged with a calibrated syringe.
    • For individuals with AIDS-related anorexia, the recommended starting dosage of dronabinol is 2.5 mg, taken twice daily, approximately 1 hour before lunch and dinner. The maximum daily dosage for this purpose is 10 mg.
    • In patients with refractory nausea and vomiting due to cancer chemotherapy, the recommended initial dosage of dronabinol for both the capsule and oral solution forms is 5 mg. This dosage should be administered 1 to 3 hours before commencing chemotherapy and repeated every 2 to 4 hours following chemotherapy, resulting in 4 to 6 daily doses. Ideally, the initial dose should be administered to patients after a fasting period of 10 hours and at least 30 minutes before consuming food. Subsequent doses can be administered irrespective of meals. The maximum permissible dosage for each dose is 15 mg, with a recommended frequency of 4 to 6 doses per day.[16]

Adverse Effects

The most commonly reported adverse effects of THC usage that necessitate discontinuation are dysphoria, hallucinations, and paranoia. Other prevalent adverse effects include sedation, confusion, headache, dry mouth, euphoria, and hypotension. In addition, seizures and seizure-like activity have been reported in patients using THC.[17][18]

With the growing prevalence of cannabis use, there has been a rising influx of case reports concerning cannabinoid hyperemesis syndrome (CHS). Typically, individuals experiencing CHS exhibit a distinctive pattern of cycling through nausea, vomiting, and abdominal pain, often after several months to years of prior cannabis use.[19] A distinguishing feature of this syndrome is the alleviation of symptoms through hot showers, which proves more effective than conventional treatments, such as antiemetics.[20] 

Topical capsaicin cream has demonstrated comparable relief to the effects of hot water hydrotherapy. When applied to the abdomen, it is believed to redirect blood flow from the enteric system to the skin.[20] However, complete relief of hyperemesis symptoms is achievable only by discontinuing cannabis use.[21]

An additional adverse outcome or complication associated with prolonged cannabis usage is amotivational syndrome, which presents clinically akin to depression accompanied by a lack of motivation. A recent extensive study established a correlation between individuals who misuse cannabis and the presence of apathy.[22]

Numerous studies have established a connection between marijuana use and an elevated risk for psychiatric conditions, including psychosis, depression, anxiety, schizophrenia, and substance use disorders.[23]

Furthermore, unapproved THC products can lead to unpredictable and unintended repercussions, as the FDA does not regulate their production and distribution. Consequently, there exists a diversity in reporting adverse effects unless explicitly attributed to THC. Dronabinol and nabilone are associated with adverse effects, including sedation, confusion, dry mouth, euphoria, dysphoria, and hypotension.[24]

Contraindications

Dronabinol and nabilone are contraindicated in cases of hypersensitivity to cannabinoids or any components present in their formulation. For dronabinol, this encompasses sesame oil in the capsule formulation and alcohol in the oral solution. Caution is advised when administering these medications to older patients due to the heightened susceptibility to postural hypotension and the potential occurrence of cannabis-induced delirium.

Dronabinol is classified as a pregnancy Category C drug, as it has not exhibited teratogenic effects in animal models at doses ranging from 0.2 to 5 times the maximum recommended human dose. However, it is essential to note that pregnant patients have not been subjected to adequately controlled studies.[15] Similarly, nabilone is also classified as a pregnancy Category C drug. Therefore, healthcare providers should exercise caution and refrain from prescribing these medications to pregnant women or nursing mothers.[16]

Monitoring

When considering FDA-approved THC preparations, healthcare providers should diligently evaluate potential psychiatric or cognitive impairment connected to THC use. In addition, they should remain vigilant about possible drug interactions that could result in similar effects. Polypharmacy poses a substantial concern for older patients. Monitoring hemodynamic changes after drug administration is also imperative. To ensure safety, patients must be given explicit instructions on refraining from driving or operating heavy machinery until they are confident that using dronabinol or nabilone does not cause any psychomotor impairment.

The risk of dependence and misuse should also be thoroughly assessed, particularly in patients with a history of substance misuse or addiction. Given the occurrence of seizures or seizure-like activity in individuals using THC, caution is paramount when prescribing the drug to patients with risk factors or a history of seizures, including those concurrently taking anti-epileptic medication.[25]

Toxicity

The median lethal dose (LD50) of THC has been determined in various animal species through oral administration and ranges from 800 to 9000 mg/kg. In humans, there have been no recorded instances of fatal overdoses resulting from acute THC use. However, estimates for a potentially lethal human dose range from 4 to 15 g.[24]

Acute intoxication is dose-dependent and typically short-lived, often encompassing cardiovascular effects at higher doses.[24] Chronic use of THC has been associated with conditions such as hypotension, tachycardia, and bradycardia.[26][24] Furthermore, chronic use of THC is linked to an extensive array of psychiatric conditions, including fear, distrust, hallucinations, stupor, and seizures.[26]

In instances of marijuana intoxication, the approach to treatment is centered on supportive care and symptom management.[27] When dealing with CHS in patients, the primary focus of the management involves discontinuing cannabis usage.[28]

Enhancing Healthcare Team Outcomes

Prudent patient selection is essential when prescribing FDA-approved THC formulations for medical purposes. Due to THC's potential sedation and euphoria effects, healthcare providers should consider the patient's history of drug misuse or dependency and the potential for polypharmacy. Furthermore, the psychoactive effects of THC, including hallucinations, dysphoria, and paranoia, can be distressing for certain patients.[17][18] Consequently, a multidisciplinary and interprofessional approach, involving physicians, advanced practice practitioners, psychiatrists, addiction specialists, nursing staff, and pharmacists, is imperative when caring for these patients. This collaborative team effort is responsible for comprehensive screening to identify potential drug misuse, address adverse effects, and manage THC-induced psychiatric and medical issues. Furthermore, prescribers and pharmacists must be aware of the complex legal framework associated with the medical use of THC. As of 2020, more than half of the states in the United States have legalized THC for medical purposes, and several states have also extended permission for its recreational use.[29]

However, the legal status of THC remains consistently dynamic. On a federal level, marijuana is categorized as a Schedule I drug, and there is no officially sanctioned federal recognition of medical marijuana usage. No formal legal decision has addressed this inconsistency between state and federal laws. Thus, healthcare providers must stay up-to-date with both state and federal regulations to ensure the well-being of both the patient and the prescriber.[30] Certain synthetic THC compounds have received FDA approval for treating AIDS-related anorexia and chemotherapy-induced nausea and vomiting in patients. Notably, specific chemotherapy regimens, which incorporate cyclophosphamide, methotrexate, and fluorouracil, are recognized for their emetogenic potential.

Randomized clinical trials have demonstrated that THC was more effective in patients receiving these chemotherapy agents than other second-line antiemetics, such as prochlorperazine and metoclopramide. Nonetheless, in the context of highly emetogenic chemotherapy regimens, such as those involving high-dose methotrexate, cisplatin, or doxorubicin, THC did not exhibit superior effectiveness.[17]

Furthermore, ongoing investigations are exploring other potential applications of THC, and its off-label utilization might offer therapeutic benefits for certain conditions in patients. THC's potential roles in managing OSA and chronic neuropathic pain are among the most promising research areas. Randomized control trials have indicated that THC can effectively improve OSA and chronic neuropathic pain. However, these studies were conducted on a limited scale and yielded results that were not entirely conclusive. Therefore, additional research is essential to comprehensively assess THC's tolerability and adverse effect profile when treating these conditions.[6][8][9]

With ongoing research, there exists a promising potential for the FDA to approve additional medical indications for THC usage. A comprehensive conversation between the prescribing or ordering clinician and the patient is essential, focusing on both the advantages and potential drawbacks of THC usage. Furthermore, effective interprofessional communication among all members of the healthcare team, including clinicians and pharmacists, can significantly enhance patient outcomes for those receiving treatment with currently approved indications for THC formulations. All interprofessional team members must keep abreast of the latest data-driven evidence for these agents and utilize open communication to share the latest advancements with other providers. This collaborative approach is pivotal in accurately evaluating the suitability of these agents for a particular patient's use.

References


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