Loss of hepatic LRPPRC alters mitochondrial bioenergetics, regulation of permeability transition and trans-membrane ROS diffusion

Cuillerier, Alexanne; Honarmand, Shamisa; Cadete, Virgilio J. J.; Ruiz, Matthieu; Forest, Anik; Deschênes, Sylvain; Beauchamp, Claudine; Charron, Guy; Rioux, John D.; Rosiers, Christine Des; Shoubridge, Eric A.; Burelle, Yan

doi:10.1093/hmg/ddx202

Cited by 42 publications

(49 citation statements)

References 70 publications

(95 reference statements)

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“…In mice with a heart conditional knockout of Lrpprc, impairment of ATP production was matched by lack of assembly of F‐ATP synthase and presence of F‐ATP synthase subcomplexes, which lacked subunits OSCP and A6L and catalysed oligomycin‐insensitive ATP hydrolysis (Mourier et al, ). Mice with hepatocyte‐specific conditional inactivation of Lrpprc showed assembly defects of F‐ATP synthase (whose activity was largely insensitive to oligomycin) with decreased formation of dimers and a remarkable inactivation of the PTP (Cuillerier et al, ). Interestingly, in spite of increased CyPD expression, the PTP was insensitive to CsA, suggesting that alterations in the peripheral stalk could have prevented CyPD binding (Cuillerier et al, ).…”

Section: Oscp Interactorsmentioning

confidence: 99%

“…Mice with hepatocyte‐specific conditional inactivation of Lrpprc showed assembly defects of F‐ATP synthase (whose activity was largely insensitive to oligomycin) with decreased formation of dimers and a remarkable inactivation of the PTP (Cuillerier et al, ). Interestingly, in spite of increased CyPD expression, the PTP was insensitive to CsA, suggesting that alterations in the peripheral stalk could have prevented CyPD binding (Cuillerier et al, ).…”

Section: Oscp Interactorsmentioning

confidence: 99%

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OSCP subunit of mitochondrial ATP synthase: role in regulation of enzyme function and of its transition to a pore

Giorgio¹,

Fogolari

Lippe

et al. 2018

British J Pharmacology

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The permeability transition pore (PTP) is a latent, high‐conductance channel of the inner mitochondrial membrane. When activated, it plays a key role in cell death and therefore in several diseases. The investigation of the PTP took an unexpected turn after the discovery that cyclophilin D (the target of the PTP inhibitory effect of cyclosporin A) binds to FOF1 (F)‐ATP synthase, thus inhibiting its catalytic activity by about 30%. This observation was followed by the demonstration that binding occurs at a particular subunit of the enzyme, the oligomycin sensitivity conferral protein (OSCP), and that F‐ATP synthase can form Ca2+‐activated, high‐conductance channels with features matching those of the PTP, suggesting that the latter originates from a conformational change in F‐ATP synthase. This review is specifically focused on the OSCP subunit of F‐ATP synthase, whose unique features make it a potential pharmacological target both for modulation of F‐ATP synthase and its transition to a pore. Linked Articles This article is part of a themed section on Mitochondrial Pharmacology: Featured Mechanisms and Approaches for Therapy Translation. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v176.22/issuetoc

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Section: Oscp Interactorsmentioning

confidence: 99%

Section: Oscp Interactorsmentioning

confidence: 99%

OSCP subunit of mitochondrial ATP synthase: role in regulation of enzyme function and of its transition to a pore

Giorgio¹,

Fogolari

Lippe

et al. 2018

British J Pharmacology

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“…LSFC patients display some lipid-handling abnormalities as evidenced from high circulating levels of long-chain acylcarnitines (LCACs), which are proxies of mitochondrial fatty acid (FA) β-oxidation perturbations (12). These patients are also affected by hepatic microvesicular steatosis (8,(13)(14)(15). Hepatic steatosis has also been reported in mice harboring liver-specific inactivation of Lrpprc (H-Lrpprc -/-) (15) and is rescued by overexpression of Lrpprc in mouse liver (13,14,16).…”

Section: Introductionmentioning

confidence: 99%

Lipidomics unveils lipid dyshomeostasis and low circulating plasmalogens as biomarkers in a monogenic mitochondrial disorder

Ruiz¹,

Cuillerier²,

Daneault³

et al. 2019

JCI Insight

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“…The main role of LRPPRC in the regulation of mitochondrial physiology appears to be related to its ability to bind RNA, in concert with the protein SLIRP, and to regulate its stability . Effects of LRPPRC mutations are not limited to mitochondrial oxidative phosphorylation; alterations in fatty acid β‐oxidation, permeability transition pore, ROS dynamics, and mitophagy have also been detected . Although no evidence of an abnormal inflammatory state in the French Canadian Leigh syndrome has yet been reported, the enhanced sensitivity to cell death observed in this disorder could have a functional link with a dysregulated activity of MAVS.…”

Section: Discussionmentioning

confidence: 99%

Negative Regulation of Mitochondrial Antiviral Signaling Protein–Mediated Antiviral Signaling by the Mitochondrial Protein LRPPRC During Hepatitis C Virus Infection

et al. 2018

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Hepatitis C virus (HCV) is highly efficient in establishing a chronic infection, having evolved multiple strategies to suppress the host antiviral responses. The HCV non-structural 5A (NS5A) protein, in addition to its role in viral replication and assembly, has long been known to hamper the interferon (IFN) response. However, the mechanism of this inhibitory activity of NS5A remains partly characterized. In a functional proteomic screening carried out in HCV replicon cells, we identified the mitochondrial protein LRPPRC as an NS5A binding factor. Notably, we found that downregulation of LRPPRC expression results in a significant inhibition of HCV infection, which is associated to an increased activation of the IFN response. Moreover, we showed that LRPPRC acts as a negative regulator of the mitochondrial-mediated antiviral immunity, by interacting with MAVS and inhibiting its association with TRAF3 and TRAF6. Finally, we demonstrated that NS5A is able to interfere with MAVS activity in a LRPPRC-dependent manner. Overall, our results indicate that NS5A contributes to the inhibition of innate immune pathways during HCV infection by exploiting the ability of LRPPRC to inhibit MAVS-regulated antiviral signaling. This article is protected by copyright. All rights reserved.

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Loss of hepatic LRPPRC alters mitochondrial bioenergetics, regulation of permeability transition and trans-membrane ROS diffusion

Cited by 42 publications

References 70 publications

OSCP subunit of mitochondrial ATP synthase: role in regulation of enzyme function and of its transition to a pore

OSCP subunit of mitochondrial ATP synthase: role in regulation of enzyme function and of its transition to a pore

Lipidomics unveils lipid dyshomeostasis and low circulating plasmalogens as biomarkers in a monogenic mitochondrial disorder

Negative Regulation of Mitochondrial Antiviral Signaling Protein–Mediated Antiviral Signaling by the Mitochondrial Protein LRPPRC During Hepatitis C Virus Infection

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