The Pathogenesis of Autoimmune Liver Disease

Arndtz, Katherine; Hirschfield, Gideon M.

doi:10.1159/000444471

Cited by 40 publications

(40 citation statements)

References 57 publications

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“…2 million deaths per year (Byass, 2014;Marcellin and Kutala, 2018). CLD progression relies mainly on (Arndtz and Hirschfield, 2016;Thrift et al, 2017;Marcellin and Kutala, 2018;Younossi et al, 2018): (i) chronic infection by hepatotropic viruses like hepatitis B virus (HBV, the most common risk factor in Asia) and hepatitis C virus (HCV), both worldwide distributed; (ii) excess alcohol consumption (i.e., alcoholic liver disease or ALD) and iii) non-alcoholic fatty liver disease (NAFLD), both predominant in western countries; iv) autoimmune liver diseases, including primary biliary cirrhosis (PBC), primary sclerosing cholangitis (PSC) and autoimmune hepatitis (AIH); v) hereditary diseases, including Wilson's disease, haemochromatosis and α1-anti-trypsin deficiency. The worldwide estimated incidence and prevalence of CLDs largely varies depending on the specific etiology, geographic area and likely other factors (sex, race, socioeconomic status) (Marcellin and Kutala, 2018).…”

Section: Etiology and Epidemiology: The Global Impact Of Cldsmentioning

confidence: 99%

Liver fibrosis: Pathophysiology, pathogenetic targets and clinical issues

Parola

Pinzani

2019

Molecular Aspects of Medicine

824

605

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The progression of chronic liver diseases (CLD), irrespective of etiology, involves chronic parenchymal injury, persistent activation of inflammatory response as well as sustained activation of liver fibrogenesis and wound healing response. Liver fibrogenesis, is a dynamic, highly integrated molecular, cellular and tissue process responsible for driving the excess accumulation of extracellular matrix (ECM) components (i.e., liver fibrosis) sustained by an eterogeneous population of hepatic myofibroblasts (MFs). The process of liver fibrogenesis recognizes a number of common and etiology-independent mechanisms and events but it is also significantly influenced by the specific etiology, as also reflected by peculiar morphological patterns of liver fibrosis development. In this review we will analyze the most relevant established and/or emerging pathophysiological issues underlying CLD progression with a focus on the role of critical hepatic cell populations, mechanisms and signaling pathways involved, as they represent potential therapeutic targets, to finally analyze selected and relevant clinical issues.

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Section: Etiology and Epidemiology: The Global Impact Of Cldsmentioning

confidence: 99%

Liver fibrosis: Pathophysiology, pathogenetic targets and clinical issues

Parola

Pinzani

2019

Molecular Aspects of Medicine

824

605

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“…There is a subtype of DILI with autoimmune background. AIH will attract more attention because many serious issues related to it remain to be elucidated [17,18,19].…”

Section: Discussionmentioning

confidence: 99%

Performance of a calculator for diagnosing the cause of liver damage

et al. 2019

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Introduction/Objective Making a calculator that would recognize patterns of abnormal liver function tests and link them to the most probable etiology could help clinicians in their initial orientation towards a definitive diagnosis in patients with liver damage. The aim of our study was to design, construct, and validate a calculator that based on a pattern of abnormalities in liver function tests of a patient with liver damage would propose the most probable etiology. Methods Patterns of abnormal liver function tests for certain etiology of liver damage were extracted from distributions of actual values taken from reports in medical literature about patients whose etiology of liver damage was proven by reliable diagnostic tests. After setting up the calculator with the patterns extracted, its diagnostic value was checked under real-life conditions, on a sample of patients with liver damage whose etiology was established by the gold standard of diagnostics (biopsy or else). The calculator validation study was carried out at the Military Medical Academy in Belgrade during a two-year period (2015)(2016). Results For all tested diagnoses, the calculator demonstrated a highly significant difference between the area under the receiver-operator curves' values and the value of 0.5 (p < 0.001), and high level of sensitivity (more than 90%, except for the model for chronic hepatitis) as well as relatively high specificity (more than 75%) were noted, indicating good ability of the calculator to detect etiology of liver damage. Conclusion New calculators showed satisfactory sensitivity and specificity for revealing major liver damage etiologies.

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“…However, with that caveat stated, the work suggests that prepregnancy immunization in the human population could provide a way to improve immunity to a disease that kills more than 4000 persons each day (46) and, furthermore, that wet nursing by a woman with a robust Th1 response could significantly enhance immunity in some vulnerable infants. What we have yet to learn is whether there are any negative consequences of maternal educational immunity, like the production of autoreactive T cells as a consequence of suckling a mother with a T cell-mediated autoimmune disease, such as type 1 diabetes (47) or primary biliary cholangitis (48). We also do not yet understand the role of maternal CD8 + cells or Tregs that home to the pup thymus and whether they participate in the development of tolerance to maternal Ags, as observed in those breastfed who later receive a transplant from their mothers (49).…”

Section: Discussionmentioning

confidence: 99%

Lactation-Based Maternal Educational Immunity Crosses MHC Class I Barriers and Can Impart Th1 Immunity to Th2-Biased Recipients

Ghosh

Muller

Walker

2017

The Journal of Immunology

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We have previously demonstrated lactational transfer of T cell–based immunity from dam to foster pup. In the short term, a significant part of transferred immunity is passive cellular immunity. However, as time progresses, this is replaced by what we have described as maternal educational immunity such that by young adulthood, all immune cells responding to a foster dam immunogen are the product of the foster pup’s thymus. To reduce confounding factors, this original demonstration used congenic/syngeneic dam and foster pup pairs. In this study, we investigated lactational transfer of immunity to Mycobacterium tuberculosis in MHC class I–mismatched animals, as well as from Th1-biased dams to Th2-biased foster pups. Using immunized C57BL/6J dams, lactational transfer to nonimmunized BALB/cJ foster pups resulted in much greater immunity than direct immunization in 5-wk-old pups (ex vivo assay of pup splenocytes). At this age, 82% of immunogen-responding cells in the pup spleen were produced through maternal educational immunity. FVB/NJ nonimmunized foster recipients had a greater number of maternal cells in the spleen and thymus but a much larger percentage was Foxp3+, resulting in equivalent immunity to direct immunization. Depletion of maternal Foxp3+ cells from pup splenocytes illustrated a substantial role for lactationally transferred dam regulatory T cells in suppression of the ex vivo response in FVB/NJ, but not BALB/cJ, recipients. We conclude that lactational transfer of immunity can cross MHC class I barriers and that Th1 immunity can be imparted to Th2-biased offspring; in some instances, it can be greater than that achieved by direct immunization.

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The Pathogenesis of Autoimmune Liver Disease

Cited by 40 publications

References 57 publications

Liver fibrosis: Pathophysiology, pathogenetic targets and clinical issues

Liver fibrosis: Pathophysiology, pathogenetic targets and clinical issues

Performance of a calculator for diagnosing the cause of liver damage

Lactation-Based Maternal Educational Immunity Crosses MHC Class I Barriers and Can Impart Th1 Immunity to Th2-Biased Recipients

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