Diferencia entre revisiones de «Kratom toxicity»
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==Background== | ==Background== | ||
[[File:Kratom leaves.jpg|thumb|Kratom flowers and foliage.]] | [[File:Kratom leaves.jpg|thumb|Kratom flowers and foliage.]] | ||
*Derived from ''Mitragyna speciosa,'' a | [[File:Powdered kratom.jpg|thumb|Typical powdered Kratom for commercial use.]] | ||
* | *Derived from ''Mitragyna speciosa,'' a tropical evergreen tree in the coffee family native to Southeast Asia | ||
* | *Leaves contain over 40 alkaloids; the two most clinically relevant are: | ||
** | **Mitragynine (most abundant, up to 66% of total alkaloid content) — partial mu-opioid receptor agonist<ref name="kruegel">Kruegel AC, Grundmann O. The medicinal chemistry and neuropharmacology of kratom: A preliminary discussion of a promising medicinal plant and analysis of its potential for abuse. ''Neuropharmacology''. 2018;134(Pt A):108-120.</ref> | ||
**7-Hydroxymitragynine (7-OH) (minor constituent, <2% of alkaloid content) — approximately 5-fold greater mu-opioid affinity than mitragynine<ref name="kruegel"/> | |||
*Both alkaloids exhibit G-protein biased agonism at mu-opioid receptors with limited beta-arrestin recruitment (theoretically less respiratory depression than classical opioids, though still reported)<ref name="kruegel"/> | |||
*Additional receptor activity at alpha-1A, alpha-2A, 5-HT1A, 5-HT2A, D1, and D2 receptors contributes to mixed stimulant-opioid clinical picture<ref name="yusof">Yusof SR, Zakaria Z, Amir Rawa MS, et al. Kratom Alkaloids: Interactions With Enzymes, Receptors, and Cellular Barriers. ''Front Pharmacol''. 2021;12:751656.</ref> | |||
*Mitragynine is metabolized by CYP3A4 to 7-hydroxymitragynine (a more potent metabolite) and inhibits CYP2D6 and CYP3A4, creating significant potential for drug-drug interactions<ref name="tanna">Tanna RS, Tian DD, Cech NB, et al. Refined Prediction of Pharmacokinetic Kratom-Drug Interactions: Time-Dependent Inhibition Considerations. ''J Pharmacol Exp Ther''. 2021;376(1):64-73.</ref> | |||
*Available in the US as powder, capsules, tablets, extracts, and liquid "shots" sold at gas stations, smoke shops, and online | |||
**Products are unregulated, with highly variable alkaloid content and potential for contamination (''[[Salmonella]]'', heavy metals including lead)<ref name="fda">U.S. Food and Drug Administration. FDA and Kratom. Updated February 2024. https://www.fda.gov/news-events/public-health-focus/fda-and-kratom</ref> | |||
*Estimated 1.7 million Americans aged ≥12 used kratom in 2021<ref name="fda"/> | |||
*Not FDA-approved for any indication; not a legal dietary supplement or food additive<ref name="fda"/> | |||
*Federally unscheduled but banned in several states (Alabama, Arkansas, Indiana, Vermont, Wisconsin, Louisiana); regulated in many others<ref name="crs">Congressional Research Service. Kratom Regulation: Federal Status and State Approaches. LSB11082. 2024.</ref> | |||
*Patients commonly use for self-treatment of [[chronic pain]], [[opioid withdrawal]], depression, and anxiety | |||
**Approximately one-third of users co-ingest with other substances<ref name="wapc">Washington Poison Center. Kratom and 7-hydroxymitragynine poisoning. 2025. https://www.wapc.org/data/data-blogs/kratom-and-7-hydroxymitragynine-poisoning/</ref> | |||
==Clinical Features== | ==Clinical Features== | ||
*Effects are dose dependent and may mimic | *Effects are dose-dependent and may mimic both opioid and stimulant toxicity | ||
*Stimulant effects | *Onset of effects typically within 10-20 minutes of ingestion; duration 2-5 hours | ||
===Low-Dose Effects (<5 g)=== | |||
*Stimulant effects predominate | |||
*Increased alertness and energy | |||
*[[Tachycardia]], [[hypertension]] | |||
*Agitation, jitteriness | |||
*Decreased appetite | |||
===High-Dose Effects (>5 g)=== | |||
*Opioid-like sedation predominates | |||
*[[Miosis]] | |||
*[[Respiratory depression]] (especially with co-ingestions or concentrated extracts) | |||
*Drowsiness, [[altered mental status]] | |||
*Nausea, [[vomiting]] | |||
*Constipation | |||
===Severe/Complicated Presentations=== | |||
*[[Seizures]]<ref name="statpearls">Eastlack SC, Cornett EM, Kaye AD. Kratom—Pharmacology, Clinical Implications, and Outlook: A Comprehensive Review. ''Pain Ther''. 2020;9(1):55-69.</ref> | |||
*[[Respiratory failure]] requiring [[intubation]] | |||
*[[Rhabdomyolysis]] and [[acute kidney injury]]<ref name="auctores">Narrative Review of Kratom in the Emergency Department. ''Auctores''. 2025.</ref> | |||
*'''Hepatotoxicity''' — typically cholestatic pattern, onset 1-8 weeks of regular use; can be severe (bilirubin >20 mg/dL); usually reversible with cessation<ref name="livertox">LiverTox: Clinical and Research Information on Drug-Induced Liver Injury. Kratom. National Institute of Diabetes and Digestive and Kidney Diseases; 2020.</ref> | |||
*Cardiac arrest (rare, primarily in polydrug exposure)<ref name="poison">Poison Control. What is kratom? https://www.poison.org/articles/kratom</ref> | |||
*[[QT prolongation]] (theoretical and case-reported) | |||
===Kratom Withdrawal=== | |||
*Occurs with chronic use; onset typically within 12-24 hours of last dose<ref name="auctores"/> | |||
*Resembles mild-moderate [[opioid withdrawal]]: myalgias, rhinorrhea, diaphoresis, insomnia, irritability, nausea, diarrhea | |||
*Generally less severe than traditional opioid withdrawal | |||
*Can be scored using the [[Clinical Opiate Withdrawal Scale]] (COWS) | |||
==Differential Diagnosis== | ==Differential Diagnosis== | ||
*[[Opioid | *[[Opioid toxicity]] | ||
*[[Opioid withdrawal]] | *[[Opioid withdrawal]] | ||
*[[Sympathomimetic | *[[Sympathomimetic toxicity]] | ||
*[[Anticholinergic toxicity]] | *[[Anticholinergic toxicity]] | ||
*[[Serotonin syndrome]] (due to serotonergic activity) | |||
*[[Tianeptine toxicity]] (similar presentation, also sold at gas stations) | |||
*[[Xylazine toxicity]] | |||
*[[Phenibut toxicity]] | |||
{{Drugs of abuse types}} | |||
==Evaluation== | ==Evaluation== | ||
* | *Primarily a '''clinical diagnosis''' — ask specifically about kratom, herbal supplements, and "gas station" products | ||
*Labs | *'''Kratom does NOT appear on standard urine drug screens'''<ref name="statpearls"/> | ||
**May cause false-negative opioid screen despite opioid-like presentation | |||
**Specialized testing for mitragynine exists but is not widely available and generally not clinically useful in the acute setting | |||
*Consider early consultation with [[Poison control]] (1-800-222-1222) | |||
===Labs=== | |||
*Not routinely required for mild presentations | |||
*For moderate-severe presentations, consider: | |||
**[[CBC]], [[BMP]]/[[CMP]] | |||
**[[LFTs]] — particularly if chronic use or concern for hepatotoxicity | |||
**[[CK]] if agitated, seizing, or prolonged immobilization ([[rhabdomyolysis]]) | |||
**[[Lactate]], [[VBG]] | |||
**[[Acetaminophen]] and [[salicylate]] levels, [[ethanol]] level to rule out co-ingestion | |||
**[[Urine drug screen]] — will be negative for kratom, but useful to evaluate for co-ingestions | |||
**[[Coagulation studies]] if hepatotoxicity suspected | |||
===ECG=== | |||
*Obtain [[EKG]] in moderate-severe presentations | |||
*Evaluate for [[tachycardia]], [[QT prolongation]] | |||
==Management== | ==Management== | ||
* | *Focus on ABCs and symptom-directed treatment | ||
**[[Naloxone]] for respiratory depression | *Consider early [[Poison control]] consultation (1-800-222-1222) | ||
**[[Benzodiazepines]] for hyperarousal, tachycardia, hypertension, and seizures | |||
**[[NSAIDs]], [[ | ===Respiratory Depression=== | ||
***Medication-assisted treatment | *Supplemental oxygen, [[BVM]] ventilation as needed | ||
*[[Naloxone]] — effective for kratom-induced respiratory depression due to mu-opioid agonism<ref name="greatimitator">Mikkelsen A, Van Roekel C, Grande EJ, et al. The Great Imitator: A Case of Accidental Kratom Overdose. ''Cureus''. 2023;15(7):e42497.</ref> | |||
**Standard dosing as per [[opioid toxicity]] protocols | |||
**Be aware of potential for rebound respiratory depression within 24 hours per poison control center reports<ref name="greatimitator"/> | |||
===Agitation / Sympathomimetic Features=== | |||
*[[Benzodiazepines]] for hyperarousal, agitation, [[tachycardia]], [[hypertension]], and [[seizures]] | |||
*IV fluids | |||
*Avoid [[haloperidol]] if concern for [[QT prolongation]] | |||
===Seizures=== | |||
*[[Benzodiazepines]] are first-line | |||
*Standard [[seizure]] management algorithm | |||
===Kratom Withdrawal=== | |||
*Symptom-directed treatment similar to [[opioid withdrawal]]: | |||
**[[NSAIDs]] for myalgias | |||
**[[Antiemetics]] (e.g., [[ondansetron]]) for nausea/vomiting | |||
**[[Loperamide]] for diarrhea | |||
**[[Clonidine]] for autonomic symptoms | |||
**IV fluids for dehydration | |||
*Medication-assisted treatment for opioid use disorder: | |||
**[[Buprenorphine]] — most commonly reported for kratom withdrawal/dependence; can be initiated in the ED per standard protocols<ref name="wapc"/> | |||
**[[Methadone]] — alternative for patients not candidates for buprenorphine | |||
===Hepatotoxicity=== | |||
*Discontinue kratom | |||
*Supportive care; most cases resolve spontaneously<ref name="livertox"/> | |||
*GI consultation for severe hepatic injury (bilirubin >20 mg/dL, coagulopathy, or signs of [[acute liver failure]]) | |||
*Corticosteroids and [[NAC]] have been used in case reports but efficacy is unproven<ref name="livertox"/> | |||
===Drug Interactions=== | |||
*Be aware that mitragynine inhibits CYP3A4 and CYP2D6<ref name="tanna"/> | |||
*Potential to increase levels of co-ingested medications metabolized by these pathways (e.g., [[benzodiazepines]], [[methadone]], certain [[antipsychotics]], [[SSRIs]]) | |||
*Polydrug exposure is common and may significantly increase morbidity and mortality | |||
==Disposition== | ==Disposition== | ||
*Discharge | *Discharge if: | ||
**Mild symptoms (nausea, mild stimulant effects) that resolve with observation and supportive care | |||
**Normal vital signs and mental status at time of disposition | |||
**Able to tolerate PO | |||
*Observation / Admission if: | |||
**Required naloxone for respiratory depression (observe ≥24 hours given risk of rebound respiratory depression)<ref name="greatimitator"/> | |||
**Persistent [[altered mental status]] | |||
**[[Seizure]] | |||
**Concern for [[rhabdomyolysis]] or [[acute kidney injury]] | |||
**Elevated [[LFTs]] or signs of hepatotoxicity | |||
**Hemodynamic instability | |||
**Significant co-ingestion | |||
*ICU admission for: | |||
**Respiratory failure / need for [[intubation]] | |||
**Refractory [[seizures]] | |||
**[[Acute liver failure]] | |||
**Hemodynamic instability requiring vasopressors | |||
*For all patients: provide counseling on risks of kratom, advise cessation, and consider referral to addiction medicine if regular use or dependence is identified | |||
*Provide [[naloxone]] prescription at discharge if ongoing use is anticipated | |||
==See Also== | ==See Also== | ||
*[[Opioids]] | *[[Opioids]] | ||
*[[Opioid toxicity]] | |||
*[[Opioid withdrawal]] | |||
*[[Buprenorphine]] | |||
*[[Tianeptine toxicity]] | |||
==External Links== | ==External Links== | ||
*[https://www.fda.gov/news-events/public-health-focus/fda-and-kratom FDA and Kratom] | |||
*[https://www.ncbi.nlm.nih.gov/books/NBK548231/ LiverTox — Kratom] | |||
*[https://www.ncbi.nlm.nih.gov/books/NBK585120/ StatPearls — Kratom Toxicity] | |||
*[https://www.poison.org/articles/kratom National Poison Control — Kratom] | |||
==References== | ==References== | ||
{{reflist|2}} | |||
[[Category:Toxicology]] | [[Category:Toxicology]] | ||
Revisión actual - 09:30 22 mar 2026
Background
- Derived from Mitragyna speciosa, a tropical evergreen tree in the coffee family native to Southeast Asia
- Leaves contain over 40 alkaloids; the two most clinically relevant are:
- Both alkaloids exhibit G-protein biased agonism at mu-opioid receptors with limited beta-arrestin recruitment (theoretically less respiratory depression than classical opioids, though still reported)[1]
- Additional receptor activity at alpha-1A, alpha-2A, 5-HT1A, 5-HT2A, D1, and D2 receptors contributes to mixed stimulant-opioid clinical picture[2]
- Mitragynine is metabolized by CYP3A4 to 7-hydroxymitragynine (a more potent metabolite) and inhibits CYP2D6 and CYP3A4, creating significant potential for drug-drug interactions[3]
- Available in the US as powder, capsules, tablets, extracts, and liquid "shots" sold at gas stations, smoke shops, and online
- Products are unregulated, with highly variable alkaloid content and potential for contamination (Salmonella, heavy metals including lead)[4]
- Estimated 1.7 million Americans aged ≥12 used kratom in 2021[4]
- Not FDA-approved for any indication; not a legal dietary supplement or food additive[4]
- Federally unscheduled but banned in several states (Alabama, Arkansas, Indiana, Vermont, Wisconsin, Louisiana); regulated in many others[5]
- Patients commonly use for self-treatment of chronic pain, opioid withdrawal, depression, and anxiety
- Approximately one-third of users co-ingest with other substances[6]
Clinical Features
- Effects are dose-dependent and may mimic both opioid and stimulant toxicity
- Onset of effects typically within 10-20 minutes of ingestion; duration 2-5 hours
Low-Dose Effects (<5 g)
- Stimulant effects predominate
- Increased alertness and energy
- Tachycardia, hypertension
- Agitation, jitteriness
- Decreased appetite
High-Dose Effects (>5 g)
- Opioid-like sedation predominates
- Miosis
- Respiratory depression (especially with co-ingestions or concentrated extracts)
- Drowsiness, altered mental status
- Nausea, vomiting
- Constipation
Severe/Complicated Presentations
- Seizures[7]
- Respiratory failure requiring intubation
- Rhabdomyolysis and acute kidney injury[8]
- Hepatotoxicity — typically cholestatic pattern, onset 1-8 weeks of regular use; can be severe (bilirubin >20 mg/dL); usually reversible with cessation[9]
- Cardiac arrest (rare, primarily in polydrug exposure)[10]
- QT prolongation (theoretical and case-reported)
Kratom Withdrawal
- Occurs with chronic use; onset typically within 12-24 hours of last dose[8]
- Resembles mild-moderate opioid withdrawal: myalgias, rhinorrhea, diaphoresis, insomnia, irritability, nausea, diarrhea
- Generally less severe than traditional opioid withdrawal
- Can be scored using the Clinical Opiate Withdrawal Scale (COWS)
Differential Diagnosis
- Opioid toxicity
- Opioid withdrawal
- Sympathomimetic toxicity
- Anticholinergic toxicity
- Serotonin syndrome (due to serotonergic activity)
- Tianeptine toxicity (similar presentation, also sold at gas stations)
- Xylazine toxicity
- Phenibut toxicity
Drugs of abuse
- 25C-NBOMe
- Alcohol
- Amphetamines
- Bath salts
- Cocaine
- Difluoroethane
- Ecstasy
- Gamma hydroxybutyrate (GHB)
- Heroin
- Inhalant abuse
- Hydrocarbon toxicity
- Difluoroethane (electronics duster)
- Marijuana
- Kratom
- Phencyclidine (PCP)
- Psilocybin ("magic mushrooms")
- Synthetic cannabinoids
- Chloral hydrate
- Body packing
Evaluation
- Primarily a clinical diagnosis — ask specifically about kratom, herbal supplements, and "gas station" products
- Kratom does NOT appear on standard urine drug screens[7]
- May cause false-negative opioid screen despite opioid-like presentation
- Specialized testing for mitragynine exists but is not widely available and generally not clinically useful in the acute setting
- Consider early consultation with Poison control (1-800-222-1222)
Labs
- Not routinely required for mild presentations
- For moderate-severe presentations, consider:
- CBC, BMP/CMP
- LFTs — particularly if chronic use or concern for hepatotoxicity
- CK if agitated, seizing, or prolonged immobilization (rhabdomyolysis)
- Lactate, VBG
- Acetaminophen and salicylate levels, ethanol level to rule out co-ingestion
- Urine drug screen — will be negative for kratom, but useful to evaluate for co-ingestions
- Coagulation studies if hepatotoxicity suspected
ECG
- Obtain EKG in moderate-severe presentations
- Evaluate for tachycardia, QT prolongation
Management
- Focus on ABCs and symptom-directed treatment
- Consider early Poison control consultation (1-800-222-1222)
Respiratory Depression
- Supplemental oxygen, BVM ventilation as needed
- Naloxone — effective for kratom-induced respiratory depression due to mu-opioid agonism[11]
- Standard dosing as per opioid toxicity protocols
- Be aware of potential for rebound respiratory depression within 24 hours per poison control center reports[11]
Agitation / Sympathomimetic Features
- Benzodiazepines for hyperarousal, agitation, tachycardia, hypertension, and seizures
- IV fluids
- Avoid haloperidol if concern for QT prolongation
Seizures
- Benzodiazepines are first-line
- Standard seizure management algorithm
Kratom Withdrawal
- Symptom-directed treatment similar to opioid withdrawal:
- NSAIDs for myalgias
- Antiemetics (e.g., ondansetron) for nausea/vomiting
- Loperamide for diarrhea
- Clonidine for autonomic symptoms
- IV fluids for dehydration
- Medication-assisted treatment for opioid use disorder:
- Buprenorphine — most commonly reported for kratom withdrawal/dependence; can be initiated in the ED per standard protocols[6]
- Methadone — alternative for patients not candidates for buprenorphine
Hepatotoxicity
- Discontinue kratom
- Supportive care; most cases resolve spontaneously[9]
- GI consultation for severe hepatic injury (bilirubin >20 mg/dL, coagulopathy, or signs of acute liver failure)
- Corticosteroids and NAC have been used in case reports but efficacy is unproven[9]
Drug Interactions
- Be aware that mitragynine inhibits CYP3A4 and CYP2D6[3]
- Potential to increase levels of co-ingested medications metabolized by these pathways (e.g., benzodiazepines, methadone, certain antipsychotics, SSRIs)
- Polydrug exposure is common and may significantly increase morbidity and mortality
Disposition
- Discharge if:
- Mild symptoms (nausea, mild stimulant effects) that resolve with observation and supportive care
- Normal vital signs and mental status at time of disposition
- Able to tolerate PO
- Observation / Admission if:
- Required naloxone for respiratory depression (observe ≥24 hours given risk of rebound respiratory depression)[11]
- Persistent altered mental status
- Seizure
- Concern for rhabdomyolysis or acute kidney injury
- Elevated LFTs or signs of hepatotoxicity
- Hemodynamic instability
- Significant co-ingestion
- ICU admission for:
- Respiratory failure / need for intubation
- Refractory seizures
- Acute liver failure
- Hemodynamic instability requiring vasopressors
- For all patients: provide counseling on risks of kratom, advise cessation, and consider referral to addiction medicine if regular use or dependence is identified
- Provide naloxone prescription at discharge if ongoing use is anticipated
See Also
External Links
References
- ↑ 1.0 1.1 1.2 Kruegel AC, Grundmann O. The medicinal chemistry and neuropharmacology of kratom: A preliminary discussion of a promising medicinal plant and analysis of its potential for abuse. Neuropharmacology. 2018;134(Pt A):108-120.
- ↑ Yusof SR, Zakaria Z, Amir Rawa MS, et al. Kratom Alkaloids: Interactions With Enzymes, Receptors, and Cellular Barriers. Front Pharmacol. 2021;12:751656.
- ↑ 3.0 3.1 Tanna RS, Tian DD, Cech NB, et al. Refined Prediction of Pharmacokinetic Kratom-Drug Interactions: Time-Dependent Inhibition Considerations. J Pharmacol Exp Ther. 2021;376(1):64-73.
- ↑ 4.0 4.1 4.2 U.S. Food and Drug Administration. FDA and Kratom. Updated February 2024. https://www.fda.gov/news-events/public-health-focus/fda-and-kratom
- ↑ Congressional Research Service. Kratom Regulation: Federal Status and State Approaches. LSB11082. 2024.
- ↑ 6.0 6.1 Washington Poison Center. Kratom and 7-hydroxymitragynine poisoning. 2025. https://www.wapc.org/data/data-blogs/kratom-and-7-hydroxymitragynine-poisoning/
- ↑ 7.0 7.1 Eastlack SC, Cornett EM, Kaye AD. Kratom—Pharmacology, Clinical Implications, and Outlook: A Comprehensive Review. Pain Ther. 2020;9(1):55-69.
- ↑ 8.0 8.1 Narrative Review of Kratom in the Emergency Department. Auctores. 2025.
- ↑ 9.0 9.1 9.2 LiverTox: Clinical and Research Information on Drug-Induced Liver Injury. Kratom. National Institute of Diabetes and Digestive and Kidney Diseases; 2020.
- ↑ Poison Control. What is kratom? https://www.poison.org/articles/kratom
- ↑ 11.0 11.1 11.2 Mikkelsen A, Van Roekel C, Grande EJ, et al. The Great Imitator: A Case of Accidental Kratom Overdose. Cureus. 2023;15(7):e42497.