Liver injury correlates with biomarkers of autoimmunity and disease activity and represents an organ system involvement in patients with systemic lupus erythematosus

Liu, Yuxin; Yu, Jianghong; Oaks, Zachary; Marchena-Mendez, Ivan; Francis, Lisa; Bonilla, Eduardo; Aleksiejuk, Phillip A.; Patel, Jessica; Bánki, Katalin; Landas, Steve K.; Perl, András

doi:10.1016/j.clim.2015.07.001

Cited by 43 publications

(33 citation statements)

References 71 publications

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“…In summary, the model of lupus pathogenesis proposed herein involves mTORC1-controlled mitochondrial dysfunction in the liver, with related generation of aPL and increased hepatocarcinogenesis in SLE (29). In support of this model, liver disease, which was defined as a $2-fold elevation in the levels of aspartate aminotransferase or alanine aminotransferase, was associated with the production of aPL in our SLE cohort (16) as well as in previous meta-analyses (17,18). Along these lines, HCC develops in the liver following chronic inflammation, which is driven by mitochondrial oxidative stress (19,36) and responds to treatment with rapamycin (48).…”

Section: Discussionsupporting

confidence: 79%

“…Interestingly, the prevalence of HCC is increased in patients with SLE (29). Recently, liver disease was found to be associated with APS in our lupus cohort (16), a finding consistent with that in metaanalyses of liver involvement in patients with APS (17,18). TAL is overexpressed in the T cells of SLE patients, which may be related to protection against oxidative stress (3).…”

supporting

confidence: 90%

“…This finding is consistent with the data reported in meta-analyses of liver involvement in patients with APS (17,18). Interestingly, treatment with rapamycin, which blocks the activation of mTORC1, prevented liver disease in our cohort of lupus patients (16). We therefore undertook the present study to examine the role of the liver in mTOR activation and its association with APS in mice that spontaneously develop SLE.…”

mentioning

confidence: 99%

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Mitochondrial Dysfunction in the Liver and Antiphospholipid Antibody Production Precede Disease Onset and Respond to Rapamycin in Lupus‐Prone Mice

Oaks

Winans

Caza

et al. 2016

Arthritis & Rheumatology

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107

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Background Anti-phospholipid antibodies (aPL) constitute a diagnostic criterion of systemic lupus erythematosus (SLE). aPL have been linked to liver disease in SLE. Since the mechanistic target of rapamycin (mTOR) is a regulator of oxidative stress, which contributes to the development of aPL, we examined the involvement of liver mitochondria in mouse lupus pathogenesis. Methods Mitochondria were isolated from lupus-prone MRL/lpr, C57BL/6.lpr and MRL mice, age-matched C57BL/6 negative controls, and transaldolase-deficient mice which exhibit oxidative stress in the liver. Electron transport chain (ETC) activity was assessed via oxygen consumption. ETC proteins, regulators of mitochondrial homeostasis, and mTOR complexes, mTORC1 and mTORC2, were examined by western blot. Anti-cardiolipin (ACLA) and anti-β2 glycoprotein I autoantibodies (anti-β2GPI) were measured by ELISA in mice treated with or without rapamycin. Results Mitochondrial oxygen consumption was increased in the liver of 4-week-old, disease-free MRL/lpr mice relative to age-matched controls. Mitophagy-initiator dynamin-related protein 1 (Drp1) was depleted while activity of mTORC1 was increased in MRL/lpr mice. In turn, mTORC2 activity was decreased in MRL and MRL/lpr mice. ACLA and anti-β2GPI levels were also elevated in 4-week-old MRL, C57BL/6.lpr, and MRL/lpr mice, preceding the development of nephritis. Transaldolase-deficient mice showed increased oxygen consumption, Drp1 depletion, mTORC1 activation, and elevated expression of NDUFS3, a pro-oxidant subunit of ETC complex I, as well as ACLA and anti-β2GPI production. Rapamycin selectively blocked mTORC1, NDUFS3 expression and aPL production both in transaldolase-deficient and lupus-prone mice. Conclusion mTORC-1-dependent mitochondrial dysfunction contributes to the generation of aPL and may represent a treatment target in SLE.

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Section: Discussionsupporting

confidence: 79%

supporting

confidence: 90%

mentioning

confidence: 99%

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Mitochondrial Dysfunction in the Liver and Antiphospholipid Antibody Production Precede Disease Onset and Respond to Rapamycin in Lupus‐Prone Mice

Oaks

Winans

Caza

et al. 2016

Arthritis & Rheumatology

Self Cite

107

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“…Liver disease, defined as a >2-fold elevation of AST or ALT, was present in 20.7 % of SLE patients independent of hepatotoxic medications [47]. Both NAC and rapamycin, but not azathioprine, cyclosporine, or cyclophosphamide, were successful in preventing liver disease [47].…”

Section: Livermentioning

confidence: 99%

“…Both NAC and rapamycin, but not azathioprine, cyclosporine, or cyclophosphamide, were successful in preventing liver disease [47]. Furthermore, liver disease correlated to higher SLE disease activity index (SLEDAI) scores in patients and thus is an important organ system to monitor [47]. …”

Section: Livermentioning

confidence: 99%

Activation of the Mechanistic Target of Rapamycin in SLE: Explosion of Evidence in the Last Five Years

et al. 2016

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The mechanistic target of rapamycin (mTOR) is a central regulator in cell growth, activation, proliferation, and survival. Activation of the mTOR pathway underlies the pathogenesis of systemic lupus erythematosus (SLE). While mTOR activation and its therapeutic reversal were originally discovered in T cells, recent investigations have also uncovered roles in other cell subsets including B cells, macrophages, and “non-immune” organs such as the liver and the kidney. Activation of mTOR complex 1 (mTORC1) precedes the onset of SLE and associated co-morbidities, such as anti-phospholipid syndrome (APS), and may act as an early marker of disease pathogenesis. Six case reports have now been published that document the development of SLE in patients with genetic activation of mTORC1. Targeting mTORC1 over-activation with N-acetylcysteine, rapamycin, and rapalogs provides an opportunity to supplant current therapies with severe side effect profiles such as prednisone or cyclophosphamide. In the present review, we will discuss the recent explosion of findings in support for a central role for mTOR activation in SLE.

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Redox Pathogenesis in Rheumatic Diseases

Laniak,

Winans,

Patel

et al. 2024

ACR Open Rheumatology

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Despite being some of the most anecdotally well‐known roads to pathogenesis, the mechanisms governing autoimmune rheumatic diseases are not yet fully understood. The overactivation of the cellular immune system and the characteristic development of autoantibodies have been linked to oxidative stress. Typical clinical manifestations, such as joint swelling and deformities and inflammation of the skin and internal organs, have also been connected directly or indirectly to redox mechanisms. The differences in generation and restraint of oxidative stress provide compelling evidence for the broad variety in pathology among rheumatic diseases and explain some of the common triggers and discordant manifestations in these diseases. Growing evidence of redox mechanisms in pathogenesis has provided a broad array of new potential therapeutic targets. Here, we explore the mechanisms by which oxidative stress is generated, explore its roles in autoimmunity and end‐organ damage, and discuss how individual rheumatic diseases exhibit unique features that offer targets for therapeutic interventions.

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Liver injury correlates with biomarkers of autoimmunity and disease activity and represents an organ system involvement in patients with systemic lupus erythematosus

Cited by 43 publications

References 71 publications

Mitochondrial Dysfunction in the Liver and Antiphospholipid Antibody Production Precede Disease Onset and Respond to Rapamycin in Lupus‐Prone Mice

Mitochondrial Dysfunction in the Liver and Antiphospholipid Antibody Production Precede Disease Onset and Respond to Rapamycin in Lupus‐Prone Mice

Activation of the Mechanistic Target of Rapamycin in SLE: Explosion of Evidence in the Last Five Years

Redox Pathogenesis in Rheumatic Diseases

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