Enhancement of acetaminophen-induced chronic hepatotoxicity in restricted fed rats: a nonclinical approach to acetaminophen-induced chronic hepatotoxicity in susceptible patients

Kondo, Kazuma; Yamada, Naohito; Suzuki, Yusuke; Toyoda, Keiko; Hashimoto, Tatsuji; Takahashi, Akiko; Kobayashi, Akio; Shoda, Toshiyuki; Kuno, Hideyuki; Sugai, Shoichiro

doi:10.2131/jts.37.911

Cited by 21 publications

(23 citation statements)

References 64 publications

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“…Although this did not achieve statistical significance, it does suggest that the paracetamol diet may have caused some low-level damage in some mice which is not measurable in the circulation, at least not after 6 weeks of treatment. Previous animal studies that have dosed once daily, via intraperitoneal injection or oral gavage, for 30-99 days with 75-300 mg/ kg showed no evidence of toxicity as assessed by liver function tests [7][8][9]. Our study, which modelled a more clinically relevant exposure to paracetamol at regular intervals over a full day, as it was consumed in the diet, rather than once daily, appears to confirm these findings.…”

Section: Discussionsupporting

confidence: 82%

“…There have been few animal studies of chronic paracetamol exposure. Two rat studies, and one mouse study, showed that low-dose paracetamol administered daily did not cause liver toxicity in the absence of other risk factors [7][8][9]. Several rat and BALB/c mouse studies have found that pretreatment with nontoxic doses of paracetamol for 4-8 days before exposure to a high dose of paracetamol can protect against hepatotoxicity, through mechanisms including reduction in cytochrome (CYP)2E1 activity, and increased glutathione (GSH) levels [10][11][12].…”

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confidence: 99%

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N‐Acetyl cysteine does not prevent liver toxicity from chronic low‐dose plus subacute high‐dose paracetamol exposure in young or old mice

Kane

Huizer-Pajkos

Mach

et al. 2016

Fundamemntal Clinical Pharma

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Paracetamol is an analgesic commonly used by people of all ages, which is well documented to cause severe hepatotoxicity with acute over-exposures. The risk of hepatotoxicity from non-acute paracetamol exposures is less extensively studied, and this is the exposure most common in older adults. Evidence on the effectiveness of N-acetyl cysteine (NAC) for non-acute paracetamol exposures, in any age group, is lacking. This study aimed to examine the effect of long-term exposure to therapeutic doses of paracetamol and sub-acute paracetamol over-exposure, in young and old mice, and to investigate whether NAC was effective at preventing paracetamol hepatotoxicity induced by these exposures. Young and old male C57BL/6 mice were fed a paracetamol-containing (1.33g/kg food) or control diet for 6 weeks. Mice were then dosed orally 8 times over 3 days with additional paracetamol (250mg/kg) or saline, followed by either one or two doses of oral NAC (1200mg/kg) or saline. Chronic low-dose paracetamol exposure did not cause hepatotoxicity in young or old mice, measured by serum alanine aminotransferase (ALT) elevation, and confirmed by histology and a DNA fragmentation assay. Sub-acute paracetamol exposure caused significant hepatotoxicity in young and old mice, measured by biochemistry (ALT) and histology. Neither a single nor double dose of NAC protected against this toxicity from sub-acute paracetamol in young or old mice. This finding has important clinical implications for treating toxicity due to different paracetamol exposure types in patients of all ages, and implies a need to develop new treatments for sub-acute paracetamol toxicity.

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Section: Discussionsupporting

confidence: 82%

mentioning

confidence: 99%

N‐Acetyl cysteine does not prevent liver toxicity from chronic low‐dose plus subacute high‐dose paracetamol exposure in young or old mice

Kane

Huizer-Pajkos

Mach

et al. 2016

Fundamemntal Clinical Pharma

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“…Chronic exposure to alcohol decreases autophagic flux by inhibiting the fusion of autophagosomes with lysosomes [87]. This may explain why chronic consumption to alcohol favors APAP hepatotoxicity [88, 89]. Besides induction of autophagy, APAP also induces the formation of mitochondrial spheroids in vivo [90], which are ring-like spherical structures with lumen surrounded by mitochondrial membranes that can contain cytoplasmic material.…”

Section: Autophagy In Acute Liver Injurymentioning

confidence: 99%

Liver Autophagy in Anorexia Nervosa and Acute Liver Injury

Kheloufi

Boulanger

Durand

et al. 2014

BioMed Research International

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Autophagy, a lysosomal catabolic pathway for long-lived proteins and damaged organelles, is crucial for cell homeostasis, and survival under stressful conditions. During starvation, autophagy is induced in numerous organisms ranging from yeast to mammals, and promotes survival by supplying nutrients and energy. In the early neonatal period, when transplacental nutrients supply is interrupted, starvation-induced autophagy is crucial for neonates' survival. In adult animals, autophagy provides amino acids and participates in glucose metabolism following starvation. In patients with anorexia nervosa, autophagy appears initially protective, allowing cells to copes with nutrient deprivation. However, when starvation is critically prolonged and when body mass index reaches 13 kg/m2 or lower, acute liver insufficiency occurs with features of autophagic cell death, which can be observed by electron microscopy analysis of liver biopsy samples. In acetaminophen overdose, a classic cause of severe liver injury, autophagy is induced as a protective mechanism. Pharmacological enhancement of autophagy protects against acetaminophen-induced necrosis. Autophagy is also activated as a rescue mechanism in response to Efavirenz-induced mitochondrial dysfunction. However, Efavirenz overdose blocks autophagy leading to liver cell death. In conclusion, in acute liver injury, autophagy appears as a protective mechanism that can be however blocked or overwhelmed.

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“…It is reasonable to anticipate population specific toxicity because the activity of CYP2E1—the major enzyme producing NAPQI—is not yet quantified, while data on the NAPQI detoxification capacity through glutathione conjugation in neonates are also lacking 27 28. Furthermore, immaturity of hepatic transporters or individual patient characteristics like malnutrition may further contribute to specific vulnerability 29 30…”

Section: What Is Not Yet Known About Paracetamol and Pda Closurementioning

confidence: 99%

Paracetamol to induce ductus arteriosus closure: is it valid?

Allegaert

Anderson

Simons

et al. 2013

Archives of Disease in Childhood

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There remains a need for alternative medical treatments for patent ductus arteriosus (PDA) closure in extreme preterm neonates because of therapeutic failure and adverse effects associated with non-selective cyclo-oxygenase inhibitors. Reports of an association between paracetamol exposure and PDA closure in a limited number of extreme preterm neonates have been published. However, causality cannot be taken for granted because a link between the current knowledge of the clinical pharmacology of paracetamol and (patho)physiology of ductal closure is not known. In contrast to non-selective cyclo-oxygenase inhibitors, paracetamol has limited effects at peripheral sites, is a poor antithrombotic and anti-inflammatory drug and exerts its effects primarily within the central nervous system. Although paracetamol appears an effective and safe analgesic in term and near term neonates, its effectiveness and safety for PDA closure are uncertain because the drug is administered in high doses and there remain a limited number of observations in this specific subpopulation so far. Prospective comparative trials are reasonable and are urgently needed to establish both the effectiveness and safety data of paracetamol when used for this indication.

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Enhancement of acetaminophen-induced chronic hepatotoxicity in restricted fed rats: a nonclinical approach to acetaminophen-induced chronic hepatotoxicity in susceptible patients

Cited by 21 publications

References 64 publications

N‐Acetyl cysteine does not prevent liver toxicity from chronic low‐dose plus subacute high‐dose paracetamol exposure in young or old mice

N‐Acetyl cysteine does not prevent liver toxicity from chronic low‐dose plus subacute high‐dose paracetamol exposure in young or old mice

Liver Autophagy in Anorexia Nervosa and Acute Liver Injury

Paracetamol to induce ductus arteriosus closure: is it valid?

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