Preferential X chromosome loss but random inactivation characterize primary biliary cirrhosis

Miozzo, Monica; Selmi, Carlo; Gentilin, Barbara; Grati, Francesca Romana; Sirchia, Silvia Maria; Oertelt, Sabine; Zuin, Massimo; Gershwin, M. Eric; Podda, Mauro; Invernizzi, Pietro

doi:10.1002/hep.21696

Cited by 123 publications

(90 citation statements)

References 34 publications

(47 reference statements)

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“…How these factors are molecularly involved in PBC onset remains unclear. Elsewhere, it was reported that X-chromosome gene expression instability might also participate in female predominance in the disease [64,65], and that monozygotic twins and sisters discordant for PBC exhibited particular epigenetic differences [66]. These collectively support the notion that epigenetic factors influence the onset of PBC.…”

Section: Epigenetics On Pbcmentioning

confidence: 65%

Genetics and epigenetics in the pathogenesis of primary biliary cholangitis

Joshita

Umemura

Tanaka

et al. 2017

Clin J Gastroenterol

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Primary biliary cholangitis (PBC) is a chronic, slowly progressive cholestatic autoimmune liver disease predominantly afflicting women. PBC is characterized by the presence of disease-specific antimitochondrial antibodies and the histological destruction of intrahepatic bile ducts, which eventually lead to cirrhosis and hepatic failure. Fortunately, ursodeoxycholic acid therapy has improved the outcome of the vast majority of PBC cases. Although the etiology of PBC has not yet been elucidated, human leukocyte antigen (HLA) class II alleles have been consistently associated with disease onset for decades. PBC patients may also have genetically determined risk factors in non-HLA regions. Meanwhile, exposure to environmental factors, such as infectious diseases and harmful chemicals, can produce epigenetic alterations in some individuals and subsequent PBC onset. In this review, we describe the influence of HLA alleles and other gene polymorphisms on PBC along with the results of genome-wide association studies on this disease and its future prospects in terms of epigenetics.

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Section: Epigenetics On Pbcmentioning

confidence: 65%

Genetics and epigenetics in the pathogenesis of primary biliary cholangitis

Joshita

Umemura

Tanaka

et al. 2017

Clin J Gastroenterol

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“…Interestingly, they found PBC patients to have an increased frequency of X chromosome monosomy in peripheral blood cells overall, as well as in all tested white blood cell subpopulations, suggesting an instabilty of the X chromosome related to PBC (91). Further work by this same group using quantitative flourescent PCR found the pattern of X chromosome loss to be preferential in PBC, compared to healthy and hepatitis C virus infected controls (92). In this same study, X chromosome inactivation (XCI) was also assessed, and no significant association between PBC and degree of XCI skewing was identified (92).…”

Section: The Sex Chromosomes and Pbcmentioning

confidence: 95%

“…Further work by this same group using quantitative flourescent PCR found the pattern of X chromosome loss to be preferential in PBC, compared to healthy and hepatitis C virus infected controls (92). In this same study, X chromosome inactivation (XCI) was also assessed, and no significant association between PBC and degree of XCI skewing was identified (92). Taken together, these findings suggest that particular X-linked alleles or haplotypes, likely in genes escaping XCI, might predispose to the development of autoimmunity as the result of haploinsufficiency due to the acquired monosomy, providing us with novel candidate regions for which to search and address in PBC.…”

Section: The Sex Chromosomes and Pbcmentioning

confidence: 96%

Genetics and Genomics of Primary Biliary Cirrhosis

Juran

Lazaridis

2008

Clinics in Liver Disease

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The etiological and pathogenic factors contributing to PBC development, progression, response to treatment, and ultimately, outcome remain a mystery. This lack of knowledge can be attributed to the complexity of PBC, wherein a number of environmental triggers may be culpable, but require coexisting genetic susceptibility to exert their effect. Recognition of the genomic regions harboring these heritable risk factors has been hindered by the rarity and late onset of PBC, which has rendered the collection of adequate numbers of patients and family members for genetic analyses a difficult task. Recent advancements in the discipline of genomics holds promise to fundamentally change our understanding, prevention, and therapy of PBC. This chance arises from the development of new high-throughput approaches to genotyping, providing the means to rapidly uncover many of the genetic polymorphisms that are relevant to disease. In order to move ahead, large registries and biospecimen repositories of patients with PBC, their family members, and well-matched controls need to be established, maintained, and continually expanded. At the same time, sizeable, comprehensive haplotype mapping based association studies of functionally plausible candidate gene groups (e.g. immune function genes) as well as more far reaching genome-wide association studies will be necessary to form the basis upon which the genetic predisposition to PBC can be defined. This first set of experimental data will provide the means for future fine mapping studies, resequencing efforts, functional experimentation, and elucidation of gene-environment and gene-gene interaction; perhaps paving new paths in PBC research.

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“…Importantly, this was observed in diseases with different organ specificities, including PBC, 19 scleroderma and autoimmune thyroid disease. 20 Loss of an X chromosome is indeed preferential and more frequently involves a parentally inherited one, 21 suggesting a possible critical involvement of X-chromosome gene product defects in the female preponderance of PBC and other autoimmune diseases, although new factors, such as microRNAs 22 or epigenetics, 23,24 should not be overlooked. Other authors have suggested that women affected with specific female-preponderant autoimmune diseases, i.e., scleroderma, manifest a skewed XCI pattern in their peripheral white blood cells.…”

Section: Introductionmentioning

confidence: 99%