Mechanisms of acetaminophen-induced cell death in primary human hepatocytes

Xie, Yuchao; McGill, Mitchell R.; Dorko, Kenneth; Kumer, Sean C.; Schmitt, Timothy M.; Forster, Jameson; Jaeschke, Hartmut

doi:10.1016/j.taap.2014.05.010

Cited by 210 publications

(229 citation statements)

References 39 publications

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“…Cells were isolated using a multi-step collagenase procedure as described in detail previously. 36 Media consisted of Williams' Medium E (Life Technologies, Grand Island, NY, USA) supplemented with L-glutamine (2 mM) (Life Technologies), HEPES (10 mM), insulin (10 − 7 M), dexamethasone (10 − 7 M), penicillin (100 U/ml), streptomycin (100 μg/ml) and amphotericin B (0.25 μg/ml). The hepatocytes were brought to a concentration of 0.5 × 10 6 cells/ml in Williams' Medium E, as described above, plus 5% bovine calf serum.…”

Section: Discussionmentioning

confidence: 99%

Serine 574 phosphorylation alters transcriptional programming of FOXO3 by selectively enhancing apoptotic gene expression

Zhao

Tikhanovich

et al. 2015

Cell Death Differ

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Forkhead box O3 (FOXO3) is a multispecific transcription factor that is responsible for multiple and conflicting transcriptional programs such as cell survival and apoptosis. The protein is heavily post-translationally modified and there is considerable evidence that post-transcriptional modifications (PTMs) regulate protein stability and nuclear-cytosolic translocation. Much less is known about how FOXO3 PTMs determine the specificity of its transcriptional program. In this study we demonstrate that exposure of hepatocytes to ethanol or exposure of macrophages to lipopolysaccharide (LPS) induces the c-Jun N-terminal kinase (JNK)-dependent phosphorylation of FOXO3 at serine-574. Chromatin immunoprecipitation (ChIP), mRNA and protein measurements demonstrate that p-574-FOXO3 selectively binds to promoters of pro-apoptotic genes but not to other well-described FOXO3 targets. Both unphosphorylated and p-574-FOXO3 bound to the B-cell lymphoma 2 (Bcl-2) promoter, but the unphosphorylated form was a transcriptional activator, whereas p-574-FOXO3 was a transcriptional repressor. The combination of increased TRAIL (TNF-related apoptosis-inducing ligand) and decreased Bcl-2 was both necessary and sufficient to induce apoptosis. LPS treatment of a human monocyte cell line (THP-1) induced FOXO3 S-574 phosphorylation and apoptosis. LPS-induced apoptosis was prevented by knockdown of FOXO3. It was restored by overexpressing wild-type FOXO3 but not by overexpressing a nonphosphorylatable S-574A FOXO3. Expression of an S-574D phosphomimetic form of FOXO3 induced apoptosis even in the absence of LPS. A similar result was obtained with mouse peritoneal macrophages where LPS treatment increased TRAIL, decreased Bcl-2 and induced apoptosis in wild-type but not FOXO3 −/− cells. This work thus demonstrates that S-574 phosphorylation generates a specifically apoptotic form of FOXO3 with decreased transcriptional activity for other well-described FOXO3 functions. Forkhead box O3 (FOXO3) is a multispecific transcription factor that serves as a longevity factor 1,2 and tumor suppressor and is critically involved in multiple seemingly independent biological process including cell-cycle arrest, 3 DNA repair, 4 antioxidant and stress responses, 5 apoptosis, 6 autophagy, glucose metabolism and aging. 7 Its many transcriptional programs are frequently in opposition to each other as it induces apoptosis, yet it is also critical for cell survival and longevity. Although there is considerable information regarding the mechanisms that regulate the nuclear/cytosolic distribution and protein stability of FOXO3, the control mechanisms that regulate transcriptional specificity are poorly understood.FOXO3 function is tightly regulated by multiple posttranslational modifications (PTMs) including phosphorylation, acetylation, ubiquitination and arginine and lysine methylation. Specific PTMs regulate the partitioning of FOXO3 between the cytosol and the nucleus 8-15 and its stability and degradation, 16 but the links between specific PTMs and FOXO3 tran...

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Section: Discussionmentioning

confidence: 99%

Serine 574 phosphorylation alters transcriptional programming of FOXO3 by selectively enhancing apoptotic gene expression

Zhao

Tikhanovich

et al. 2015

Cell Death Differ

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“…Currently, primary human hepatocytes are difficult to attain, expensive, and of very limited supply. While some newer cell lines, such as HepaRG cells recapitulate more of the facets of primary human hepatocytes (4,(21)(22)(23), they still only express a relatively small degree of hepatocyte functional genes such as drug metabolizing enzymes and xenobiotic transporters (24). Human ESCs are highly proliferative, have an indefinite life span, and could thus be used to generate on a routine basis new and useful human hepatocyte-like cells that fairly accurately resemble primary human hepatocytes.…”

Section: Drug-induced Liver Injury-new Models New Methodsmentioning

confidence: 99%

“…Critical to the generation of new drugs is the continued development of our understanding of APAP-induced ALF in human patients. While a number of recent papers from our group and others have made considerable advances in understanding mechanisms of toxicity in patients and human hepatocytes (2)(3)(4)(5), there is still a lack of actionable therapeutic targets. Liver transplantation is the gold standard procedure for treating late-stage ALF but this operation is expensive and comes with additional costs of lifelong anti-rejection medication.…”

Section: Acetaminophen-induced Injury and Acute Liver Failure As A CLmentioning

confidence: 99%

Noncoding RNAs as therapeutics for acetaminophen-induced liver injury

Woolbright

Jaeschke

2016

Stem Cell Investig.

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Acetaminophen-induced injury and acute liver failure as a clinically relevant modelAcetaminophen-(APAP) induced acute liver failure (ALF) is a major cause of morbidity and mortality in the US (1). Currently, the major therapeutic is N-acetylcysteine (NAC), which is highly effective when given within 8 h of drug overdose. However, late-presenting patients commonly have poor outcomes, and NAC is not effective in these patients. As such, additional therapeutics are urgently needed to treat late-presenting patients. Critical to the generation of new drugs is the continued development of our understanding of APAP-induced ALF in human patients. While a number of recent papers from our group and others have made considerable advances in understanding mechanisms of toxicity in patients and human hepatocytes (2-5), there is still a lack of actionable therapeutic targets. Liver transplantation is the gold standard procedure for treating late-stage ALF but this operation is expensive and comes with additional costs of lifelong anti-rejection medication. In addition, due to limited donor organs, this therapeutic option is not always available (1). There are also ethical issues to consider as a majority of APAP-induced liver injury cases are due to attempted suicide. It is thus imperative that new modalities of treatment, including novel pharmacological agents, be explored for patients who suffer from drug-induced liver injury and acute liver failure.The mechanisms behind APAP-induced liver injury have been extensively examined over the last 40 years (6,7). APAP is typically non-toxic when taken at therapeutic dosages as it is largely metabolized through phase II metabolism by glucuronosyltransferases (glucuronidation) and sulfotransferases (sulfation), and then excreted via the urine (7).Minor levels of APAP are metabolized by cytochrome P450 2E1 (Cyp2E1), which results in the formation of the reactive metabolite N-acetyl-p-benzoquinone imine (NAPQI) (7). However, when sulfation is saturated (8), additional quantities of APAP are metabolized by Cyp2E1 and NAPQI accumulation initiates liver toxicity. Excess NAPQI causes significant depletion of glutathione, protein adduct formation especially in mitochondria (9,10) and a mitochondrial oxidative and nitrosative stress (11), which is then amplified by translocation of c-Jun N-terminal kinase (JNK) to the mitochondria (12,13). This triggers the opening of the mitochondrial permeability transition pore resulting in collapse of the membrane potential, cessation of ATP formation, and matrix swelling (14). The latter effect results in the outer membrane rupture with release of mitochondrial membrane proteins including apoptosis inducing factor and endonuclease G, which translocate to the nucleus and trigger DNA fragmentation (6). The extensive mitochondrial dysfunction and karyolysis are responsible for the necrotic cell death (6). A number of therapeutics have been proposed based on these mechanisms and the pathways that control them; however, new mechanisms that complement our cu...

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“…This indicates that acylcarnitine levels in plasma may indeed reflect mitochondrial dysfunction, not cell death. Interestingly, acylcarnitine levels did not significantly increase during APAP hepatotoxicity in patients despite the evidence that mitochondrial dysfunction is critical for APAP-induced liver injury in patients [164, 268]. However, it was shown that treatment of mice with NAC, which does not only support GSH synthesis but also mitochondrial energetics [18], strongly reduced the increase in acylcarnitine levels in mice [266].…”

Section: Mitochondrial Biomarkers In Drug-induced Liver Injurymentioning

confidence: 99%

Mitochondrial dysfunction as a mechanism of drug-induced hepatotoxicity: current understanding and future perspectives

et al. 2018

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Mitochondria are critical cellular organelles for energy generation and are now also recognized as playing important roles in cellular signaling. Their central role in energy metabolism, as well as their high abundance in hepatocytes, make them important targets for drug-induced hepatotoxicity. This review summarizes the current mechanistic understanding of the role of mitochondria in drug-induced hepatotoxicity caused by acetaminophen, diclofenac, anti-tuberculosis drugs such as rifampin and isoniazid, anti-epileptic drugs such as valproic acid and constituents of herbal supplements such as pyrrolizidine alkaloids. The utilization of circulating mitochondrial-specific biomarkers in understanding mechanisms of toxicity in humans will also be examined. In summary, it is well-established that mitochondria are central to acetaminophen-induced cell death. However, the most promising areas for clinically useful therapeutic interventions after acetaminophen toxicity may involve the promotion of adaptive responses and repair processes including mitophagy and mitochondrial biogenesis, In contrast, the limited understanding of the role of mitochondria in various aspects of hepatotoxicity by most other drugs and herbs requires more detailed mechanistic investigations in both animals and humans. Development of clinically relevant animal models and more translational studies using mechanistic biomarkers are critical for progress in this area.

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Mechanisms of acetaminophen-induced cell death in primary human hepatocytes

Cited by 210 publications

References 39 publications

Serine 574 phosphorylation alters transcriptional programming of FOXO3 by selectively enhancing apoptotic gene expression

Serine 574 phosphorylation alters transcriptional programming of FOXO3 by selectively enhancing apoptotic gene expression

Noncoding RNAs as therapeutics for acetaminophen-induced liver injury

Mitochondrial dysfunction as a mechanism of drug-induced hepatotoxicity: current understanding and future perspectives

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