Valproate Toxicity

Earn CME/CE in your profession:

Free Review Questions

Continuing Education Activity

Valproate toxicity results from an excessive accumulation of valproic acid in the body, often triggered by factors like high dosages, rapid dose adjustments, or interactions with other medications. Symptoms vary widely, including gastrointestinal distress symptoms such as nausea and vomiting, neurological manifestations like drowsiness, confusion, and, in severe cases, coma or fatality. Timely identification of risk factors and early symptom recognition is pivotal for intervening and mitigating adverse consequences. Treatment strategies involve a multifaceted approach, including supportive care to manage symptoms and specific interventions like L-carnitine therapy or hemodialysis to remove excess valproic acid from the bloodstream.

Through this course, participants better understand valproate toxicity comprehensively, including proficient identification of risk factors, thorough patient assessment techniques, and implementing appropriate diagnostic and therapeutic measures. Additionally, collaborating with an interprofessional team is emphasized, as this enhances patient outcomes significantly by facilitating seamless communication and coordination across various healthcare disciplines. By leveraging the expertise and resources of diverse specialists, patient care is optimized, ensuring timely and targeted interventions that improve safety and clinical effectiveness.

Objectives:

  • Screen patients for valproate toxicity, particularly hypoalbuminemic individuals or those exhibiting persistent symptoms despite normal total valproate levels.

  • Implement appropriate diagnostic and therapeutic measures for patients suspected of valproate toxicity, such as obtaining unbound valproate levels and initiating L-carnitine therapy or hemodialysis when indicated.

  • Differentiate between symptoms of valproate toxicity and other medical conditions to facilitate accurate diagnosis and timely intervention.

  • Collaborate with interprofessional teams to ensure comprehensive patient care, leveraging expertise from various specialties to optimize outcomes.

Introduction

The valproate ion is the therapeutically active substance in valproic acid, sodium valproate, and divalproex.[1] Valproate is commonly used for generalized and partial seizures, bipolar disorders, schizoaffective disorders, neuropathic pain, and migraine prophylaxis.[2] Valproate toxicity can occur accidentally and intentionally. Toxicity is most likely to occur with dose ramping, in hypoalbuminemia, from drug-drug interactions, or in attempts to cause self-harm. 

Patients with acute valproate overdose typically experience hyperammonemia, encephalopathy, and hepatotoxicity. Symptoms consistent with severe valproate overdose include hypotension, tachycardia, respiratory depression, metabolic acidosis, cerebral edema, and valproate-related hyperammonemic encephalopathy.

Etiology

Valproate toxicity commonly occurs when ramping up the dose to achieve a therapeutic effect. Valproate toxicity may also occur when free or unbound drug levels become elevated. Elevated free drug concentrations are common in older patients and patients with hypoalbuminemia, and also in those who are pregnant, have renal dysfunction, liver disease, or in those who use medications that compete with valproate for albumin binding sites.[3] Additionally, patients who intentionally overdose on valproate during attempts of self harm experience varying degrees of valproate toxicity.[4]

Epidemiology

According to the American Association of Poison Control Centers' National Poison Data System, cases of acute ingestion of valproate increased from 2717 in 1994 to 8705 in 2005.[5] More recently, cases of acute ingestion of valproate cases have stabilized. There were 3211 cases of acute valproate ingestion in 2010 and 2996 cases in 2018.[6] Children may be at particular risk for valproate toxicity, though it can occur in patients of all ages.[7]

Pathophysiology

Patients with valproate toxicity commonly experience hyperammonemia, encephalopathy, and hepatotoxicity.[8] Valproate decreases tissue carnitine levels, which results in microvesicular steatosis and hyperammonemia.[9][10] Valproate-induced encephalopathy is typically related to the effects of hyperammonemia. However, valproate-induced cerebral edema may also be impacted by altered valproate metabolism, which allows the presence of toxic drug metabolites to enter the brain.[8][11] Valproate-induced hepatotoxicity is likely due to inhibiting beta-oxidation of fatty acids, which results in mitochondrial injury.

Toxicokinetics

In the United States, oral valproate formulations include valproic acid, sodium valproate, and divalproex. Valproic acid and sodium valproate are immediate-release formulations, while divalproex is formulated as delayed- or extended-release. Valproate is also formulated for intravenous use as sodium valproate.[12] The liver metabolizes valproate primarily through glucuronide conjugation and beta-oxidation. The average elimination half-life of valproate is approximately 11 hours.[13] However, the elimination half-life of valproate can increase to 30 or more hours in the setting of acute overdose despite elimination via first-order kinetics.[14] In the setting of valproate toxicity, a greater degree of omega-oxidation occurs in the liver, which increases the risk of hepatotoxicity, cerebral edema, and hyperammonemia.[11] Cytochrome P (CYP)2C9 and CYP2A6 enzymes also play a role in valproate metabolism. Results from a recently published meta-analysis showed that patients with CYP2C9*3 and CYP2A6*4 genotype variants had higher serum valproate concentrations than patients without.[15]

Very little valproate is excreted in the urine as an unchanged drug. Aspirin increases free serum valproate levels by competing for plasma protein binding sites. Hypoalbuminemia, a condition common in patients who are older and in those with liver disease, also increases free serum valproate levels. Because total valproate serum levels may remain constant despite alterations in protein binding, measuring free or unbound serum levels is best practice in the setting of valproate toxicity.[16]

History and Physical

When assessing a patient with suspected valproate toxicity, clinicians should ascertain the specific time of valproate ingestion, valproate formulation, the amount of valproate ingested, other possible coingestants (eg, acetaminophen or alcohol), and a list of all of the patient's prior psychiatric or medical problems. Patients with acute ingestion of 200 mg/kg of valproate or serum valproate concentrations of 180 mg/L or greater often experience central nervous system dysfunction. Manifestations of central nervous system dysfunction include tremors, agitation, miosis, and other focal neurological deficits. Patients who experience valproate-related hyperammonemic encephalopathy may experience confusion, seizures, and lethargy, which can progress to stupor, coma, and death.[17][18] Additionally, patients with valproate toxicity may experience respiratory depression, hypotension, and tachycardia. Gastrointestinal symptoms consistent with valproate toxicity include vomiting, diarrhea, and abdominal pain.[11] 

Interestingly, the dermatohistopathology of valproate toxicity has been consistent with cases of hypersensitivity vasculitis and psoriasiform eruption. Patients on chronic valproate therapy may also exhibit symptoms consistent with alopecia due to telogen effluvium, including diffuse hair loss, thinning, and graying.[19] Valproate is also a potential teratogen. Fetal exposure to valproate during pregnancy can result in a wide range of congenital malformations, including spina bifida, anencephaly, craniofacial abnormalities, and genitourinary defects.[20]

Evaluation

Therapeutic serum concentrations of valproate usually range from 50 to 100 mg/L. Valproate levels should be obtained every 2 to 4 hours for patients with suspected valproate toxicity and until the serum valproate level starts declining. A steady decline in the level suggests a peak serum level has been reached.[21] Unbound valproate levels are an assessment tool in patients who are hypoalbuminemic, or when signs of valproate toxicity are present despite low or normal total valproate levels.[16]

Other important laboratory tests to order for patients with suspected valproate toxicity include a complete blood count with differential. If the patient is experiencing valproate toxicity, thrombocytopenia, and decreased granulocyte counts may be present. Additionally, a comprehensive metabolic panel is helpful to assess the patient for hypoglycemia, hepatotoxicity, electrolyte abnormalities, and acid-base disorders. Blood ammonia levels should be studied for patients experiencing encephalopathy. Toxicologic screening for coingestants, including other anticonvulsants, aspirin, and acetaminophen should also considered. A pregnancy test should be ordered for women of childbearing age.[21]

Other tests to consider include a 12-lead echocardiogram that shows an atrioventricular conduction block.[22] Sometimes, severe valproate toxicity is associated with atrial tachycardia.[23] A computed tomography scan of the head is necessary when patients present with signs of focal neurological deficits, profound central nervous system depression, or suspicion of cerebral edema.[19]

Treatment / Management

Initial therapy for patients with valproate toxicity should focus on medical stabilization and resuscitation. Specifically, initial interventions should focus on maintaining the airway, breathing, and circulation. Patients with severe respiratory depression may require endotracheal intubation and mechanical ventilation. Intravenous access may be needed to provide intravenous fluid and vasopressors for patients presenting with hypotension. Benzodiazepines should be administered if there is a seizure due to valproate toxicity.[24] 

Other interventions to consider early for patients with valproate toxicity are gastrointestinal decontamination and lavage. If the patient presents within 2 hours of a valproate overdose, activated charcoal may be used for gastrointestinal decontamination. Valproate is available in enteric-coated and extended-release formulations, which have slow absorption. Administration of activated charcoal may be considered beyond 2 hours from ingestion for patients who have taken enteric-coated and extended-release valproate formulations.[25] The dose of activated charcoal is 1 g/kg of body weight. If the patient cannot swallow reliably, the administration of activated charcoal should be withheld. Gastric lavage may also be considered to eliminate valproate from the digestive tract. Food and Drug Administration guidelines indicate that gastric lavage treatment may be effective up to 10 or 12 hours after drug intake.[26] 

After initial stabilization, it is prudent to consider the use of L-carnitine for patients presenting with an acute overdose of valproate and altered mental status. L-carnitine should be administered intravenously with a loading dose of 100 mg/kg, followed by 50 mg/kg intravenously every 8 hours. Serum ammonia levels should be simultaneously measured, and when serum ammonia levels start decreasing, L-carnitine therapy can be discontinued.[27] In the pediatric population, resulting evidence from a few case reports shows that carnitine may alter the generation of potentially toxic metabolites, but it may not translate into improved clinical prognosis.[28] Interestingly, the mu-opioid receptor antagonist naloxone may reverse the central nervous system depression in some cases of valproate poisoning.[29][30] Naloxone may also be useful for chronic valproate intoxication.[31]

Hemodialysis is indicated for serum valproate concentrations greater than 1300 mg/L and in patients experiencing shock or cerebral edema. Hemodialysis can greatly reduce the elimination half-life of valproate. In one case study, hemodialysis decreased the half-life of valproate from 13 hours to 1.7 hours. Additionally, hemodialysis contributed to significant clinical improvement for the patient within 4 hours of treatment. Intermittent hemodialysis is the preferred technique for patients experiencing valproate toxicity, although continuous renal replacement therapy is an acceptable alternative if the patient cannot tolerate intermittent hemodialysis. Hemodialysis treatment can be discontinued if the serum valproate concentration drops below 100 mg/L and the patient shows signs of clinical improvement, including normotension, improved mental status, pH normalization, and resolution of electrolyte abnormalities.[32]

Differential Diagnosis

Symptoms of valproate toxicity overlap with many conditions. Thus, a detailed history, physical examination, laboratory evaluation, and cerebral imaging are required to diagnose valproate toxicity.[33] The most common symptoms of valproate toxicity are altered mental status and central nervous system depression, which can be due to a wide range of conditions. Suspicion of meningitis should arise when a patient presents with fever and neck stiffness accompanied by altered mental status. 

Herpes simplex virus-1 encephalitis typically shows temporal lobe involvement in magnetic resonance images. Additionally, cranial neoplasm, intracranial hemorrhage, hydrocephalus, and traumatic brain injury should be ruled out as the cause of these symptoms. Valproate-induced tremors occur in about 10% of patients and require differentiation from essential tremors or tremors associated with Parkinson disease. 

A comprehensive metabolic panel should be ordered to search for metabolic derangements, including hypoglycemia and hypernatremia. As serum ammonia is frequently elevated with valproate poisoning, disorders of urea cycle disorders and hepatic encephalopathy should merit consideration. Finally, other causes of anion gap metabolic acidosis should be investigated. Common causes of anion gap metabolic acidosis include uremia, methanol poisoning, diabetic ketoacidosis, and lactic acidosis.

Prognosis

The prognosis for patients with valproate toxicity will depend on the total amount of valproate ingested, the opportunity to implement decontamination and elimination strategies, and the supportive care given. Severe ingestions may resolve without any sequelae after aggressive decontamination, elimination, and adequate supportive caIn one observational, retrospective study involving 316 patients, the prognosis of patients with acute valproate toxicity was good with supportive care alone. According to the multivariate analysis within the study, a coma during the initial presentation was associated with a poor prognosis. Other poor prognostic factors include advanced age, metabolic derangements, and ingesting large amounts of valproate.[34]

Complications

Acute valproate toxicity can result in dose-related and reversible hepatotoxicity. Usually, ceasing the drug therapy results in the normalization of liver function abnormalities, but fulminant hepatic failure and death have been reported with valproate toxicity.[35][36] Concerningly, liver transplants in children with valproate-induced acute hepatic failure have reduced survival rates compared to liver transplants from other causes of drug-induced liver injury.[37] Cerebral edema may lead to herniation, prolonged central nervous system depression, and coma.[11][14] Valproate-related hyperammonemic encephalopathy can lead to confusion, lethargy, and increased seizure frequency. If severe valproate toxicity is untreated, death may result.[38][39]

Consultations

A poison control center should always be consulted when a patient presents with valproate toxicity. Contact with a poison control center is critical when the diagnosis of valproate toxicity is unclear or if the patient is critically ill. A nephrology consultation and consideration for hemodialysis is recommended when valproate toxicity is accompanied by cerebral edema or shock or if the serum valproate concentration is more than 1300 mg/L.[32] All patients with intentional valproate overdose also require consultation with a psychiatrist.

Deterrence and Patient Education

On discharge, the patient should receive counsel that liver problems can happen with valproate overdose, which can be fatal. Parents need to know that children under 2 years old are at higher risk of deadly liver problems, including Alpers–Huttenlocher syndrome.[37] Pregnant women should be educated that valproate may cause severe congenital disabilities, including spina bifida and neurodevelopmental disorders, and that contraception should be used if women are sexually active while taking valproate.[20] Patients should also be informed of the risk of pancreatitis with long-term therapy. Specifically, patients should be advised to immediately contact their clinician or an emergency department if they develop symptoms such as acute abdominal pain, nausea, vomiting, or fever.[40]

Enhancing Healthcare Team Outcomes

To improve patient-centered care and outcomes related to valproate toxicity, physicians, advanced practice providers, nurses, pharmacists, and other health professionals must develop comprehensive skills and strategies. Physicians and advanced practice providers should identify risk factors, apply their expertise in assessing patients for signs of overdose, implement appropriate interventions, and coordinate multidisciplinary care.

Nurses are crucial in monitoring patients and providing supportive care during stabilization and resuscitation. Pharmacists should ensure accurate medication management and dosing adjustments. Effective interprofessional communication among team members is essential for sharing critical information, interpreting laboratory results, and making timely decisions regarding treatment modalities like L-carnitine and hemodialysis. Care coordination efforts should prioritize patient safety and optimize team performance, ultimately improving outcomes for patients experiencing valproate toxicity.

Details

Author

Ashish R. Patel

Editor:

Shivaraj Nagalli

Updated:

5/6/2024 12:55:35 AM

Feedback:

Send Us Your Comments

References

[1]

Delage C, Palayer M, Etain B, Hagenimana M, Blaise N, Smati J, Chouchana M, Bloch V, Besson VC. Valproate, divalproex, valpromide: Are the differences in indications justified? Biomedicine & pharmacotherapy = Biomedecine & pharmacotherapie. 2023 Feb:158():114051. doi: 10.1016/j.biopha.2022.114051. Epub 2022 Dec 13     [PubMed PMID: 36521249]

[2]

Löscher W. Basic pharmacology of valproate: a review after 35 years of clinical use for the treatment of epilepsy. CNS drugs. 2002:16(10):669-94     [PubMed PMID: 12269861]

[3]

Smits JEMP, Wallenburg E, van Spanje A, van Luin M, Marijnissen RM. Valproate Intoxication in a Patient With Blood Valproate Levels Within Therapeutic Range. The Journal of clinical psychiatry. 2017 Apr:78(4):e413-e414. doi: 10.4088/JCP.15cr10147. Epub     [PubMed PMID: 28448701]

[4]

Ferrey AE, Geulayov G, Casey D, Wells C, Fuller A, Bankhead C, Ness J, Clements C, Gunnell D, Kapur N, Hawton K. Relative toxicity of mood stabilisers and antipsychotics: case fatality and fatal toxicity associated with self-poisoning. BMC psychiatry. 2018 Dec 27:18(1):399. doi: 10.1186/s12888-018-1993-3. Epub 2018 Dec 27     [PubMed PMID: 30587176]

Level 3 (low-level) evidence

[5]

Bronstein AC, Spyker DA, Cantilena LR Jr, Green JL, Rumack BH, Dart RC. 2010 Annual Report of the American Association of Poison Control Centers' National Poison Data System (NPDS): 28th Annual Report. Clinical toxicology (Philadelphia, Pa.). 2011 Dec:49(10):910-41. doi: 10.3109/15563650.2011.635149. Epub     [PubMed PMID: 22165864]

[6]

Gummin DD, Mowry JB, Spyker DA, Brooks DE, Beuhler MC, Rivers LJ, Hashem HA, Ryan ML. 2018 Annual Report of the American Association of Poison Control Centers' National Poison Data System (NPDS): 36th Annual Report. Clinical toxicology (Philadelphia, Pa.). 2019 Dec:57(12):1220-1413. doi: 10.1080/15563650.2019.1677022. Epub 2019 Nov 21     [PubMed PMID: 31752545]

[7]

Powell-Jackson PR, Tredger JM, Williams R. Hepatotoxicity to sodium valproate: a review. Gut. 1984 Jun:25(6):673-81     [PubMed PMID: 6428980]

[8]

Rupasinghe J, Jasinarachchi M. Progressive encephalopathy with cerebral oedema and infarctions associated with valproate and diazepam overdose. Journal of clinical neuroscience : official journal of the Neurosurgical Society of Australasia. 2011 May:18(5):710-1. doi: 10.1016/j.jocn.2010.08.022. Epub 2011 Feb 23     [PubMed PMID: 21349718]

[9]

. Valproate. LiverTox: Clinical and Research Information on Drug-Induced Liver Injury. 2012:():     [PubMed PMID: 31643607]

[10]

Schumacher JD, Guo GL. Mechanistic review of drug-induced steatohepatitis. Toxicology and applied pharmacology. 2015 Nov 15:289(1):40-7. doi: 10.1016/j.taap.2015.08.022. Epub 2015 Sep 5     [PubMed PMID: 26344000]

[11]

Dupuis RE, Lichtman SN, Pollack GM. Acute valproic acid overdose. Clinical course and pharmacokinetic disposition of valproic acid and metabolites. Drug safety. 1990 Jan-Feb:5(1):65-71     [PubMed PMID: 2106903]

[12]

Citrome L. Valproate: do formulations matter? Journal of clinical pharmacy and therapeutics. 2008 Aug:33(4):457; author reply 458. doi: 10.1111/j.1365-2710.2008.00919_1.x. Epub     [PubMed PMID: 18613865]

[13]

Chadwick DW. Concentration-effect relationships of valproic acid. Clinical pharmacokinetics. 1985 Mar-Apr:10(2):155-63     [PubMed PMID: 3922659]

[14]

Gram L, Bentsen KD. Valproate: an updated review. Acta neurologica Scandinavica. 1985 Aug:72(2):129-39     [PubMed PMID: 2931939]

[15]

Yoon HY, Ahn MH, Yee J, Lee N, Han JM, Gwak HS. Influence of CYP2C9 and CYP2A6 on plasma concentrations of valproic acid: a meta-analysis. European journal of clinical pharmacology. 2020 Aug:76(8):1053-1058. doi: 10.1007/s00228-020-02872-6. Epub 2020 May 8     [PubMed PMID: 32385545]

Level 1 (high-level) evidence

[16]

Doré M, San Juan AE, Frenette AJ, Williamson D. Clinical Importance of Monitoring Unbound Valproic Acid Concentration in Patients with Hypoalbuminemia. Pharmacotherapy. 2017 Aug:37(8):900-907. doi: 10.1002/phar.1965. Epub 2017 Jul 18     [PubMed PMID: 28574586]

[17]

Khoo SH, Leyland MJ. Cerebral edema following acute sodium valproate overdose. Journal of toxicology. Clinical toxicology. 1992:30(2):209-14     [PubMed PMID: 1588670]

[18]

Dealberto MJ. Valproate-induced hyperammonaemic encephalopathy: review of 14 cases in the psychiatric setting. International clinical psychopharmacology. 2007 Nov:22(6):330-7     [PubMed PMID: 17917551]

Level 3 (low-level) evidence

[19]

Chateauvieux S, Morceau F, Dicato M, Diederich M. Molecular and therapeutic potential and toxicity of valproic acid. Journal of biomedicine & biotechnology. 2010:2010():. pii: 479364. doi: 10.1155/2010/479364. Epub 2010 Jul 29     [PubMed PMID: 20798865]

[20]

Alsdorf R, Wyszynski DF. Teratogenicity of sodium valproate. Expert opinion on drug safety. 2005 Mar:4(2):345-53     [PubMed PMID: 15794725]

Level 3 (low-level) evidence

[21]

Mortensen PB, Hansen HE, Pedersen B, Hartmann-Andersen F, Husted SE. Acute valproate intoxication: biochemical investigations and hemodialysis treatment. International journal of clinical pharmacology, therapy, and toxicology. 1983 Feb:21(2):64-8     [PubMed PMID: 6404845]

[22]

Davutoglu V, Neyal M, Altunbas G. Valproic Acid as a Cause of Transient Atrio-Ventricular Conduction Block Episodes. Journal of atrial fibrillation. 2017 Feb-Mar:9(5):1520. doi: 10.4022/jafib.1520. Epub 2017 Feb 28     [PubMed PMID: 29250271]

[23]

Meyer S, Kuhlmann MK, Peters FT, Limbach HG, Lindinger A. Severe valproic acid intoxication is associated with atrial tachycardia: secondary detoxication by hemoperfusion. Klinische Padiatrie. 2005 Mar-Apr:217(2):82-5     [PubMed PMID: 15770579]

[24]

Sztajnkrycer MD. Valproic acid toxicity: overview and management. Journal of toxicology. Clinical toxicology. 2002:40(6):789-801     [PubMed PMID: 12475192]

Level 3 (low-level) evidence

[25]

Graudins A, Aaron CK. Delayed peak serum valproic acid in massive divalproex overdose--treatment with charcoal hemoperfusion. Journal of toxicology. Clinical toxicology. 1996:34(3):335-41     [PubMed PMID: 8667473]

[26]

Liu R, Xiao L, Hu Y, Yan Q, Liu X. Rescue strategies for valproic acid overdose poisoning: Case series and literature review. Clinical case reports. 2024 Jan:12(1):e8367. doi: 10.1002/ccr3.8367. Epub 2023 Dec 27     [PubMed PMID: 38161627]

Level 2 (mid-level) evidence

[27]

Perrott J, Murphy NG, Zed PJ. L-carnitine for acute valproic acid overdose: a systematic review of published cases. The Annals of pharmacotherapy. 2010 Jul-Aug:44(7-8):1287-93. doi: 10.1345/aph.1P135. Epub 2010 Jun 29     [PubMed PMID: 20587742]

Level 3 (low-level) evidence

[28]

Russell S. Carnitine as an antidote for acute valproate toxicity in children. Current opinion in pediatrics. 2007 Apr:19(2):206-10     [PubMed PMID: 17496767]

Level 3 (low-level) evidence

[29]

Alberto G, Erickson T, Popiel R, Narayanan M, Hryhorczuk D. Central nervous system manifestations of a valproic acid overdose responsive to naloxone. Annals of emergency medicine. 1989 Aug:18(8):889-91     [PubMed PMID: 2502939]

[30]

Montero FJ. Naloxone in the reversal of coma induced by sodium valproate. Annals of emergency medicine. 1999 Mar:33(3):357-8     [PubMed PMID: 10036355]

[31]

Thanacoody HK. Chronic valproic acid intoxication: reversal by naloxone. Emergency medicine journal : EMJ. 2007 Sep:24(9):677-8     [PubMed PMID: 17711961]

[32]

Ghannoum M, Laliberté M, Nolin TD, MacTier R, Lavergne V, Hoffman RS, Gosselin S, EXTRIP Workgroup. Extracorporeal treatment for valproic acid poisoning: systematic review and recommendations from the EXTRIP workgroup. Clinical toxicology (Philadelphia, Pa.). 2015 Jun:53(5):454-65. doi: 10.3109/15563650.2015.1035441. Epub     [PubMed PMID: 25950372]

Level 1 (high-level) evidence

[33]

Murty S. Antiepileptic Overdose. Indian journal of critical care medicine : peer-reviewed, official publication of Indian Society of Critical Care Medicine. 2019 Dec:23(Suppl 4):S290-S295. doi: 10.5005/jp-journals-10071-23301. Epub     [PubMed PMID: 32021007]

[34]

Shadnia S, Amiri H, Hassanian-Moghaddam H, Rezai M, Vasei Z, Ghodrati N, Zamani N. Favorable results after conservative management of 316 valproate intoxicated patients. Journal of research in medical sciences : the official journal of Isfahan University of Medical Sciences. 2015 Jul:20(7):656-61. doi: 10.4103/1735-1995.166211. Epub     [PubMed PMID: 26622254]

[35]

Bryant AE 3rd, Dreifuss FE. Valproic acid hepatic fatalities. III. U.S. experience since 1986. Neurology. 1996 Feb:46(2):465-9     [PubMed PMID: 8614514]

[36]

Star K, Edwards IR, Choonara I. Valproic acid and fatalities in children: a review of individual case safety reports in VigiBase. PloS one. 2014:9(10):e108970. doi: 10.1371/journal.pone.0108970. Epub 2014 Oct 10     [PubMed PMID: 25302991]

Level 3 (low-level) evidence

[37]

Mindikoglu AL, King D, Magder LS, Ozolek JA, Mazariegos GV, Shneider BL. Valproic acid-associated acute liver failure in children: case report and analysis of liver transplantation outcomes in the United States. The Journal of pediatrics. 2011 May:158(5):802-7. doi: 10.1016/j.jpeds.2010.10.033. Epub 2010 Dec 16     [PubMed PMID: 21167499]

Level 3 (low-level) evidence

[38]

Verrotti A, Trotta D, Morgese G, Chiarelli F. Valproate-induced hyperammonemic encephalopathy. Metabolic brain disease. 2002 Dec:17(4):367-73     [PubMed PMID: 12602513]

[39]

Duarte J, Macias S, Coria F, Fernandez E, Clavería LE. Valproate-induced coma: case report and literature review. The Annals of pharmacotherapy. 1993 May:27(5):582-3     [PubMed PMID: 8347908]

Level 3 (low-level) evidence

[40]

Perucca E. Pharmacological and therapeutic properties of valproate: a summary after 35 years of clinical experience. CNS drugs. 2002:16(10):695-714     [PubMed PMID: 12269862]