4-Methylpyrazole protects against acetaminophen hepatotoxicity in mice and in primary human hepatocytes

Akakpo, Jephte Y.; Ramachandran, Anup; Kandel, Sylvie E.; Ni, Hong‐Min; Kumer, Sean C.; Rumack, Barry H.; Jaeschke, Hartmut

doi:10.1177/0960327118774902

Cited by 82 publications

(75 citation statements)

References 51 publications

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“…Recently, 4methylpyrazole (Fomepizole), an antidote against methanol poisoning, has been shown to be highly effective against APAP-induced liver injury by inhibiting P450 enzyme when given early in mice and human hepato-cytes 180 or by inhibiting of JNK activation when administered after the drug metabolism phase. 181 In addition, metformin, a first-line drug to treat type 2 diabetes mellitus, substantially attenuated APAP hepatotoxicity 57,182 mainly by inhibiting complex I-mediated superoxide formation. 57 A caveat for any new drug is that it has to be beneficial in the presence of NAC, the current standard of care.…”

Section: Novel Therapeutic Approaches Against Apap Hepatotoxicitymentioning

confidence: 99%

Acetaminophen Hepatotoxicity

2019

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Acetaminophen (APAP) is one of the most popular and safe pain medications worldwide. However, due to its wide availability, it is frequently implicated in intentional or unintentional overdoses where it can cause severe liver injury and even acute liver failure (ALF). In fact, APAP toxicity is responsible for 46% of all ALF cases in the United States. Early mechanistic studies in mice demonstrated the formation of a reactive metabolite, which is responsible for hepatic glutathione depletion and initiation of the toxicity. This insight led to the rapid introduction of N-acetylcysteine as a clinical antidote. However, more recently, substantial progress was made in further elucidating the detailed mechanisms of APAP-induced cell death. Mitochondrial protein adducts trigger a mitochondrial oxidant stress, which requires amplification through a MAPK cascade that ultimately results in activation of c-jun N-terminal kinase (JNK) in the cytosol and translocation of phospho-JNK to the mitochondria. The enhanced oxidant stress is responsible for the membrane permeability transition pore opening and the membrane potential breakdown. The ensuing matrix swelling causes the release of intermembrane proteins such as endonuclease G, which translocate to the nucleus and induce DNA fragmentation. These pathophysiological signaling mechanisms can be additionally modulated by removing damaged mitochondria by autophagy and replacing them by mitochondrial biogenesis. Importantly, most of the mechanisms have been confirmed in human hepatocytes and indirectly through biomarkers in plasma of APAP overdose patients. The extensive necrosis caused by APAP overdose leads to a sterile inflammatory response. Although recruitment of inflammatory cells is necessary for removal of cell debris in preparation for regeneration, these cells have the potential to aggravate the injury. This review touches on the newest insight into the intracellular mechanisms of APAP-induced cells death and the resulting inflammatory response. Furthermore, it discusses the translation of these findings to humans and the emergence of new therapeutic interventions.

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Section: Novel Therapeutic Approaches Against Apap Hepatotoxicitymentioning

confidence: 99%

Acetaminophen Hepatotoxicity

2019

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“…Studies to better understand these roles, such as the influence of mitochondrial dynamics and biogenesis in mediating recovery and regeneration are ongoing with the ultimate hope to develop mitochondrial targeted therapeutics to prevent APAPinduced acute liver failure. Our unpublished data indicate that drugs such as 4methylpyrazole, which provides protection against APAP-induced injury (Akakpo et al, 2018), inhibits not only cytochrome P450 enzymes but also prevents JNK activation and its mitochondrial translocation and could thus be a useful therapeutic with similar potency as the current standard of care N-acetylcysteine. The SOD mimetics Calmangafodipir and Mito-TEMPO were also shown to have beneficial effects in APAP overdose in mice (Bedda et al, 2003;Du et al, 2018) and Calmangafodipir is currently in clinical trials (Dear et al, 2017).…”

Section: Resultsmentioning

confidence: 92%

Acetaminophen hepatotoxicity: A mitochondrial perspective

Ramachandran

Jaeschke

2019

Advances in Pharmacology

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“…The 50 mg/kg 4-MP dose used in the mice by Akakpo et al is approximately equivalent to 4 mg/kg in humans; theoretically, 15 mg/kg 4-MP is several times higher than the effective dose in mice and is also the approved dose for humans in toxic alcohol poisoning. However, a therapeutic dose of 4-MP in humans for APAP poisoning would need to be elucidated [ 10 ]. In the presence of 4-MP, NAPQI formation via CYP450 2E1 is reduced [ 11 ].…”

Section: Discussionmentioning

confidence: 99%

A Case Report of Massive Acetaminophen Poisoning Treated with a Novel “Triple Therapy”: N-Acetylcysteine, 4-Methylpyrazole, and Hemodialysis

Kiernan

Fritzges

Henry

et al. 2019

Case Reports in Emergency Medicine

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Massive acetaminophen (N-acetyl-p-aminophenol; APAP) ingestion is characterized by a rapid onset of mitochondrial dysfunction, including metabolic acidosis, lactemia, and altered mental status without hepatotoxicity which may not respond to the standard doses of N-acetylcysteine (NAC). A 64-year-old woman without medical history presented comatose after an ingestion of 208 tablets of Tylenol PM™ (APAP 500 mg and diphenhydramine 25 mg). The initial APAP concentration measured 1,017 µg/mL (therapeutic range 10-30 µg/mL), and elevated anion gap metabolic acidosis, lactemia, and 5-oxoprolinemia were detected. High-dose intravenous (IV) NAC, 4-methylpyrazole (4-MP), and hemodialysis (HD) were initiated. She was transferred to a liver transplant center and continued both NAC and HD therapies until complete resolution of metabolic acidosis and coma without developing hepatitis. She was discharged without sequelae. This is the fourth highest APAP concentration recorded in a surviving patient. Moreover, this is the first report of a novel “triple therapy” using NAC, 4-MP, and HD in the setting of massive APAP ingestion that presents with coma, elevated anion gap metabolic acidosis, and lactemia. Emergency physicians should recognize these critically ill patients and consider high-dose NAC, 4-MP, and HD to be initiated in the emergency department (ED).

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4-Methylpyrazole protects against acetaminophen hepatotoxicity in mice and in primary human hepatocytes

Cited by 82 publications

References 51 publications

Acetaminophen Hepatotoxicity

Acetaminophen Hepatotoxicity

Acetaminophen hepatotoxicity: A mitochondrial perspective

A Case Report of Massive Acetaminophen Poisoning Treated with a Novel “Triple Therapy”: N-Acetylcysteine, 4-Methylpyrazole, and Hemodialysis

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