The modulation of co-stimulatory molecules by circulating exosomes in primary biliary cirrhosis

Tomiyama, Takashi; Yang, Guoxiang; Zhao, Ming; Zhang, Weici; Tanaka, Hajime; Wang, Jing; Leung, Patrick S.C.; Okazaki, Kazuichi; He, Xiaosong; Lu, Qianjin; Coppel, Ross L.; Bowlus, Christopher L.; Gershwin, M. Eric

doi:10.1038/cmi.2015.86

Cited by 49 publications

(37 citation statements)

References 63 publications

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“…Epigenetic Change(s) Consequences PBC DNA demethylation of gene promoter of CXCR3 in X chromosome of CD4 + T lymphocytes [35] DNA demethylation of multiple other gene promoters in X chromosome of CD4 + , CD8 + and CD14 + T lymphocytes [35] MiR-451a and miR-642a-3p increased [187] Demethylation correlates inversely with CXCR3 expression [35] CXCR3 orchestrates immune and NK cell migration to injury site [185,186] MiRNAs affect immune regulation [187] PBC progression may result [35] PSC 21 miRNAs distinguish PSC [103] 33 miRNAs distinguish CAC [103] MiR-200c principal marker of PSC [103] MiR-222, 483-5p upregulated in CAC [103] Aberrant methylation of CAC genes [191] Uncertain pathogenic effects [103] Possible biomarkers for PSC, CAC [190] NAFLD Differential methylation of 9 genes [192] Disrupted insulin signalling and metabolism [192] 46 miRNAs differentiated in NASH [104,128] MiR-34a and miR-146b upregulated [104,128] Downregulated miR-122 affects lipids [104] Bariatric surgery reverses some changes [192] Weight loss increases gene methylation [193] Metabolic pathways altered by gene methylation and miRNAs [104,192] Weight reduction may reverse some epigenetic changes [192,193] AIH MiR-21 increased in Japanese patients [44] MiR-21 and miR-122 correlate with ALT [44] Low miR-21 and miR-122 in cirrhosis [44] MiR-21 targets PDCD4 gene [44,194] MiR-122 increases INF-1 production [196] Vitamin D deficiency alters VDRE effects on gene activity [215,…”

Section: Liver Diseasementioning

confidence: 99%

Epigenetic changes and their implications in autoimmune hepatitis

Czaja

2018

Eur J Clin Investigation

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Background: The genetic risk of autoimmune hepatitis is insufficient to explain the observed risk, and epigenetic changes may explain disparities in disease occurrence in different populations within and between countries. The goal of this review was to examine how epigenetic changes induced by the environment or inherited as a phenotypic trait may affect autoimmune hepatitis and be amenable to therapeutic intervention. Materials and methods: Pertinent abstracts were identified in PubMed by multiple search terms. The number of abstracts reviewed was 1689, and the number of full-length articles reviewed exceeded 150. Results: Activation of pro-inflammatory genes in autoimmune disease is associated with hypomethylation of deoxyribonucleic acid and modification of histones within chromatin. Organ-specific microribonucleic acids can silence genes by marking messenger ribonucleic acids for degradation, and they can promote inflammatory activity or immunosuppression. High circulating levels of the microribonucleic acids 21 and 122 have been demonstrated in autoimmune hepatitis, and they may increase production of pro-inflammatory cytokines. Microribonucleic acids are also essential for maintaining regulatory T cells. Drugs, pollutants, infections, diet and ageing can induce inheritable epigenetic changes favouring autoimmunity. Reversal is feasible by manipulating enzymes, transcription factors, gene-silencing molecules and toxic exposures or by administering methyl donors and correcting vitamin D deficiency. Gene targets, site specificity, efficacy and consequences are uncertain. Conclusions: Potentially reversible epigenetic changes may affect the occurrence and outcome of autoimmune hepatitis, and investigations are warranted to determine the nature of these changes, key genomic targets, and feasible interventions and their consequences.

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Section: Liver Diseasementioning

confidence: 99%

Epigenetic changes and their implications in autoimmune hepatitis

Czaja

2018

Eur J Clin Investigation

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“…A s with most autoimmune diseases, primary biliary cholangitis (PBC) is female-predominant and has a long latency period between detection of autoantibodies and the clinical appearance of immunopathology. (1)(2)(3)(4) Although there are clearly major defects in adaptive immunity, including dysregulation of multiple T-cell and B-cell pathways, (5)(6)(7)(8)(9)(10)(11) there is significant evidence for the role of innate immunity in modulating and perhaps even initiating disease activity. (12)(13)(14)(15)(16)(17) Indeed, we have proposed that PBC is a multihit disease involving independent but overlapping immune path-ways that interact at different stages of disease activity, ultimately leading to the clinical entity of severe portal inflammation with potential cirrhosis.…”

Section: See Editorial On Page 1024mentioning

confidence: 99%

Chronic expression of interferon‐gamma leads to murine autoimmune cholangitis with a female predominance

et al. 2016

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In most autoimmune diseases the serologic hallmarks of disease precede clinical pathology by years. Therefore the use of animal models in defining early disease events becomes critical. Herein we have taken advantage of a “designer” mouse with dysregulation of interferon gamma (IFNγ) characterized by prolonged and chronic expression of IFNγ through deletion of the IFNγ 3′ UTR AU-rich element. These mice develop primary biliary cholangitis (PBC) with a female predominance that mimics human disease and is characterized by upregulation of total bile acids, spontaneous production of AMA, and portal duct inflammation. Transfer of CD4 T cells from ARE-Del−/− to B6/Rag1−/− mice induced moderate portal inflammation, and parenchymal inflammation, RNA-sequencing of liver gene expression revealed that upregulated genes potentially define early stages of cholangitis. Interestingly, upregulated genes specifically overlap with the gene expression signature of biliary epithelial cells in PBC, implying that IFNγ may play a pathogenic role in biliary epithelial cells (BEC) in the initiation stage of PBC. Moreover, differentially expressed genes in female mice have stronger Type I and II interferon signaling and lymphocyte-mediated immune responses and thus may drive the female bias of the disease. In conclusion, changes in IFNγ expression are critical for the pathogenesis of PBC.

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“…Other studies investigating PBC and liver fibrosis found that miR‐451a and miR‐642a‐3p were present at significantly higher levels in exosomes from patients with PBC compared to healthy controls and a progressive increase in circulating exosomal CCN2 was present in experimental fibrosis …”

Section: Exosomes As Novel Biomarkers Of Liver Diseasesmentioning

confidence: 93%

“…Therefore, exosomes may promote the progression of cirrhosis and other liver diseases with portal hypertension by inducing LSEC dysfunction. Furthermore, Tomiyama et al found that circulating exosomes from patients with primary biliary cirrhosis (PBC) selectively induced expression of co‐stimulatory molecules in different subsets of antigen‐presenting cells . This alteration may be involved in the pathogenesis of PBC and other autoimmune liver diseases.…”

Section: Exosomes In Liver Diseasesmentioning

confidence: 99%

Emerging role of exosomes in liver physiology and pathology

Cai

Cheng

Pan

et al. 2016

Hepatology Research

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Exosomes can mediate intercellular communication by conveying various bioactive molecules. Plentiful evidence suggests that exosomes are involved in many liver diseases including hepatitis C virus infection, hepatitis B virus infection, hepatocellular carcinoma, liver fibrosis, cirrhosis, non-alcoholic fatty liver disease, and alcoholic liver disease. Moreover, exosomes are present in nearly all human body fluids. Therefore, exosomal miRNA or proteins have the potential to be novel biomarkers of liver diseases. In the treatment of liver diseases, exosomes could participate in adaptive immune response and mesenchymal stem cell-based therapy. Exosomes can also be used as vehicles for genetic materials and drug delivery.

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The modulation of co-stimulatory molecules by circulating exosomes in primary biliary cirrhosis

Cited by 49 publications

References 63 publications

Epigenetic changes and their implications in autoimmune hepatitis

Epigenetic changes and their implications in autoimmune hepatitis

Chronic expression of interferon‐gamma leads to murine autoimmune cholangitis with a female predominance

Emerging role of exosomes in liver physiology and pathology

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