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Literature DB >> 18337250

Role of JNK translocation to mitochondria leading to inhibition of mitochondria bioenergetics in acetaminophen-induced liver injury.

Naoko Hanawa¹, Mie Shinohara, Behnam Saberi, William A Gaarde, Derick Han, Neil Kaplowitz.

Abstract

Previously, we demonstrated JNK plays a central role in acetaminophen (APAP)-induced liver injury (Gunawan, B. K., Liu, Z. X., Han, D., Hanawa, N., Gaarde, W. A., and Kaplowitz, N. (2006) Gastroenterology 131, 165-178). In this study, we examine the mechanism involved in activating JNK and explore the downstream targets of JNK important in promoting APAP-induced liver injury in vivo. JNK inhibitor (SP600125) was observed to significantly protect against APAP-induced liver injury. Increased mitochondria-derived reactive oxygen species were implicated in APAP-induced JNK activation based on the following: 1) mitochondrial GSH depletion (maximal at 2 h) caused increased H2O2 release from mitochondria, which preceded JNK activation (maximal at 4 h); 2) treatment of isolated hepatocytes with H2O2 or inhibitors (e.g. antimycin) that cause increased H2O2 release from mitochondria-activated JNK. An important downstream target of JNK following activation was mitochondria based on the following: 1) JNK translocated to mitochondria following activation; 2) JNK inhibitor treatment partially protected against a decline in mitochondria respiration caused by APAP treatment; and 3) addition of purified active JNK to mitochondria isolated from mice treated with APAP plus JNK inhibitor (mitochondria with severe GSH depletion, covalent binding) directly inhibited respiration. Cyclosporin A blocked the inhibitory effect of JNK on mitochondria respiration, suggesting JNK was directly inducing mitochondrial permeability transition in isolated mitochondria from mice treated with APAP plus JNK inhibitor. Addition of JNK to mitochondria isolated from control mice did not affect respiration. Our results suggests that APAP-induced liver injury involves JNK activation, due to increased reactive oxygen species generated by GSH-depleted mitochondria, and translocation of activated JNK to mitochondria where JNK induces mitochondrial permeability transition and inhibits mitochondria bioenergetics.

Entities: Chemical Disease Gene Species

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Year: 2008 PMID： 18337250 PMCID： PMC2376214 DOI： 10.1074/jbc.M708916200

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

57 in total

1. Mitochondrial respiratory chain-dependent generation of superoxide anion and its release into the intermembrane space.

Authors: D Han; E Williams; E Cadenas
Journal: Biochem J Date: 2001-01-15 Impact factor: 3.857

2. c-Jun N-terminal kinase regulates mitochondrial bioenergetics by modulating pyruvate dehydrogenase activity in primary cortical neurons.

Authors: Qiongqiong Zhou; Philip Y Lam; Derick Han; Enrique Cadenas
Journal: J Neurochem Date: 2007-10-18 Impact factor: 5.372

3. Translocation of SAPK/JNK to mitochondria and interaction with Bcl-x(L) in response to DNA damage.

Authors: S Kharbanda; S Saxena; K Yoshida; P Pandey; M Kaneki; Q Wang; K Cheng; Y N Chen; A Campbell; T Sudha; Z M Yuan; J Narula; R Weichselbaum; C Nalin; D Kufe
Journal: J Biol Chem Date: 2000-01-07 Impact factor: 5.157

4. Mitochondrial superoxide anion production and release into intermembrane space.

Authors: Derick Han; Fernando Antunes; Francesca Daneri; Enrique Cadenas
Journal: Methods Enzymol Date: 2002 Impact factor: 1.600

5. NF-kappaB inhibition sensitizes hepatocytes to TNF-induced apoptosis through a sustained activation of JNK and c-Jun.

Authors: Hailing Liu; Chau R Lo; Mark J Czaja
Journal: Hepatology Date: 2002-04 Impact factor: 17.425

6. A protective role for cyclooxygenase-2 in drug-induced liver injury in mice.

Authors: T P Reilly; J N Brady; M R Marchick; M Bourdi; J W George; M F Radonovich; C A Pise-Masison; L R Pohl
Journal: Chem Res Toxicol Date: 2001-12 Impact factor: 3.739

7. Direct activation of mitochondrial apoptosis machinery by c-Jun N-terminal kinase in adult cardiac myocytes.

Authors: Hiroki Aoki; Peter M Kang; James Hampe; Koichi Yoshimura; Takafumi Noma; Masunori Matsuzaki; Seigo Izumo
Journal: J Biol Chem Date: 2002-01-10 Impact factor: 5.157

8. Vinblastine-induced phosphorylation of Bcl-2 and Bcl-XL is mediated by JNK and occurs in parallel with inactivation of the Raf-1/MEK/ERK cascade.

Authors: M Fan; M Goodwin; T Vu; C Brantley-Finley; W A Gaarde; T C Chambers
Journal: J Biol Chem Date: 2000-09-29 Impact factor: 5.157

Review 9. Biochemical and cellular mechanisms of toxic liver injury.

Authors: Neil Kaplowitz
Journal: Semin Liver Dis Date: 2002 Impact factor: 6.115

10. Mode of cell death after acetaminophen overdose in mice: apoptosis or oncotic necrosis?

Authors: Jaspreet S Gujral; Tamara R Knight; Anwar Farhood; Mary Lynn Bajt; Hartmut Jaeschke
Journal: Toxicol Sci Date: 2002-06 Impact factor: 4.849

243 in total

1. Mitochondrial HSP70 cognate-mediated differential expression of JNK1/2 in the pollution stressed grey mullets, Mugil cephalus.

Authors: E Padmini; B Vijaya Geetha
Journal: Fish Physiol Biochem Date: 2012-02-28 Impact factor: 2.794

Review 2. Hepatocyte death: a clear and present danger.

Authors: Harmeet Malhi; Maria Eugenia Guicciardi; Gregory J Gores
Journal: Physiol Rev Date: 2010-07 Impact factor: 37.312

3. c-Jun N-terminal kinase modulates oxidant stress and peroxynitrite formation independent of inducible nitric oxide synthase in acetaminophen hepatotoxicity.

Authors: Chieko Saito; John J Lemasters; Hartmut Jaeschke
Journal: Toxicol Appl Pharmacol Date: 2010-04-25 Impact factor: 4.219

Role of JNK translocation to mitochondria leading to inhibition of mitochondria bioenergetics in acetaminophen-induced liver injury.

1. Mitochondrial respiratory chain-dependent generation of superoxide anion and its release into the intermembrane space.

2. c-Jun N-terminal kinase regulates mitochondrial bioenergetics by modulating pyruvate dehydrogenase activity in primary cortical neurons.

3. Translocation of SAPK/JNK to mitochondria and interaction with Bcl-x(L) in response to DNA damage.

4. Mitochondrial superoxide anion production and release into intermembrane space.

5. NF-kappaB inhibition sensitizes hepatocytes to TNF-induced apoptosis through a sustained activation of JNK and c-Jun.

6. A protective role for cyclooxygenase-2 in drug-induced liver injury in mice.

7. Direct activation of mitochondrial apoptosis machinery by c-Jun N-terminal kinase in adult cardiac myocytes.

8. Vinblastine-induced phosphorylation of Bcl-2 and Bcl-XL is mediated by JNK and occurs in parallel with inactivation of the Raf-1/MEK/ERK cascade.

Review 9. Biochemical and cellular mechanisms of toxic liver injury.

10. Mode of cell death after acetaminophen overdose in mice: apoptosis or oncotic necrosis?

1. Mitochondrial HSP70 cognate-mediated differential expression of JNK1/2 in the pollution stressed grey mullets, Mugil cephalus.

Review 2. Hepatocyte death: a clear and present danger.

3. c-Jun N-terminal kinase modulates oxidant stress and peroxynitrite formation independent of inducible nitric oxide synthase in acetaminophen hepatotoxicity.

Review 4. Mechanisms of pathogenesis in drug hepatotoxicity putting the stress on mitochondria.

5. Distinct functions of JNK and c-Jun in oxidant-induced hepatocyte death.

Review 6. Mitochondrial dysfunction and cell death in neurodegenerative diseases through nitroxidative stress.

7. Mouse liver protein sulfhydryl depletion after acetaminophen exposure.

8. Inhibition of JNK mitochondrial localization and signaling is protective against ischemia/reperfusion injury in rats.

Review 9. Regulation of drug-induced liver injury by signal transduction pathways: critical role of mitochondria.

10. Activation of mitochondrial ERK protects cancer cells from death through inhibition of the permeability transition.