Your search keyword '"cholangiocytes"' showing total 636 results

1. Bile Acids-Based Therapies for Primary Sclerosing Cholangitis: Current Landscape and Future Developments.

Author

Fiorucci, Stefano, Urbani, Ginevra, Di Giorgio, Cristina, Biagioli, Michele, and Distrutti, Eleonora

Subjects

*BILE ducts, *BILE acids, *URSODEOXYCHOLIC acid, *GUT microbiome, *CHOLANGITIS

Abstract

Primary sclerosing cholangitis (PSC) is a rare, chronic liver disease with no approved therapies. The ursodeoxycholic acid (UDCA) has been widely used, although there is no evidence that the use of UDCA delays the time to liver transplant or increases survival. Several candidate drugs are currently being developed. The largest group of these new agents is represented by FXR agonists, including obeticholic acid, cilofexor, and tropifexor. Other agents that target bile acid metabolism are ASTB/IBAP inhibitors and fibroblasts growth factor (FGF)19 analogues. Cholangiocytes, the epithelial bile duct cells, play a role in PSC development. Recent studies have revealed that these cells undergo a downregulation of GPBAR1 (TGR5), a bile acid receptor involved in bicarbonate secretion and immune regulation. Additional agents under evaluation are PPARs (elafibranor and seladelpar), anti-itching agents such as MAS-related G-protein–coupled receptors antagonists, and anti-fibrotic and immunosuppressive agents. Drugs targeting gut bacteria and bile acid pathways are also under investigation, given the strong link between PSC and gut microbiota. [ABSTRACT FROM AUTHOR]

Published

2024

2. Current Landscape and Evolving Therapies for Primary Biliary Cholangitis.

Author

Fiorucci, Stefano, Urbani, Ginevra, Di Giorgio, Cristina, Biagioli, Michele, and Distrutti, Eleonora

Subjects

*HEPATIC fibrosis, *BILE ducts, *THERAPEUTICS, *CIRRHOSIS of the liver, *DISEASE susceptibility

Abstract

Primary Biliary Cholangitis (PBC) is a chronic autoimmune liver disorder characterized by progressive cholestatic that, if untreated, can progress to liver fibrosis, cirrhosis and liver decompensation requiring liver transplant. Although the pathogenesis of the disease is multifactorial, there is a consensus that individuals with a genetic predisposition develop the disease in the presence of specific environmental triggers. A dysbiosis of intestinal microbiota is increasingly considered among the potential pathogenic factors. Cholangiocytes, the epithelial cells lining the bile ducts, are the main target of a dysregulated immune response, and cholangiocytes senescence has been recognized as a driving mechanism, leading to impaired bile duct function, in disease progression. Bile acids are also recognized as playing an important role, both in disease development and therapy. Thus, while bile acid-based therapies, specifically ursodeoxycholic acid and obeticholic acid, have been the cornerstone of therapy in PBC, novel therapeutic approaches have been developed in recent years. In this review, we will examine published and ongoing clinical trials in PBC, including the recently approved peroxisome-proliferator-activated receptor (PPAR) agonist, elafibranor and seladelpar. These novel second-line therapies are expected to improve therapy in PBC and the development of personalized approaches. [ABSTRACT FROM AUTHOR]

Published

2024

3. Corrigendum: Cellular heterogeneity and plasticity during NAFLD progression

Author

Hyun-Ju Park, Juyong Choi, Hyunmi Kim, Da-Yeon Yang, Tae Hyeon An, Eun-Woo Lee, Baek-Soo Han, Sang Chul Lee, Won Kon Kim, Kwang-Hee Bae, and Kyoung-Jin Oh

Subjects

NAFLD, heterogeneity, hepatocytes, Cholangiocytes, hepatic stellate cells, Kupffer cells, Biology (General), QH301-705.5

Published

2024

4. The crosstalk between cholangiocytes and hepatic stellate cells promotes the progression of epithelial-mesenchymal transition and periductal fibrosis during Clonorchis sinensis infection

Author

Junyeong Yi, Ji Hoon Jeong, Jihee Won, Seok Chung, and Jhang Ho Pak

Subjects

Clonorchis sinensis, Excretory-secretory products, Cholangiocytes, Hepatic stellate cells, Intercellular crosstalk, Epithelial-mesenchymal transition, Infectious and parasitic diseases, RC109-216

Abstract

A bstract Background Clonorchis sinensis infection is one of the risk factors that provokes chronic inflammation, epithelial hyperplasia, periductal fibrosis and even cholangiocarcinoma (CCA). Disrupted or aberrant intercellular communication among liver-constituting cells leads to pathological states that cause various hepatic diseases. This study was designed to investigate the pathological changes caused by C. sinensis excretory-secretory products (ESPs) in non-cancerous human cell lines (cholangiocytes [H69 cell line] and human hepatic stellate cells [LX2 cell line]) and their intercellular crosstalk, as well the pathological changes in infected mouse liver tissues. Methods The cells were treated with ESPs, following which transforming growth factor beta 1 (TGF-β1) and interleukin-6 (IL-6) secretion levels and epithelial-mesenchymal transition (EMT)- and fibrosis-related protein expression were measured. The ESP-mediated cellular motility (migration/invasion) between two cells was assessed using the Transwell and three-dimensional microfluidic assay models. The livers of C. sinensis-infected mice were stained using EMT and fibrotic marker proteins. Results Treatment of cells with ESPs increased TGF-β1 and IL-6 secretion and the expression of EMT- and fibrosis-related proteins. The ESP-mediated mutual cell interaction further affected the cytokine secretion and protein expression levels and promoted cellular motility. N-cadherin overexpression and collagen fiber deposition were observed in the livers of C. sinensis-infected mice. Conclusions These findings suggest that EMT and biliary fibrosis occur through intercellular communication between cholangiocytes and hepatic stellate cells during C. sinensis infection, promoting malignant transformation and advanced hepatobiliary abnormalities. Graphical Abstract

Published

2024

5. Cholangiocyte organoids to study drug-induced injury

Author

Zhenguo Wang, Chen Xing, Luc J. W. van der Laan, Monique M. A. Verstegen, Bart Spee, and Rosalinde Masereeuw

Subjects

Intrahepatic cholangiocyte organoids, Cholangiocytes, Drug induced bile duct injury, Advanced in vitro model, Chlorpromazine, Bile acid, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract Background Drug induced bile duct injury is a frequently observed clinical problem leading to a wide range of pathological features. During the past decades, several agents have been identified with various postulated mechanisms of bile duct damage, however, mostly still poorly understood. Methods Here, we investigated the mechanisms of chlorpromazine (CPZ) induced bile duct injury using advanced in vitro cholangiocyte cultures. Intrahepatic cholangiocyte organoids (ICOs) were driven into mature cholangiocyte like cells (CLCs), which were exposed to CPZ under cholestatic or non-cholestatic conditions through the addition of a bile acid cocktail. Results CPZ caused loss of monolayer integrity by reducing expression levels of tight junction protein 1 (TJP1), E-cadherin 1 (CDH1) and lysyl oxidase homolog 2 (LOXL2). Loss of zonula occuludens-1 (ZO-1) and E-cadherin was confirmed by immunostaining after exposure to CPZ and rhodamine-123 leakage further confirmed disruption of the cholangiocyte barrier function. Furthermore, oxidative stress seemed to play a major role in the early damage response by CPZ. The drug also decreased expression of three main basolateral bile acid transporters, ABCC3 (ATP binding cassette subfamily C member 3), SLC51A/B (solute carrier family 51 subunit alpha/beta) and multidrug resistance transporter ABCB1 (ATP binding cassette subfamily B member 1), thereby contributing to bile acid accumulation. CPZ did not induce an inflammatory response by itself, but addition of TNFα revealed a synergistic effect. Conclusion These results show that ICOs present a model to identify toxic drugs affecting the bile ducts while providing mechanistic insights into hepatotoxicity.

Published

2024

6. Modulation of hepatic cellular tight junctions via coculture with cholangiocytes enables non-destructive bile recovery.

Author

Tokito, Fumiya, Kiyofuji, Mikito, Choi, Hyunjin, Nishikawa, Masaki, Takezawa, Toshiaki, and Sakai, Yasuyuki

Subjects

*TIGHT junctions, *BILE, *CELL culture, *DRUG interactions, *BILE acids, *LIVER cells, *PHARMACODYNAMICS

Abstract

Estimation of the biliary clearance of drugs and their metabolites in humans is crucial for characterizing hepatobiliary disposition and potential drug-drug interactions. Sandwich-cultured hepatocytes, while useful for in vitro bile analysis, require cell destruction for bile recovery, limiting long-term or repeated dose drug effect evaluations. To overcome this limitation, we investigated the feasibility of coculturing a human hepatic carcinoma cell line (HepG2-NIAS cells) and a human cholangiocarcinoma cell line (TFK-1 cells) using the collagen vitrigel membrane in a variety of coculture configurations. The coculture configuration with physiological bile flow increased the permeability of fluorescein-labeled bile acids (CLF) across the HepG2-NIAS cell layer by approximately 1.2-fold compared to the HepG2-NIAS monoculture. This enhancement was caused by paracellular leakage due to the loosened tight junctions of HepG2-NIAS, confirmed by the use of an inhibitor for bile acid transporters, the increase of permeability of dextran, and the decrease of the transepithelial electrical resistance (TEER) value. Based on the results of loosening hepatic tight junctions via coculture with TFK-1 in the CLF permeability assay, we next attempted to collect the CLF accumulated in the bile canaliculi of HepG2-NIAS. The recovery of the CLF accumulated in the bile canaliculi was increased 1.4 times without disrupting hepatic tight junctions by the coculture of HepG2-NIAS cells and TFK-1 cells compared to the monoculture of HepG2-NIAS cells. This non-destructive bile recovery has the potential as a tool for estimating the biliary metabolite and provides valuable insights to improve in vitro bile analysis. [ABSTRACT FROM AUTHOR]

Published

2024

7. Diagnostic yield and novel candidate genes by next generation sequencing in 166 children with intrahepatic cholestasis.

Author

Zheng, Yucan, Guo, Hongmei, Chen, Leilei, Cheng, Weixia, Yan, Kunlong, Zhang, Zhihua, Li, Mei, Jin, Yu, Hu, Guorui, Wang, Chunli, Zhou, Chunlei, Zhou, Wei, Jia, Zhanjun, Zheng, Bixia, and Liu, Zhifeng

Abstract

Background and aims: Cholestatic liver disease is a leading referral to pediatric liver transplant centers. Inherited disorders are the second most frequent cause of cholestasis in the first month of life. Methods: We retrospectively characterized the genotype and phenotype of 166 participants with intrahepatic cholestasis, and re-analyzed phenotype and whole-exome sequencing (WES) data from patients with previously undetermined genetic etiology for newly published genes and novel candidates. Functional validations of selected variants were conducted in cultured cells. Results: Overall, we identified disease-causing variants in 31% (52/166) of our study participants. Of the 52 individuals, 18 (35%) had metabolic liver diseases, 9 (17%) had syndromic cholestasis, 9 (17%) had progressive familial intrahepatic cholestasis, 3 (6%) had bile acid synthesis defects, 3(6%) had infantile liver failure and 10 (19%) had a phenocopy of intrahepatic cholestasis. By reverse phenotyping, we identified a de novo variant c.1883G > A in FAM111B of a case with high glutamyl transpeptidase (GGT) cholestasis. By re-analyzing WES data, two patients were newly solved, who had compound heterozygous variants in recently published genes KIF12 and USP53, respectively. Our additional search for novel candidates in unsolved WES families revealed four potential novel candidate genes (NCOA6, CCDC88B, USP24 and ATP11C), among which the patients with variants in NCOA6 and ATP11C recapitulate the cholestasis phenotype in mice models. Conclusions: In a single-center pediatric cohort, we identified monogenic variants in 22 known human intrahepatic cholestasis or phenocopy genes, explaining up to 31% of the intrahepatic cholestasis patients. Our findings suggest that re-evaluating existing WES data from well-phenotyped patients on a regular basis can increase the diagnostic yield for cholestatic liver disease in children. [ABSTRACT FROM AUTHOR]

Published

2024

8. The crosstalk between cholangiocytes and hepatic stellate cells promotes the progression of epithelial-mesenchymal transition and periductal fibrosis during Clonorchis sinensis infection.

Author

Yi, Junyeong, Jeong, Ji Hoon, Won, Jihee, Chung, Seok, and Pak, Jhang Ho

Abstract

Abstract: Background: Clonorchis sinensis infection is one of the risk factors that provokes chronic inflammation, epithelial hyperplasia, periductal fibrosis and even cholangiocarcinoma (CCA). Disrupted or aberrant intercellular communication among liver-constituting cells leads to pathological states that cause various hepatic diseases. This study was designed to investigate the pathological changes caused by C. sinensis excretory-secretory products (ESPs) in non-cancerous human cell lines (cholangiocytes [H69 cell line] and human hepatic stellate cells [LX2 cell line]) and their intercellular crosstalk, as well the pathological changes in infected mouse liver tissues. Methods: The cells were treated with ESPs, following which transforming growth factor beta 1 (TGF-β1) and interleukin-6 (IL-6) secretion levels and epithelial-mesenchymal transition (EMT)- and fibrosis-related protein expression were measured. The ESP-mediated cellular motility (migration/invasion) between two cells was assessed using the Transwell and three-dimensional microfluidic assay models. The livers of C. sinensis-infected mice were stained using EMT and fibrotic marker proteins. Results: Treatment of cells with ESPs increased TGF-β1 and IL-6 secretion and the expression of EMT- and fibrosis-related proteins. The ESP-mediated mutual cell interaction further affected the cytokine secretion and protein expression levels and promoted cellular motility. N-cadherin overexpression and collagen fiber deposition were observed in the livers of C. sinensis-infected mice. Conclusions: These findings suggest that EMT and biliary fibrosis occur through intercellular communication between cholangiocytes and hepatic stellate cells during C. sinensis infection, promoting malignant transformation and advanced hepatobiliary abnormalities. [ABSTRACT FROM AUTHOR]

Published

2024

9. Cholangiocyte Organoids: The New Frontier in Regenerative Medicine for the Study and Treatment of Cholangiopathies.

Author

Babboni, Serena, Vacca, Pier Giuseppe, Simonini, Ludovica, Pezzati, Daniele, Martinelli, Caterina, Frongillo, Francesco, Bianco, Giuseppe, Marciano, Emanuele, Basta, Giuseppina, Ghinolfi, Davide, and Del Turco, Serena

Subjects

*REGENERATIVE medicine, *ORGANOIDS, *HEPATIC fibrosis, *BILIARY tract, *CELL communication, *CHOLANGITIS

Abstract

Cholangiopathies include a group of chronic progressive disorders, affecting the cholangiocytes, the epithelial cells that line the biliary tree, leading to liver parenchymal fibrosis and eventually end-stage liver disease necessitating transplantation. Experimental modeling of these multifactorial cholestatic diseases faces challenges due to the lack of adequate experimental in vitro and in vivo models. A novel approach employs three-dimensional organoid systems that offer several advantages for modeling disease and testing drug response in vitro. Organoids mimic intercellular communication, replicate the architecture of organs, and maintain the cell's original phenotype. Cholangiocyte organoids provide an in vitro model to study the pathogenesis and pharmacotherapeutic treatment of cholangiopathies and show great promise for regenerative therapies. In particular, patient-derived organoids allow personalized medicine approaches and the study of individual disease characteristics. This review highlights the significance of cholangiocyte organoid models in advancing our understanding of cholangiopathies and driving advancements in regenerative medicine strategies. [ABSTRACT FROM AUTHOR]

Published

2024

10. Cholangiocyte organoids to study drug-induced injury.

Author

Wang, Zhenguo, Xing, Chen, van der Laan, Luc J. W., Verstegen, Monique M. A., Spee, Bart, and Masereeuw, Rosalinde

Subjects

*ATP-binding cassette transporters, *P-glycoprotein, *LYSYL oxidase, *BILE ducts

Abstract

Background: Drug induced bile duct injury is a frequently observed clinical problem leading to a wide range of pathological features. During the past decades, several agents have been identified with various postulated mechanisms of bile duct damage, however, mostly still poorly understood. Methods: Here, we investigated the mechanisms of chlorpromazine (CPZ) induced bile duct injury using advanced in vitro cholangiocyte cultures. Intrahepatic cholangiocyte organoids (ICOs) were driven into mature cholangiocyte like cells (CLCs), which were exposed to CPZ under cholestatic or non-cholestatic conditions through the addition of a bile acid cocktail. Results: CPZ caused loss of monolayer integrity by reducing expression levels of tight junction protein 1 (TJP1), E-cadherin 1 (CDH1) and lysyl oxidase homolog 2 (LOXL2). Loss of zonula occuludens-1 (ZO-1) and E-cadherin was confirmed by immunostaining after exposure to CPZ and rhodamine-123 leakage further confirmed disruption of the cholangiocyte barrier function. Furthermore, oxidative stress seemed to play a major role in the early damage response by CPZ. The drug also decreased expression of three main basolateral bile acid transporters, ABCC3 (ATP binding cassette subfamily C member 3), SLC51A/B (solute carrier family 51 subunit alpha/beta) and multidrug resistance transporter ABCB1 (ATP binding cassette subfamily B member 1), thereby contributing to bile acid accumulation. CPZ did not induce an inflammatory response by itself, but addition of TNFα revealed a synergistic effect. Conclusion: These results show that ICOs present a model to identify toxic drugs affecting the bile ducts while providing mechanistic insights into hepatotoxicity. [ABSTRACT FROM AUTHOR]

Published

2024

11. Opisthorchis viverrini excretory-secretory products suppress GLUT8 of cholangiocytes.

Author

Kha, Sandy, Chaiyadet, Sujittra, Saichua, Prasert, Tangkawatana, Sirikachorn, Sripa, Banchob, and Suttiprapa, Sutas

Abstract

Opisthorchis viverrini infection and the subsequent bile duct cancer it induces remains a significant public health problem in Southeast Asia. Opisthorchiasis has been reported to cause reduced plasma glucose levels among infected patients. The underlying mechanism for this phenomenon is unclear. In the present study, evidence is presented to support the hypothesis that O. viverrini exploits host cholangiocyte glucose transporters (GLUTs) in a similar manner to that of rodent intestinal nematodes, to feed on unabsorbed glucose in the bile for survival. GLUT levels in a cholangiocyte H69 cell line co-cultured with excretory-secretory products of O. viverrini were examined using qPCR and immunoblotting. GLUT 8 mRNA and expressed proteins were found to be downregulated in H69 cells in the presence of O. viverrini. This suggests that O. viverrini alters glucose metabolism in cells within its vicinity by limiting transporter expression resulting in increased bile glucose that it can utilize and potentially explains the previously reported anti-insulin effect of opisthorchiasis. [ABSTRACT FROM AUTHOR]

Published

2024

12. Unraveling the complexities of fibrosis and ductular reaction in liver disease: pathogenesis, mechanisms, and therapeutic insights.

Author

Marakovits, Corinn and Francis, Heather

Subjects

*LIVER diseases, *HEPATIC fibrosis, *BILIARY atresia, *BILE ducts, *MYOFIBROBLASTS, *LIVER cells, *FIBROSIS

Abstract

Ductular reaction and fibrosis are hallmarks of many liver diseases including primary sclerosing cholangitis, primary biliary cholangitis, biliary atresia, alcoholic liver disease, and metabolic dysfunction-associated steatotic liver disease/metabolic dysfunction- associated steatohepatitis. Liver fibrosis is the accumulation of extracellular matrix often caused by excess collagen deposition by myofibroblasts. Ductular reaction is the proliferation of bile ducts (which are composed of cholangiocytes) during liver injury. Many other cells including hepatic stellate cells, hepatocytes, hepatic progenitor cells, mesenchymal stem cells, and immune cells contribute to ductular reaction and fibrosis by either directly or indirectly interacting with myofibroblasts and cholangiocytes. This review summarizes the recent findings in cellular links between ductular reaction and fibrosis in numerous liver diseases. [ABSTRACT FROM AUTHOR]

Published

2024

13. Bile Acids-Based Therapies for Primary Sclerosing Cholangitis: Current Landscape and Future Developments

Author

Stefano Fiorucci, Ginevra Urbani, Cristina Di Giorgio, Michele Biagioli, and Eleonora Distrutti

Subjects

bile acids, biliary fibrosis, cholangiocytes, cholestasis, farnesoid X receptor, GPBAR1 (TGR5), Cytology, QH573-671

Abstract

Primary sclerosing cholangitis (PSC) is a rare, chronic liver disease with no approved therapies. The ursodeoxycholic acid (UDCA) has been widely used, although there is no evidence that the use of UDCA delays the time to liver transplant or increases survival. Several candidate drugs are currently being developed. The largest group of these new agents is represented by FXR agonists, including obeticholic acid, cilofexor, and tropifexor. Other agents that target bile acid metabolism are ASTB/IBAP inhibitors and fibroblasts growth factor (FGF)19 analogues. Cholangiocytes, the epithelial bile duct cells, play a role in PSC development. Recent studies have revealed that these cells undergo a downregulation of GPBAR1 (TGR5), a bile acid receptor involved in bicarbonate secretion and immune regulation. Additional agents under evaluation are PPARs (elafibranor and seladelpar), anti-itching agents such as MAS-related G-protein–coupled receptors antagonists, and anti-fibrotic and immunosuppressive agents. Drugs targeting gut bacteria and bile acid pathways are also under investigation, given the strong link between PSC and gut microbiota.

Published

2024

14. Current Landscape and Evolving Therapies for Primary Biliary Cholangitis

Author

Stefano Fiorucci, Ginevra Urbani, Cristina Di Giorgio, Michele Biagioli, and Eleonora Distrutti

Subjects

cholangiocytes, cholestasis, farnesoid-x-receptor (FXR), macrophages, peroxisome-proliferator-associated receptors (PPAR), T cells, Cytology, QH573-671

Abstract

Primary Biliary Cholangitis (PBC) is a chronic autoimmune liver disorder characterized by progressive cholestatic that, if untreated, can progress to liver fibrosis, cirrhosis and liver decompensation requiring liver transplant. Although the pathogenesis of the disease is multifactorial, there is a consensus that individuals with a genetic predisposition develop the disease in the presence of specific environmental triggers. A dysbiosis of intestinal microbiota is increasingly considered among the potential pathogenic factors. Cholangiocytes, the epithelial cells lining the bile ducts, are the main target of a dysregulated immune response, and cholangiocytes senescence has been recognized as a driving mechanism, leading to impaired bile duct function, in disease progression. Bile acids are also recognized as playing an important role, both in disease development and therapy. Thus, while bile acid-based therapies, specifically ursodeoxycholic acid and obeticholic acid, have been the cornerstone of therapy in PBC, novel therapeutic approaches have been developed in recent years. In this review, we will examine published and ongoing clinical trials in PBC, including the recently approved peroxisome-proliferator-activated receptor (PPAR) agonist, elafibranor and seladelpar. These novel second-line therapies are expected to improve therapy in PBC and the development of personalized approaches.

Published

2024

15. Spatially segregated defects and IGF1-responsiveness of hilar and peripheral biliary organoids from a model of Alagille syndrome.

Author

Iqbal, Afshan, Van Hul, Noemi, Belicova, Lenka, Corbat, Agustin A., Hankeova, Simona, and Andersson, Emma R.

Subjects

*INTRAHEPATIC bile ducts, *ORGANOIDS, *BILE ducts, *RNA sequencing, *TRANSCRIPTOMES, *BIOACTIVE glasses

Abstract

Background & Aims: Alagille syndrome (ALGS) manifests with peripheral intrahepatic bile duct (IHBD) paucity, which can spontaneously resolve. In a model for ALGS, Jag1Ndr/Ndr mice, this occurs with distinct architectural mechanisms in hilar and peripheral IHBDs. Here, we investigated region-specific IHBD characteristics and addressed whether IGF1, a cholangiocyte mitogen that is downregulated in ALGS and in Jag1Ndr/Ndr mice, can improve biliary outcomes. Methods: Intrahepatic cholangiocyte organoids (ICOs) were derived from hilar and peripheral adult Jag1+/+ and Jag1Ndr/Ndr livers (hICOs and pICOs, respectively). ICOs were grown in Matrigel or microwell arrays, and characterized using bulk RNA sequencing, immunofluorescence, and high throughput analyses of nuclear sizes. ICOs were treated with IGF1, followed by analyses of growth, proliferation, and death. CellProfiler and Python scripts were custom written for image analyses. Key results were validated in vivo by immunostaining. Results: Cell growth assays and transcriptomics demonstrated that Jag1Ndr/Ndr ICOs were less proliferative than Jag1+/+ ICOs. IGF1 specifically rescued survival and growth of Jag1Ndr/Ndr pICOs. Jag1Ndr/Ndr hICOs were the least proliferative, with lower Notch signalling and an enrichment of hepatocyte signatures and IGF uptake/transport pathways. In vitro ( Jag1Ndr/Ndr hICOs) and in vivo ( Jag1Ndr/Ndr hilar portal tracts) analyses revealed ectopic HNF4a+ hepatocytes. Conclusions: Hilar and peripheral Jag1Ndr/Ndr ICOs exhibit differences in Notch signalling status, proliferation, and cholangiocyte commitment which may result in cholangiocyte- to-hepatocyte transdifferentiation. While Jag1Ndr/Ndr pICOs can be rescued by IGF1, hICOs are unresponsive, perhaps due to their hepatocyte-like state and/or expression of IGF transport components. IGF1 represents a potential therapeutic for peripheral bile ducts. [ABSTRACT FROM AUTHOR]

Published

2024

16. Mechanistic insights into Cholangiocyte pathobiology following Primary Cilia loss

Author

Waddell, Scott Hamilton, Mill, Pleasantine, and Boulter, Luke

Subjects

Primary cilia, cholangiocarcinoma, liver disease, mouse models, cholangiocytes, intrahepatic CC

Abstract

Primary cilia (PC) are sensory organelles that project from the apical membranes of most mammalian cell types and are essential for proper development of the embryo and homeostasis in adult tissues. Disruption to cilia function drives a myriad of diseases termed ciliopathies, multi-syndromic pathologies that affect numerous organs, including the liver. In the liver, PC are found on cholangiocytes (epithelial cells of the biliary tract) and their dysfunction leads to hepatic cyst development, which can cause abdominal pain and leads to a low quality of life for patients with polycystic liver disease. Additionally, PC are lost from cholangiocytes in malignant disease (cholangiocarcinoma; CC; an aggressive liver cancer for which there is no cure), and previous work by others has implied that PC function as tumour suppressor organelles. While some molecular mechanisms underlying PC dysfunction in biliary disease have been identified, the full extent to which PC are responsible for the initiation and maintenance of diseased states in the liver is not clear. Understanding the molecular role of PC in these pathologies will lead to the identification of new molecular processes that could be modulated to limit disease progression and improve patient outcomes. Here, I generated a novel mouse model to conditionally delete PC from the biliary tract to drive hepatic cystogenesis. I profiled the transcriptomes of normal and cystic cholangiocytes at single cell resolution to develop a global understanding of the underlying mechanisms of cystogenesis. From this dataset and subsequent validation I identified that cholangiocytes lacking PC expand their basement membrane by the cell autonomous expression of a number of extracellular matrix (ECM) and matricellular proteins and also upregulate integrin expression to sense changes to their extracellular environment. My data shows that this external change resulted in actin cytoskeletal rearrangements and I propose that this is the basis of morphological changes at the tissue level to support cyst formation. To address the relevance of PC in malignant disease, I developed a new transgenic model of intrahepatic CC (ICC) where PC could be deleted specifically in cancer cells. Loss of PC compounded with loss of Trp53 and Pten and liver injury to increase tumour burden. RNA sequencing showed that tumours without PC do not increase proliferation, but do upregulate progenitor markers and downregulate immunoregulatory genes. This indicates that PC-loss allows tumour cells to maintain an immunologically cold microenvironment and implicates PC-loss in the immunomodulatory landscape of ICC. I then aimed to understand if PC loss can synergise with liver injury (in the presence of tumour suppressors Trp53 and Pten) to initiate tumorigenesis. While PC loss exacerbated biliary disease on the background of tissue damage, I show no evidence of tumour initiation. The work presented here shows that PC dysfunction in the biliary tract supports cyst development through cell autonomous signalling, initiated by modification to the extracellular matrix, which then influences the actin cytoskeleton and biliary morphology. Secondly, PC loss in tumorigenesis exacerbates disease and allows ICC cells to modify their immune microenvironment. Together, this work highlights the molecular relevance of PC dysfunction in polycystic liver disease and ICC, and identifies a number of new research avenues that can be explored to treat these diseases.

Published

2022

17. A beneficial response of fetal wound healing gone bad in the bile duct: The overarching cause of biliary atresia?

Author

Trampert, David C. and Beuers, Ulrich

Subjects

*BILIARY atresia, *BILE ducts, *WOUND healing, *EXTRACELLULAR matrix, *HYALURONIC acid

Published

2024

18. The role of miRNAs in the development of cholangiopathies. Part 1

Author

A.E. Abaturov and V.L. Babуch

Subjects

microrna, mirna, mir, cholangiopathy, cholangiocytes, primary sclerosing cholangitis, primary biliary cholangitis, review, Pediatrics, RJ1-570

Abstract

The role of miRNA in the development of cholangiopathies is given in the scientific review. This article discusses the role of miRNA in primary sclerosing cholangitis and primary biliary cho­langitis. To write the article, information was searched using Scopus, Web of Science, MedLine, PubMed, Google Scholar, Embase, Global Health, The Cochrane Library databases. The authors state that in hepatobiliary diseases, namely cholangiopathies, micro-RNAs affect the regulation of hepatocyte, cholangiocyte proliferation, cell cycle, inflammatory processes, fibrosis, chemoresistance and cell survival. Researchers have determined that patients with primary sclerosing cholangitis have significantly increased levels of miR-26a, miR-30b, miR-126, miR-122, miR-194, miR-1281 in blood serum and miR-412, miR-640, miR-1537 and miR-3189 in the bile of relatively healthy individuals. It is known that the number of differentially expressed miRNAs in patients with primary biliary cholangitis reaches 97, of which the most diagnostically significant is miR-139-5p. Scientists note that increased miR-139-5p expression in hepatocytes correlates with increased production of TNF-α and repression of c-FOS gene transcription. It is stated that the researchers proposed an alternative hypothesis of miRNA-mediated induction of the inflammatory reaction of the bile ducts in primary biliary cholangitis. The hypothesis is presented that the activity of the generation of miR-106b-5p, miR-20a-5p, and miR-93-5p, which perform key regulatory functions in it, is the basis of the functioning of the miRNA-mRNA network in primary biliary cholangitis. Thus, the data of modern research indicate that cholangiopathies are accompanied by a change in the spectrum of production of various micro-RNAs that regulate the activation of inflammation, regeneration, proliferation, apoptosis of hepatocytes and cholangiocytes. A decrease or increase in the level of some micro-RNA expression is critical in the pathological processes that occur in primary sclerosing cholangitis and primary biliary cholangitis, but micro-RNAs can be not only markers, but also targets of these processes.

Published

2023

19. Autophagy impairment in human bile duct carcinoma cells.

Author

Petrungaro, Simonetta, de Franchis, Valerio, Filippini, Antonio, Facchiano, Antonio, Gaudio, Eugenio, and Giampietri, Claudia

Subjects

BILE ducts, AUTOPHAGY, RAPAMYCIN, WESTERN immunoblotting, CARCINOMA, PROTEIN expression

Abstract

Bile duct epithelial cells, named cholangiocytes, may undergo a neoplastic transformation leading to cholangiocarcinoma. The role autophagy plays in cancer is still debated and few information are available in cholangiocarcinoma. We report in vitro data, at least in part validated in vivo,i ndicating that autophagy is impaired in intrahepatic cholangiocarcinoma cells, as compared to healthy cholangiocytes, evaluated through LC3II and p62 Western blot analyses. Autophagy impairment was found to be associated with low expression of TFEB protein and high expression of three proteins i.e., c-FLIP, caspase-10 and cleaved BCLAF-1, as compared to healthy cholangiocytes. We highlight biological effects of autophagy impairment in cholangiocarcinoma showing that autophagy induction, via rapamycin, as well as caspase inhibition, via Q-VD-OPh, are able to reduce proliferation marker PCNA level, colony size and protein content of cultured cholangiocarcinoma cells. The increased protein expression of p62, c-FLIP, caspase-10 observed in vitro in cholangiocarcinoma cells was paralleled by significant increase at gene expression levels in vivo; in fact, significant increase of transcript levels of p62, c-FLIP and caspase-10 was observed in 34 biopsies from human cholangiocarcinoma patients compared to 9 biopsies from 9 healthy controls, as reported in the GEPIA2 public database. The significant increase of p62 level in cholangiocarcinoma was found as a relatively uncommon finding in solid cancers, since it was also found in only 7 cancer types out of 31 cancer types investigated, including melanoma and hepatocarcinoma. In conclusion, we present data suggesting a molecular machinery controlling autophagy in cholangiocytes and autophagy impairment in cholangiocarcinoma. [ABSTRACT FROM AUTHOR]

Published

2023

20. Chuanxiong Rhizoma extracts prevent cholestatic liver injury by targeting H3K9ac-mediated and cholangiocyte-derived secretory protein PAI-1 and FN.

Author

LI, Yajing, MA, Zhi, DING, Mingning, JIA, Kexin, XU, Bing, ZHOU, Fei, LUO, Ranyi, XUE, Xiaoyong, WU, Ruiyu, GAO, Feng, and LI, Xiaojiaoyang

Abstract

Chuanxiong Rhizoma (CX, the dried rhizome of Ligusticum wallichii Franch.), a well-known traditional Chinese medicine, is clinically used for treating cardiovascular, cerebrovascular and hepatobiliary diseases. Cholestatic liver damage is one of the chronic liver diseases with limited effective therapeutic strategies. Currently, little is known about the mechanism links between CX-induced anti-cholestatic action and intercellular communication between cholangiocytes and hepatic stellate cells (HSCs). The study aimed to evaluate the hepatoprotective activity of different CX extracts including the aqueous, alkaloid, phenolic acid and phthalide extracts of CX (CX AE , CX AL , CX PA and CX PHL) and investigate the intercellular communication-related mechanisms by which the most effective extracts work on cholestatic liver injury. The active compounds of different CX extracts were identified by UPLC-MS/MS. A cholestatic liver injury mouse model induced by bile duct ligation (BDL), and transforming growth factor-β (TGF-β)-treated human intrahepatic biliary epithelial cholangiocytes (HIBECs) and HSC cell line (LX-2 cells) were used for in vivo and in vitro studies. Histological and other biological techniques were also applied. The results indicated that CX AE , CX AL and CX PHL significantly reduced ductular reaction (DR) and improved liver fibrosis in the BDL mice. Meanwhile, both CX AE and CX PHL suppressed DR in injured HIBECs and reduced collagen contraction force and the expression of fibrosis biomarkers in LX-2 cells treated with TGF-β. CX PHL suppressed the transcription and transfer of plasminogen activator inhibitor-1 (PAI-1) and fibronectin (FN) from the 'DR-like' cholangiocytes to activated HSCs. Mechanistically, the inhibition of PAI-1 and FN by CX PHL was attributed to the untight combination of the acetyltransferase KAT2A and SMAD3, followdd by the suppression of histone 3 lysine 9 acetylation (H3K9ac)-mediated transcription in cholangiocytes. In conclusion, CX PHL exerts stronger anti-cholestatic activity in vivo and in vitro than other CX extracts, and its protective effect on the intracellular communication between cholangiocytes and HSCs is achieved by reducing KAT2A/H3K9ac-mediated transcription and release of PAI-1 and FN. [ABSTRACT FROM AUTHOR]

Published

2023

21. Impaired hepatocyte regeneration confers lineage plasticity in the biliary epithelium : a study of the transcriptional heterogeneity within the biliary epithelium following injury

Author

Aleksieva, Niya, Forbes, Stuart, and Kaji, Keisuke

Subjects

chronic liver disease, hepatocytes, cholangiocytes, cholangiocyte-derived hepatocytes

Abstract

Chronic liver disease is a major global health burden, accounting for approximately 2 million deaths per year and the prevalence in the United Kingdom is ever-increasing. Currently the only definitive treatment option for patients suffering from chronic liver disease is orthotopic liver transplant. The shortage of suitable donor organs prompts the search for novel disease-modifying and curative therapies. Despite the varying aetiology, chronic liver disease is always characterised by compromised regenerative capacity of hepatocytes - the main functional cell types of the liver. Recent studies highlight the capacity for lineage plasticity of the biliary cells which can act as facultative liver progenitor cells and differentiate into hepatocytes to repair the damaged liver parenchyma. However, it is still unknown whether all biliary cells have a similar regenerative capacity, or a population of pre-committed progenitors exist in the liver. I hypothesise that in the damaged liver the biliary cells are transcriptionally heterogeneous and that differentiation of biliary cells into hepatocytes is underpinned by a modulation of a unique set of genes and signalling pathways. I utilised two established clinically relevant murine models of chronic liver disease to study the mechanisms that underpin the differential regenerative response following diet induced liver injury, depending on the proliferative capacity of the native hepatocytes. I employed bulk transcriptomic and scRNA-Seq technologies to study the transcriptional differences that arise in biliary cells isolated from these models. I identified populations of cells exclusively present in the models in which biliary to hepatocyte differentiation occurs. These results confirm that following liver injury, the biliary cells represent a heterogeneous population and reveal novel potential therapeutic targets that can inform cell therapy and drug discovery campaigns, seeking to develop innovative solutions for the treatment of chronic liver disease by enhancing the endogenous capacity of biliary cells to differentiate into hepatocytes on demand.

Published

2021

22. Cholangiocytes

Author

Pant, AB

Published

2024

23. Autophagy impairment in human bile duct carcinoma cells

Author

Simonetta Petrungaro, Valerio de Franchis, Antonio Filippini, Antonio Facchiano, Eugenio Gaudio, and Claudia Giampietri

Subjects

autophagic genes and proteins, cholangiocytes, proliferation markers, caspase, cancer, Physiology, QP1-981

Abstract

Bile duct epithelial cells, named cholangiocytes, may undergo a neoplastic transformation leading to cholangiocarcinoma. The role autophagy plays in cancer is still debated and few information are available in cholangiocarcinoma. We report in vitro data, at least in part validated in vivo,i ndicating that autophagy is impaired in intrahepatic cholangiocarcinoma cells, as compared to healthy cholangiocytes, evaluated through LC3II and p62 Western blot analyses. Autophagy impairment was found to be associated with low expression of TFEB protein and high expression of three proteins i.e., c-FLIP, caspase-10 and cleaved BCLAF-1, as compared to healthy cholangiocytes. We highlight biological effects of autophagy impairment in cholangiocarcinoma showing that autophagy induction, via rapamycin, as well as caspase inhibition, via Q-VD-OPh, are able to reduce proliferation marker PCNA level, colony size and protein content of cultured cholangiocarcinoma cells. The increased protein expression of p62, c-FLIP, caspase-10 observed in vitro in cholangiocarcinoma cells was paralleled by significant increase at gene expression levels in vivo; in fact, significant increase of transcript levels of p62, c-FLIP and caspase-10 was observed in 34 biopsies from human cholangiocarcinoma patients compared to 9 biopsies from 9 healthy controls, as reported in the GEPIA2 public database. The significant increase of p62 level in cholangiocarcinoma was found as a relatively uncommon finding in solid cancers, since it was also found in only 7 cancer types out of 31 cancer types investigated, including melanoma and hepatocarcinoma. In conclusion, we present data suggesting a molecular machinery controlling autophagy in cholangiocytes and autophagy impairment in cholangiocarcinoma.

Published

2023

24. Proteomic Modulation in TGF-β-Treated Cholangiocytes Induced by Curcumin Nanoparticles.

Author

Ceccherini, Elisa, Signore, Giovanni, Tedeschi, Lorena, Vozzi, Federico, Di Giorgi, Nicoletta, Michelucci, Elena, Cecchettini, Antonella, and Rocchiccioli, Silvia

Subjects

*CURCUMIN, *PROTEOMICS, *APOPTOSIS, *MASS spectrometry, *NANOPARTICLES, *PROTEIN expression, *PLANT polyphenols

Abstract

Curcumin is a natural polyphenol that exhibits a variety of beneficial effects on health, including anti-inflammatory, antioxidant, and hepato-protective properties. Due to its poor water solubility and membrane permeability, in the present study, we prepared and characterized a water-stable, freely dispersible nanoformulation of curcumin. Although the potential of curcumin nanoformulations in the hepatic field has been studied, there are no investigations on their effect in fibrotic pathological conditions involving cholangiocytes. Exploiting an in vitro model of transforming growth factor-β (TGF-β)-stimulated cholangiocytes, we applied the Sequential Window Acquisition of All Theoretical Mass Spectra (SWATH-MS)-based quantitative proteomic approaches to study the proteome modulation induced by curcumin nanoformulation. Our results confirmed the well-documented anti-inflammatory properties of this nutraceutic, highlighting the induction of programmed cell death as a mechanism to counteract the cellular damages induced by TGF-β. Moreover, curcumin nanoformulation positively influenced the expression of several proteins involved in TGF-β-mediated fibrosis. Given the crucial importance of deregulated cholangiocyte functions during cholangiopathies, our results provide the basis for a better understanding of the mechanisms associated with this pathology and could represent a rationale for the development of more targeted therapies. [ABSTRACT FROM AUTHOR]

Published

2023

25. Galanin System in the Human Bile Duct and Perihilar Cholangiocarcinoma.

Author

Huber, Sara, Fitzner, Theresia, Feichtinger, René G., Hochmann, Sarah, Kraus, Theo, Sotlar, Karl, Kofler, Barbara, and Varga, Martin

Subjects

*BILE ducts, *GALANIN, *CHOLANGIOCARCINOMA, *IMMUNOSTAINING, *PEPTIDES

Abstract

Background: Perihilar cholangiocarcinoma (pCCA) is characterised by poor outcomes. Early diagnosis is essential for patient survival. The peptide galanin (GAL) and its receptors GAL1–3 are expressed in various tumours. Detailed characterisation of the GAL system in pCCA is lacking. Our study sought to characterise GAL and GAL1–3 receptor (GAL1–3–R) expression in the healthy human bile duct, in cholestasis and pCCA. Methods: Immunohistochemical staining was performed in healthy controls (n = 5) and in the peritumoural tissues (with and without cholestasis) (n = 20) and tumour tissues of pCCA patients (n = 33) using validated antibodies. The score values of GAL and GAL1–3–R expression were calculated and statistically evaluated. Results: GAL and GAL1–R were expressed in various bile duct cell types. GAL2–R was only slightly but still expressed in almost all the examined tissues, and GAL3–R specifically in cholangiocytes and capillaries. In a small pCCA patient cohort (n = 18), high GAL expression correlated with good survival, whereas high GAL3–R correlated with poor survival. Conclusions: Our in-depth characterisation of the GAL system in the healthy human biliary duct and pCCA in a small patient cohort revealed that GAL and GAL3–R expression in tumour cells of pCCA patients could potentially represent suitable biomarkers for survival. [ABSTRACT FROM AUTHOR]

Published

2023

26. Liver cell therapies: cellular sources and grafting strategies.

Author

Zhang, Wencheng, Cui, Yangyang, Du, Yuan, Yang, Yong, Fang, Ting, Lu, Fengfeng, Kong, Weixia, Xiao, Canjun, Shi, Jun, Reid, Lola M., and He, Zhiying

Abstract

The liver has a complex cellular composition and a remarkable regenerative capacity. The primary cell types in the liver are two parenchymal cell populations, hepatocytes and cholangiocytes, that perform most of the functions of the liver and that are helped through interactions with non-parenchymal cell types comprising stellate cells, endothelia and various hemopoietic cell populations. The regulation of the cells in the liver is mediated by an insoluble complex of proteins and carbohydrates, the extracellular matrix, working synergistically with soluble paracrine and systemic signals. In recent years, with the rapid development of genetic sequencing technologies, research on the liver's cellular composition and its regulatory mechanisms during various conditions has been extensively explored. Meanwhile breakthroughs in strategies for cell transplantation are enabling a future in which there can be a rescue of patients with end-stage liver diseases, offering potential solutions to the chronic shortage of livers and alternatives to liver transplantation. This review will focus on the cellular mechanisms of liver homeostasis and how to select ideal sources of cells to be transplanted to achieve liver regeneration and repair. Recent advances are summarized for promoting the treatment of end-stage liver diseases by forms of cell transplantation that now include grafting strategies. [ABSTRACT FROM AUTHOR]

Published

2023

27. Inhibiting Wnt Signaling Reduces Cholestatic Injury by Disrupting the Inflammatory AxisSummary

Author

Mary Ayers, Karis Kosar, Yuhua Xue, Chhavi Goel, Matthew Carson, Elizabeth Lee, Silvia Liu, Eva Brooks, Pamela Cornuet, Michael Oertel, Bharat Bhushan, and Kari Nejak-Bowen

Subjects

Cholangiocytes, Bile Acids, Farnesoid X Receptor, β-catenin, Nuclear Factor Kappa κB, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: β-Catenin, the effector molecule of the Wnt signaling pathway, has been shown to play a crucial role in bile acid homeostasis through direct inhibition of farnesoid X receptor (FXR), which has pleiotropic effects on bile acid homeostasis. We hypothesize that simultaneous suppression of β-catenin signaling and activation of FXR in a mouse model of cholestasis will reduce injury and biliary fibrosis through inhibition of bile acid synthesis. Methods: To induce cholestasis, we performed bile duct ligation (BDL) on wild-type male mice. Eight hours after surgery, mice received FXR agonists obeticholic acid, tropifexor, or GW-4064 or Wnt inhibitor Wnt-C59. Severity of cholestatic liver disease and expression of target genes were evaluated after either 5 days or 12 days of treatment. Results: We found that although the FXR agonists worsened BDL-induced injury and necrosis after 5 days, Wnt-C59 did not. After 12 days of BDL, Wnt-C59 treatment, but not GW-4064 treatment, reduced both the number of infarcts and the number of inflammatory cells in liver. RNA sequencing analysis of whole livers revealed a notable suppression of nuclear factor kappa B signaling when Wnt signaling is inhibited. We then analyzed transcriptomic data to identify a cholangiocyte-specific signature in our model and demonstrated that Wnt-C59–treated livers were enriched for genes expressed in quiescent cholangiocytes, whereas genes expressed in activated cholangiocytes were enriched in BDL alone. A similar decrease in biliary injury and inflammation occurred in Mdr2 KO mice treated with Wnt-C59. Conclusions: Inhibiting Wnt signaling suppresses cholangiocyte activation and disrupts the nuclear factor kappa B–dependent inflammatory axis, reducing cholestatic-induced injury.

Published

2023

28. The immunogenicity of cholangiocyte cellular therapies

Author

Tysoe, Olivia, Saeb-Parsy, Kourosh, and Vallier, Ludovic

Subjects

cellular therapies, immunogenicity, cholangiocytes, stem cells, humanised mice, HLA matching

Abstract

Cholangiocytes are the epithelial cells of the biliary system, responsible for the transport and modification of bile. Cholangiocyte disorders, known as cholangiopathies, are a diverse group of life-threatening conditions characterised by cholestasis, ductopenia and eventual liver failure. There are currently no curative treatments for cholangiopathies aside from liver transplantation and while individual cholangiopathies are rare, together they account for a third of adult and 70% of paediatric liver transplants. There is a scarcity of suitable organs for transplantation, however, so development of cholangiocyte cellular therapies capable of replacing or repairing damaged bile ducts would have significant therapeutic value. The safety of such therapies must be assessed before they are suitable for clinical translation and an essential component of that is an evaluation of immunogenicity. In this dissertation I investigated the immunogenicity of cholangiocyte organoids (COs) from an established system developed within the Vallier lab. I first assessed the survival of COs in vivo and generate CO lines expressing luciferase to allow for real-time bioluminescent imaging in vivo. I characterised the expression of HLA molecules on COs compared to primary cholangiocytes and after exposure to a series of pro-inflammatory environments and demonstrated that expression of HLA molecules is reduced in COs compared to primary cholangiocytes but that exposure to pro-inflammatory cytokines restored high levels of HLA expression. I also showed that physiologically-relevant concentrations of pro-inflammatory cytokines were sufficient to upregulate HLA class II expression on COs. To assess the immunogenicity of COs in a transplant environment I used two humanised mouse models. I demonstrated that these models can induce an immune response against allogeneic COs and compared the response to allogeneic and autologous COs in both models. I identified HLA-matched CO lines and immune cell donors and investigated the impact of HLA-matching on the immunogenicity of CO allografts in a humanised mouse model. Overall, the work presented in this dissertation advances the understanding of the immunogenicity of cholangiocyte organoids, both in terms of their expression of immunogenic antigens and the response towards COs within both an allogeneic and autologous transplantation setting.

Published

2019

29. Bile Acids and Biliary Fibrosis.

Author

Aseem, Sayed Obaidullah, Hylemon, Phillip B., and Zhou, Huiping

Subjects

*BILE acids, *FARNESOID X receptor, *FIBROSIS

Abstract

Biliary fibrosis is the driving pathological process in cholangiopathies such as primary biliary cholangitis (PBC) and primary sclerosing cholangitis (PSC). Cholangiopathies are also associated with cholestasis, which is the retention of biliary components, including bile acids, in the liver and blood. Cholestasis may worsen with biliary fibrosis. Furthermore, bile acid levels, composition and homeostasis are dysregulated in PBC and PSC. In fact, mounting data from animal models and human cholangiopathies suggest that bile acids play a crucial role in the pathogenesis and progression of biliary fibrosis. The identification of bile acid receptors has advanced our understanding of various signaling pathways involved in regulating cholangiocyte functions and the potential impact on biliary fibrosis. We will also briefly review recent findings linking these receptors with epigenetic regulatory mechanisms. Further detailed understanding of bile acid signaling in the pathogenesis of biliary fibrosis will uncover additional therapeutic avenues for cholangiopathies. [ABSTRACT FROM AUTHOR]

Published

2023

30. Cellular heterogeneity and plasticity during NAFLD progression

Author

Hyun-Ju Park, Juyong Choi, Hyunmi Kim, Da-Yeon Yang, Tae Hyeon An, Eun-Woo Lee, Baek-Soo Han, Sang Chul Lee, Won Kon Kim, Kwang-Hee Bae, and Kyoung-Jin Oh

Subjects

NAFLD, heterogeneity, hepatocytes, Cholangiocytes, hepatic stellate cells, Kupffer cells, Biology (General), QH301-705.5

Abstract

Nonalcoholic fatty liver disease (NAFLD) is a progressive liver disease that can progress to nonalcoholic steatohepatitis (NASH), NASH-related cirrhosis, and hepatocellular carcinoma (HCC). NAFLD ranges from simple steatosis (or nonalcoholic fatty liver [NAFL]) to NASH as a progressive form of NAFL, which is characterized by steatosis, lobular inflammation, and hepatocellular ballooning with or without fibrosis. Because of the complex pathophysiological mechanism and the heterogeneity of NAFLD, including its wide spectrum of clinical and histological characteristics, no specific therapeutic drugs have been approved for NAFLD. The heterogeneity of NAFLD is closely associated with cellular plasticity, which describes the ability of cells to acquire new identities or change their phenotypes in response to environmental stimuli. The liver consists of parenchymal cells including hepatocytes and cholangiocytes and nonparenchymal cells including Kupffer cells, hepatic stellate cells, and endothelial cells, all of which have specialized functions. This heterogeneous cell population has cellular plasticity to adapt to environmental changes. During NAFLD progression, these cells can exert diverse and complex responses at multiple levels following exposure to a variety of stimuli, including fatty acids, inflammation, and oxidative stress. Therefore, this review provides insights into NAFLD heterogeneity by addressing the cellular plasticity and metabolic adaptation of hepatocytes, cholangiocytes, hepatic stellate cells, and Kupffer cells during NAFLD progression.

Published

2023

31. MicroRNA-27a-3p targets FoxO signalling to induce tumour-like phenotypes in bile duct cells.

Author

Duwe, Lea, Munoz-Garrido, Patricia, Lewinska, Monika, Lafuente-Barquero, Juan, Satriano, Letizia, Høgdall, Dan, Taranta, Andrzej, Nielsen, Boye S., Ghazal, Awaisa, Matter, Matthias S., Banales, Jesus M., Aldana, Blanca I., Gao, Yu-Tang, Marquardt, Jens U., Roberts, Lewis R., Oliveira, Rui C., Koshiol, Jill, O'Rourke, Colm J., and Andersen, Jesper B.

Subjects

*BILE ducts, *NON-coding RNA, *PHENOTYPES, *GENETIC transcription regulation, *HIERARCHICAL clustering (Cluster analysis)

Abstract

Cholangiocarcinoma (CCA) is a heterogeneous and lethal malignancy, the molecular origins of which remain poorly understood. MicroRNAs (miRs) target diverse signalling pathways, functioning as potent epigenetic regulators of transcriptional output. We aimed to characterise miRNome dysregulation in CCA, including its impact on transcriptome homeostasis and cell behaviour. Small RNA sequencing was performed on 119 resected CCAs, 63 surrounding liver tissues, and 22 normal livers. High-throughput miR mimic screens were performed in three primary human cholangiocyte cultures. Integration of patient transcriptomes and miRseq together with miR screening data identified an oncogenic miR for characterization. MiR-mRNA interactions were investigated by a luciferase assay. MiR-CRISPR knockout cells were generated and phenotypically characterized in vitro (proliferation, migration, colony, mitochondrial function, glycolysis) and in vivo using subcutaneous xenografts. In total, 13% (140/1,049) of detected miRs were differentially expressed between CCA and surrounding liver tissues, including 135 that were upregulated in tumours. CCA tissues were characterised by higher miRNome heterogeneity and miR biogenesis pathway expression. Unsupervised hierarchical clustering of tumour miRNomes identified three subgroups, including distal CCA-enriched and IDH1 mutant-enriched subgroups. High-throughput screening of miR mimics uncovered 71 miRs that consistently increased proliferation of three primary cholangiocyte models and were upregulated in CCA tissues regardless of anatomical location, among which only miR-27a-3p had consistently increased expression and activity in several cohorts. FoxO signalling was predominantly downregulated by miR-27a-3p in CCA, partially through targeting of FOXO1. MiR-27a knockout increased FOXO1 levels in vitro and in vivo , impeding tumour behaviour and growth. The miRNomes of CCA tissues are highly remodelled, impacting transcriptome homeostasis in part through regulation of transcription factors like FOXO1. MiR-27a-3p arises as an oncogenic vulnerability in CCA. Cholangiocarcinogenesis entails extensive cellular reprogramming driven by genetic and non-genetic alterations, but the functional roles of these non-genetic events remain poorly understood. By unveiling global miRNA upregulation in patient tumours and their functional ability to increase proliferation of cholangiocytes, these small non-coding RNAs are implicated as critical non-genetic alterations promoting biliary tumour initiation. These findings identify possible mechanisms for transcriptome rewiring during transformation, with potential implications for patient stratification. [Display omitted] • CCA tissues are characterized by miR upregulation, increased miR biogenesis pathway expression and miR heterogeneity. • Most miRs upregulated in CCA resulted in increased proliferation when introduced into human cholangiocyte models in vitro. • MiR-27a-3p affects FoxO signalling in individuals with CCA in vitro and in vivo. • CRISPR/Cas9 nickase knockout of miR-27a abrogates tumorigenicity in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2023

32. Mesenchymal stem cells: A novel treatment option for primary sclerosing cholangitis.

Author

Lightner, Amy L., Dadgar, Neda, Vaidya, Anil, Simon, Robert, Fulmer, Clifton, Siddiki, Hassan, Narayanan Menon, K. V., Liu, Peter, and Matthew Walsh, R.

Subjects

*STEM cell treatment, *CHOLANGITIS, *BILE ducts, *MESENCHYMAL stem cells, *POSTOPERATIVE period, *LIVER cells, *LIVER diseases

Abstract

Primary sclerosing cholangitis (PSC) is a progressive liver disease for which there is no effective therapy. Hepatocytes and cholangiocytes from a PSC patient were cocultured with mesenchymal stem cells (MSCs) to assess in vitro change. A single patient with progressive PSC was treated with 150 million MSCs via direct injection into the common bile duct. Coculture of MSCs with cholangiocytes and hepatocytes showed in vitro improvement. Local delivery of MSCs into a single patient with progressive PSC was safe. Radiographic and endoscopic evaluation showed stable distribution of multifocal structuring in the early postoperative period. MSCs may be effective for the treatment of PSC. [ABSTRACT FROM AUTHOR]

Published

2023

33. Secretin alleviates biliary and liver injury during late-stage primary biliary cholangitis via restoration of secretory processes.

Author

Kennedy, Lindsey, Carpino, Guido, Owen, Travis, Ceci, Ludovica, Kundu, Debjyoti, Meadows, Vik, Kyritsi, Konstantina, Franchitto, Antonio, Onori, Paolo, Isidan, Abdulkadir, Zhang, Wenjun, Ekser, Burcin, Alvaro, Domenico, Gaudio, Eugenio, Gershwin, M. Eric, Francis, Heather, Glaser, Shannon, and Alpini, Gianfranco

Subjects

*TRANSFORMING growth factors-beta, *SECRETIN, *CHOLANGITIS, *LIVER injuries, *HEPATIC fibrosis

Abstract

Primary biliary cholangitis (PBC) is characterised by ductopenia, ductular reaction, impairment of anion exchanger 2 (AE2) and the 'bicarbonate umbrella'. Ductulo-canalicular junction (DCJ) derangement is hypothesised to promote PBC progression. The secretin (Sct)/secretin receptor (SR) axis regulates cystic fibrosis transmembrane receptor (CFTR) and AE2, thus promoting choleresis. We evaluated the role of Sct/SR signalling on biliary secretory processes and subsequent injury in a late-stage PBC mouse model and human samples. At 32 weeks of age, female and male wild-type and dominant-negative transforming growth factor beta receptor II (late-stage PBC model) mice were treated with Sct for 1 or 8 weeks. Bulk RNA-sequencing was performed in isolated cholangiocytes from mouse models. Biliary Sct/SR/CFTR/AE2 expression and bile bicarbonate levels were reduced in late-stage PBC mouse models and human samples. Sct treatment decreased bile duct loss, ductular reaction, inflammation, and fibrosis in late-stage PBC models. Sct reduced hepatic bile acid levels, modified bile acid composition, and restored the DCJ and 'bicarbonate umbrella'. RNA-sequencing identified that Sct promoted mature epithelial marker expression, specifically anterior grade protein 2 (Agr2). Late-stage PBC models and human samples exhibited reduced biliary mucin 1 levels, which were enhanced by Sct treatment. Loss of Sct/SR signalling in late-stage PBC results in a faulty 'bicarbonate umbrella' and reduced Agr2-mediated mucin production. Sct restores cholangiocyte secretory processes and DCJ formation through enhanced mature cholangiocyte phenotypes and bile duct growth. Sct treatment may be beneficial for individuals with late-stage PBC. Secretin (Sct) regulates biliary proliferation and bicarbonate secretion in cholangiocytes via its receptor, SR, and in mouse models and human samples of late-stage primary biliary cholangitis (PBC), the Sct/SR axis is blunted along with loss of the protective 'bicarbonate umbrella'. We found that both short- and long-term Sct treatment ameliorated ductular reaction, immune cell influx, and liver fibrosis in late-stage PBC mouse models. Importantly, Sct treatment promoted bicarbonate and mucin secretion and hepatic bile acid efflux, thus reducing cholestatic and toxic bile acid-associated injury in late-stage PBC mouse models. Our work perpetuates the hypothesis that PBC pathogenesis hinges on secretory defects, and restoration of secretory processes that promote the 'bicarbonate umbrella' may be important for amelioration of PBC-associated damage. [Display omitted] • The biliary secretin/secretin receptor axis is diminished in late-stage PBC. • Secretin treatment alleviates liver damage in a late-stage PBC model. • Secretin restores the protective 'bicarbonate umbrella' in a late-stage PBC model. • Secretin treatment promotes choleresis and restores ductulo-canalicular junctions. • The secretin/secretin receptor axis promotes mature cholangiocyte differentiation. [ABSTRACT FROM AUTHOR]

Published

2023

34. Immunobiology of the biliary tract system.

Author

Björkström, Niklas K.

Subjects

*BILIARY tract, *IMMUNOLOGY, *TECHNOLOGICAL innovations, *CARCINOGENESIS, *DUODENUM

Abstract

The biliary tract is a complex tubular organ system spanning from the liver to the duodenum. It is the site of numerous acute and chronic disorders, many of unknown origin, that are often associated with cancer development and for which there are limited treatment options. Cholangiocytes with proinflammatory capacities line the lumen and specialised types of immune cells reside in close proximity. Recent technological breakthroughs now permit spatiotemporal assessments of immune cells within distinct niches and have increased our understanding of immune cell tissue residency. In this review, a comprehensive overview of emerging knowledge on the immunobiology of the biliary tract system is provided, with a particular emphasis on the role of distinct immune cells in biliary disorders. [ABSTRACT FROM AUTHOR]

Published

2022

35. Results of Intrahepatic Cholangiocarcinoma Resections: a Single-Center Analysis.

Author

Saglam, Kutay, Bag, Yusuf Murat, Bilen, Zafer, Isik, Burak, Aydin, Cemalettin, and Yilmaz, Sezai

Abstract

Introduction: Intrahepatic cholangiocarcinoma (ICC) is the second most common primary neoplasm of the liver after hepatocellular carcinoma (HCC). Although an underlying cause is not usually found, liver flukes, cirrhosis, primary sclerosing cholangitis, and viral hepatitis have been found to increase the risk in recent years. In this study, we aimed to present our experience on ICC and compare the outcomes of patients with a concomitant liver pathology and with incidentally detected ICC. Patients and Methods: Thirty-three patients who underwent surgical resection for ICC were included in the study. Patients were divided into two groups, group one (with concomitant liver disease, n = 13) and group two (incidentally detected ICC, n = 18). Demographics, perioperative findings, pathological properties, recurrence rates, and survival rates were retrospectively analyzed and compared between the groups. Results: The mean age of patients was 59.77 ± 9.81 years, of whom sixteen (51.6%) were males. Thirteen patients (41.9%) had concomitant liver disease, the most common being chronic hepatitis B infection. Eighteen patients (58.1%) had incidentally detected ICC. There were no significant differences between the groups except for follow-up time and recurrence rate. The recurrence rate was significantly higher in the incidentally detected ICC group (61.1% versus 7.7%, p = 0.003). Follow-up time was significantly higher in patients with concomitant liver disease (42 versus 17.5 months, p = 0.007). The mortality rate was higher in the incidentally detected ICC group (55.6 to 23.1%, p = 0.071) but the difference did not reach statistical significance. Conclusion: Surgical resection in ICC patients with underlying liver disease is associated with better prognosis than in incidentally detected ICC patients. Incidental ICC may be a different tumor with different biology, hence the high recurrence rates. [ABSTRACT FROM AUTHOR]

Published

2022

36. Bile Acid Toxicity and Protein Kinases

Author

Engin, Atilla, Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Xiao, Junjie, Series Editor, Engin, Ayse Basak, editor, and Engin, Atilla, editor

Published

2021

37. Imbalanced immunobiological reactivity, infection and mutagenesis factors in the hepatobiliary system affected by a natural focal habitat factor — a trematode invasion by Opisthorchis felineus

Author

A. G. Rybka

Subjects

opisthorchis felineus, opisthorchis, invasion, chronic opisthorchiasis, immunobiological reactivity, immunological memory, memory cells, antigens, antibodies, immune complexes, genotype, genotypic properties, cholangiocytes, proliferation, microflora/ microbiota, primary/secondary bile acids, endogenous mutagens (carcinogens), somatic mutations, carcinogenesis, cholangiocarcinoma, cholangiocarcinogenesis, Infectious and parasitic diseases, RC109-216

Abstract

An interaction between decreasing host anti-infective defense due to long-term invasion with Opisthorchis felineus in the hepatobiliary system, duct bile colonization by microflora and revealing the endogenous mutagenesis (carcinogenesis) factor in bile — secondary bile acids — is considered in the article. The role of organism genotype in pathogen-related immune response to Opisthorchis felineus trematode and helminth development in the hepatobiliary system has been shown. The role of dysregulated mechanisms of tissue homeostasis in induction of compensatory chronic homeostatic proliferation and somatic cell oncogenesis is discussed. The study results evidence that disturbed functioning of regulatory T cells, inhibition of the NK cell effector function and very high functional activity of memory B cells are of great importance in imbalanced host immunobiological reactivity, caused by chronic opistorchis invasion. Decreased host anti-infective protection causes intrahepatic bile duct infection with different bacterial species. Presence of secondary bile acids in hepatobiliary system was associated with biliary bacterial strains inhabiting intestinal tract: Proteus vulgaris, Proteus mirabilis, Citrobacter freundii, Bacteroides alcaligues faecalis, Clostridium, Streptococcus faecalis, Еscherichia coli — gut microflora agents. Participation of microbiota in bile acid biotransformation immediately in the duct bile has been confirmed in experiments in vitro. Experimental methods on Drosophila melanogaster and Salmonella typhimurium strains: TA100, TA98 allowed to find out that bile from chronic opistorchiasis patients exerts higher mutagenic activity compared to control groups. Mutational events in somatic and bacterial cells depend on the presence of secondary bile acids (deoxycholic, lithocholic) in duct bile, as well as the level of total bile acid concentration. The study data confirm the concept by Professor A.A. Shain about the presence of endogenous risk factor for developing primary cholangiocellular liver cancer such as secondary bile acids in the bile of chronic opistorchiasis patients. A concept of cholangiocarcinogenesis, based on mutational events, is added up with disturbance of generative cycle in tissue cells and their differentiation due to decreased chalone factor activity, as well as sensitivity threshold to it. Level of investigation and understanding of mechanisms underlying cholangiocarcinogenesis during chronic opisthorchis invasion will allow to develop pathogenetic approaches to correct homeostasis regulation and prevention of cholangiocarcinomas.

Published

2021

38. Inactivation of caspase 8 in liver parenchymal cells confers protection against murine obstructive cholestasis

Author

Cubero Palero, Francisco Javier, Trautwein, Christian, Cubero Palero, Francisco Javier, and Trautwein, Christian

Abstract

2018 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved. En esta publicación han participado: 1Department of Internal Medicine III, University Hospital, RWTH, Aachen, Germany; 2Department of Immunology, Ophtalmology & ORL,Complutense University School of Medicine, Madrid, Spain; 3 12 de Octubre Health Research Institute (imas12), Madrid, Spain; 4Department of Hepatobiliary Surgery, Nanjing Drum Tower Hospital, The Affiliated Hospital of Nanjing University Medical School, Nanjing Jiangsu, China; 5Department of Anesthesiology and Pain Management, Shanghai East Hospital, Tongji University, Shanghai, China; 6Institute of Pathology, Braunschweig Hospital, Braunschweig, Germany, Background & Aims: Caspase 8 (CASP8) is the apical initiator caspase in death receptor-mediated apoptosis. Strong evidence for a link between death receptor signaling pathways and cholestasis has recently emerged. Herein, we investigated the role of CASP8-dependent and independent pathways during experimental cholestasis. Methods: Liver injury was characterized in a cohort of human sera (n = 28) and biopsies from patients with stage IV primary biliary cholangitis. In parallel, mice with either specific deletion of Casp8 in liver parenchymal cells (Casp8Dhepa) or hepatocytes (Casp8Dhep), and mice with constitutive Ripk3 (Ripk3 / ) deletion, were subjected to surgical ligation of the common bile duct (BDL) from 2 to 28 days. Floxed (Casp8fl/fl) and Ripk3+/+ mice were used as controls. Moreover, the pan-caspase inhibitor IDN-7314 was used, and cell death mechanisms were studied in primary isolated hepatocytes. Results: Overexpression of activated caspase 3, CASP8 and RIPK3 was characteristic of liver explants from patients with primary biliary cholangitis. Twenty-eight days after BDL, Casp8Dhepa mice showed decreased necrotic foci, serum aminotransferase levels and apoptosis along with diminished compensatory proliferation and ductular reaction. These results correlated with a decreased inflammatory profile and ameliorated liver fibrogenesis. A similar phenotype was observed in Ripk3-/- mice. IDN-7314 treatment decreased CASP8 levels but failed to prevent BDL-induced cholestasis, independently of CASP8 in hepatocytes. Conclusion: These findings show that intervention against CASP8 in liver parenchymal cells – specifically in cholangiocytes– might be a beneficial option for treating obstructive cholestasis, while broad pan-caspase inhibition might trigger undesirable side effects. Lay summary: Loss of caspase 8 – a protein involved in programmed cell death – in liver parenchymal cells protects against experimental cholestasis. Therefore, specific pharmacological interve, IZKF, Ministerio de Economía, Comercio y Empresa, Depto. de Inmunología, Oftalmología y ORL, Fac. de Medicina, TRUE, pub

Published

2024

39. Anatomy and Embryology of the Liver

Author

Morini, Sergio, Carpino, Guido, Carotti, Simone, Gaudio, Eugenio, Radu-Ionita, Florentina, editor, Pyrsopoulos, Nikolaos T., editor, Jinga, Mariana, editor, Tintoiu, Ion C., editor, Sun, Zhonghua, editor, and Bontas, Ecaterina, editor

Published

2020

40. Effect of exogenous microflora of the hepatobiliary system on the biochemical composition of bile and lipid peroxidation processes of somatic cell membranes in chronic opisthorchiasis

Author

N. M. Fedorov, A. G. Rybka, and P. B. Zotov

Subjects

opisthorchiasis, cholangiocytes, microflora, bile acids, lipid peroxidation, membrane permeability, cholangiocarcinogenesis, Medicine

Abstract

It has been epidemiologically established that the rate of primary cholangiocarcinomas increases greatly in the ObIrtysh basin which is hyperendemic for helminth Opisthorchis felineus in comparison with other regions where the population is not infested. In this connection chronic opisthorchiasis is considered as facultative liver precancer. The study of cholangiocarcinogenesis mechanisms will allow developing pathogenetic approaches to prevention of this tumor. Aim of the study was to investigate the significance of microbiota of the hepatobiliary tract of chronic opisthorchiasis patients in changing of biochemical composition of bile and investigation of its biological influence on somatic cells membrane. Material and methods. Objects of research: bacteria; inbred mice infected by opisthorchis; samples of bile, cultures of human embryo fibroblasts and splenocytes of inbred mice in vitro; blood plasma; standard primary and secondary bile acids. We studied: species of bacteria colonizing bile ducts; quantitative and qualitative composition of bile acids, and level of diene conjugates and malondialdehyde in duct bile samples; biological activity of bile on processes of lipid peroxidation of cell membranes in vitro; influence of bile and lipid peroxidation products on cytomembrane permeability; activity of antioxidant systems of the body. Results and discussion. It was found out, that bile of patients with chronic opisthorchiasis in majority of cases (77.0 %) was infected by different species of bacteria. In 30.0 % of cases certain types of intestinal bacteria (Proteus vulgaris, P. mirabilis, Citrobacter freundii, Bacteroides alcaligues faecalis, Clostridium, Streptococcus faecalis, Escherichia coli) change biochemical composition of duct bile – deconjugated primary and secondary bile acids and also high level of total bile acids are detected. Bile of the above biochemical composition, against the background of depletion of antioxidant system, induces activation of cell membrane lipid peroxidation processes and significantly increases their permeability to toxic components of bile. These processes are promotor in cholangiocarcinogenesis.

Published

2021

41. Decreased expression of anion exchanger type 2 contributes to biliary epithelial injuries by aggravating intracellular accumulation of bile acids

Author

Long Cheng, Si-ping Chen, Jia-qi Wang, and Tao Wang

Subjects

Liver transplantation, Cholangiocytes, Bile acid transporter, Bile duct, Cold ischemia, Surgery, RD1-811

Published

2022

42. Galanin System in the Human Bile Duct and Perihilar Cholangiocarcinoma

Author

Sara Huber, Theresia Fitzner, René G. Feichtinger, Sarah Hochmann, Theo Kraus, Karl Sotlar, Barbara Kofler, and Martin Varga

Subjects

galanin, galanin receptor, peptide, bile duct, cholangiocytes, cholestasis, Cytology, QH573-671

Abstract

Background: Perihilar cholangiocarcinoma (pCCA) is characterised by poor outcomes. Early diagnosis is essential for patient survival. The peptide galanin (GAL) and its receptors GAL1–3 are expressed in various tumours. Detailed characterisation of the GAL system in pCCA is lacking. Our study sought to characterise GAL and GAL1–3 receptor (GAL1–3–R) expression in the healthy human bile duct, in cholestasis and pCCA. Methods: Immunohistochemical staining was performed in healthy controls (n = 5) and in the peritumoural tissues (with and without cholestasis) (n = 20) and tumour tissues of pCCA patients (n = 33) using validated antibodies. The score values of GAL and GAL1–3–R expression were calculated and statistically evaluated. Results: GAL and GAL1–R were expressed in various bile duct cell types. GAL2–R was only slightly but still expressed in almost all the examined tissues, and GAL3–R specifically in cholangiocytes and capillaries. In a small pCCA patient cohort (n = 18), high GAL expression correlated with good survival, whereas high GAL3–R correlated with poor survival. Conclusions: Our in-depth characterisation of the GAL system in the healthy human biliary duct and pCCA in a small patient cohort revealed that GAL and GAL3–R expression in tumour cells of pCCA patients could potentially represent suitable biomarkers for survival.

Published

2023

43. Proteomic Modulation in TGF-β-Treated Cholangiocytes Induced by Curcumin Nanoparticles

Author

Elisa Ceccherini, Giovanni Signore, Lorena Tedeschi, Federico Vozzi, Nicoletta Di Giorgi, Elena Michelucci, Antonella Cecchettini, and Silvia Rocchiccioli

Subjects

cholangiocytes, curcumin, nanoparticles, TGF-β, proteomics, LC-MS/MS, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Curcumin is a natural polyphenol that exhibits a variety of beneficial effects on health, including anti-inflammatory, antioxidant, and hepato-protective properties. Due to its poor water solubility and membrane permeability, in the present study, we prepared and characterized a water-stable, freely dispersible nanoformulation of curcumin. Although the potential of curcumin nanoformulations in the hepatic field has been studied, there are no investigations on their effect in fibrotic pathological conditions involving cholangiocytes. Exploiting an in vitro model of transforming growth factor-β (TGF-β)-stimulated cholangiocytes, we applied the Sequential Window Acquisition of All Theoretical Mass Spectra (SWATH-MS)-based quantitative proteomic approaches to study the proteome modulation induced by curcumin nanoformulation. Our results confirmed the well-documented anti-inflammatory properties of this nutraceutic, highlighting the induction of programmed cell death as a mechanism to counteract the cellular damages induced by TGF-β. Moreover, curcumin nanoformulation positively influenced the expression of several proteins involved in TGF-β-mediated fibrosis. Given the crucial importance of deregulated cholangiocyte functions during cholangiopathies, our results provide the basis for a better understanding of the mechanisms associated with this pathology and could represent a rationale for the development of more targeted therapies.

Published

2023

44. Liver regeneration: Cellular origin and molecular mechanisms.

Author

Huang, Ru, Zhang, Xin, Gracia‐Sancho, Jordi, and Xie, Wei‐Fen

Subjects

*LIVER regeneration, *LIVER injuries, *SKIN regeneration, *LIVER cells, *LIVER diseases, *WNT genes, *THERAPEUTICS

Abstract

The liver is known as an organ with high proliferation potential. Clarifying the cellular origin and deepening the understanding of liver regeneration mechanisms will help provide new directions for the treatment of liver disease. With the development and application of lineage tracing technology, the specific distribution and dynamic changes of hepatocyte subpopulations in homeostasis and liver injury have been illustrated. Self‐replication of hepatocytes is responsible for the maintenance of liver function and mass under homeostasis. The compensatory proliferation of remaining hepatocytes is the main mechanism of liver regeneration following acute and chronic liver injury. Transdifferentiation between hepatocytes and cholangiocytes has been recognized upon severe chronic liver injury. Wnt/β‐catenin, Hippo/YAP and Notch signalling play essential roles in the maintenance of homeostatic liver and hepatocyte‐to‐cholangiocyte conversion under liver injury. In this review, we summarized the recent studies on cell origin of newly generated hepatocytes and the underlying mechanisms of liver regeneration in homeostasis and liver injury. [ABSTRACT FROM AUTHOR]

Published

2022

45. Protective mechanisms and current clinical evidence of hypothermic oxygenated machine perfusion (HOPE) in preventing post-transplant cholangiopathy.

Author

Schlegel, Andrea, Porte, Robert, and Dutkowski, Philipp

Subjects

*PERFUSION, *BILIARY tract, *LIVER transplantation, *COLD storage, *OVERALL survival

Abstract

The development of cholangiopathies after liver transplantation impacts on the quality and duration of graft and patient survival, contributing to higher costs as numerous interventions are required to treat strictures and infections at the biliary tree. Prolonged donor warm ischaemia time in combination with additional cold storage are key risk factors for the development of biliary strictures. Based on this, the clinical implementation of dynamic preservation strategies is a current hot topic in the field of donation after circulatory death (DCD) liver transplantation. Despite various retrospective studies reporting promising results, also regarding biliary complications, there are only a few randomised-controlled trials on machine perfusion. Recently, the group from Groningen has published the first randomised-controlled trial on hypothermic oxygenated perfusion (HOPE), demonstrating a significant reduction of symptomatic ischaemic cholangiopathies with the use of a short period of HOPE before DCD liver implantation. The most likely mechanism for this important effect, also shown in several experimental studies, is based on mitochondrial reprogramming under hypothermic aerobic conditions, e.g. exposure to oxygen in the cold, with a controlled and slow metabolism of ischaemically accumulated succinate and simultaneous ATP replenishment. This unique feature prevents mitochondrial oxidative injury and further downstream tissue inflammation. HOPE treatment therefore supports livers by protecting them from ischaemia-reperfusion injury (IRI), and thereby also prevents the development of post-transplant biliary injury. With reduced IRI-associated inflammation, recipients are also protected from activation of the innate immune system, with less acute rejections seen after HOPE. [ABSTRACT FROM AUTHOR]

Published

2022

46. Human Cholangiocytes Form a Polarized and Functional Bile Duct on Hollow Fiber Membranes

Author

Zhenguo Wang, João Faria, Luc J. W. van der Laan, Louis C. Penning, Rosalinde Masereeuw, and Bart Spee

Subjects

intrahepatic cholangiocyte organoids, cholangiocytes, bioengineered bile duct, hollow fiber membrane, monolayer, polarity, Biotechnology, TP248.13-248.65

Abstract

Liver diseases affect hundreds of millions of people worldwide; most often the hepatocytes or cholangiocytes are damaged. Diseases of the biliary tract cause severe patient burden, and cholangiocytes, the cells lining the biliary tract, are sensitive to numerous drugs. Therefore, investigations into proper cholangiocyte functions are of utmost importance, which is restricted, in vitro, by the lack of primary human cholangiocytes allowing such screening. To investigate biliary function, including transepithelial transport, cholangiocytes must be cultured as three-dimensional (3D) ductular structures. We previously established murine intrahepatic cholangiocyte organoid-derived cholangiocyte-like cells (CLCs) and cultured them onto polyethersulfone hollow fiber membranes (HFMs) to generate 3D duct structures that resemble native bile ducts at the structural and functional level. Here, we established an efficient, stepwise method for directed differentiation of human intrahepatic cholangiocyte organoids (ICOs) into CLCs. Human ICO-derived CLCs showed key characteristics of cholangiocytes, such as the expression of structural and functional markers, formation of primary cilia, and P-glycoprotein-mediated transport in a polarized fashion. The organoid cultures exhibit farnesoid X receptor (FXR)-dependent functions that are vital to liver bile acid homeostasis in vivo. Furthermore, human ICO-derived CLCs cultured on HFMs in a differentiation medium form tubular architecture with some tight, confluent, and polarized monolayers that better mimic native bile duct characteristics than differentiated cultures in standard 2D or Matrigel-based 3D culture plates. Together, our optimized differentiation protocol to obtain CLC organoids, when applied on HFMs to form bioengineered bile ducts, will facilitate studying cholangiopathies and allow developing therapeutic strategies.

Published

2022

47. Human placenta mesenchymal stem cell-derived exosomes delay H2O2-induced aging in mouse cholangioids

Author

Wenyi Chen, Jiaqi Zhu, Feiyan Lin, Yanping Xu, Bing Feng, Xudong Feng, Xinyu Sheng, Xiaowei Shi, Qiaoling Pan, Jinfeng Yang, Jiong Yu, Lanjuan Li, and Hongcui Cao

Subjects

Exosomes, Primary sclerosing cholangitis, Senescence, Cholangiocytes, Organoids, Medicine (General), R5-920, Biochemistry, QD415-436

Abstract

Abstract Background Cholangiocyte senescence is an important pathological process in diseases such as primary sclerosing cholangitis (PSC) and primary biliary cirrhosis (PBC). Stem cell/induced pluripotent stem cell-derived exosomes have shown anti-senescence effects in various diseases. We applied novel organoid culture technology to establish and characterize cholangiocyte organoids (cholangioids) with oxidative stress-induced senescence and then investigated whether human placenta mesenchymal stem cell (hPMSC)-derived exosomes exerted a protective effect in senescent cholangioids. Methods We identified the growth characteristics of cholangioids by light microscopy and confocal microscopy. Exosomes were introduced concurrently with H2O2 into the cholangioids. Using immunohistochemistry and immunofluorescence staining analyses, we assessed the expression patterns of the senescence markers p16INK4a, p21WAF1/Cip1, and senescence-associated β-galactosidase (SA-β-gal) and then characterized the mRNA and protein expression levels of chemokines and senescence-associated secretory phenotype (SASP) components. Results Well-established cholangioids expressed cholangiocyte-specific markers. Oxidative stress-induced senescence enhanced the expression of the senescence-associated proteins p16INK4a, p21WAF1/Cip1, and SA-β-gal in senescent cholangioids compared with the control group. Treatment with hPMSC-derived exosomes delayed the cholangioid aging progress and reduced the levels of SASP components (i.e., interleukin-6 and chemokine CC ligand 2). Conclusions Senescent organoids are a potential novel model for better understanding senescence progression in cholangiocytes. hPMSC-derived exosomes exert protective effects against senescent cholangioids under oxidative stress-induced injury by delaying aging and reducing SASP components, which might have therapeutic potential for PSC or PBC.

Published

2021

48. Bile Acids and Biliary Fibrosis

Author

Sayed Obaidullah Aseem, Phillip B. Hylemon, and Huiping Zhou

Subjects

biliary fibrosis, bile acids, bile acid receptors, cholangiocytes, cholangiopathies, Cytology, QH573-671

Abstract

Biliary fibrosis is the driving pathological process in cholangiopathies such as primary biliary cholangitis (PBC) and primary sclerosing cholangitis (PSC). Cholangiopathies are also associated with cholestasis, which is the retention of biliary components, including bile acids, in the liver and blood. Cholestasis may worsen with biliary fibrosis. Furthermore, bile acid levels, composition and homeostasis are dysregulated in PBC and PSC. In fact, mounting data from animal models and human cholangiopathies suggest that bile acids play a crucial role in the pathogenesis and progression of biliary fibrosis. The identification of bile acid receptors has advanced our understanding of various signaling pathways involved in regulating cholangiocyte functions and the potential impact on biliary fibrosis. We will also briefly review recent findings linking these receptors with epigenetic regulatory mechanisms. Further detailed understanding of bile acid signaling in the pathogenesis of biliary fibrosis will uncover additional therapeutic avenues for cholangiopathies.

Published

2023

49. Highly Efficient Methods to Culture Mouse Cholangiocytes and Small Intestine Organoids.

Author

Chen, Wenyi, Yao, Qigu, Wang, Ruo, Fen, Bing, Chen, Junyao, Xu, Yanping, Yu, Jiong, Li, Lanjuan, and Cao, Hongcui

Subjects

SMALL intestine, INTRAHEPATIC bile ducts, ORGANOIDS, GALLBLADDER, LUNGS

Abstract

Background: Organoids, which enable disease modeling and drug screening closer to an in vivo environment, can be isolated and grown from organs such as the brain, small intestine, kidney, lungs, and liver. To facilitate the establishment of liver and small intestinal organoids, we developed efficient protocols for cholangiocytes and intestine crypts collecting and organoid culturing. Methods: Cholangiocytes were collected from intrahepatic bile ducts, the gallbladder, and small intestine crypts by gravity settling and multistep centrifugation methods. The cells isolated were embedded with Matrigel and grew in three-dimensional spheroids in a suitable culture medium. The stability of organoid cells was assessed by subculture, cryopreservation, and thawing. RNA and DNA extraction of organoids, as well as immunostaining procedure, were also optimized. Hand-picking procedures were developed and performed to ensure similar growth characteristics of organoids. Results: A large number of cholangiocytes and small intestine crypts were collected under these protocols. Cholangiocytes developed into cyst-like structures after 3–4 days in Matrigel. After 1–2 weeks of cultivation, small intestinal organoids (in-orgs) developed buds and formed a mature structure. Compared to organoids derived from the gallbladder, cholangiocyte organoids (Cho-orgs) from intrahepatic the bile ducts grew more slowly but had a longer culture term, expressed the cholangiocytes markers Krt19 and Krt7, and recapitulated in vivo tissue organization. Conclusions: Our protocols simplified the cell collection procedure and avoided the possibility of exposing tissue-derived stem cells to mechanical damage or chemical injury by gravity settling and multistep centrifugation. In addition, our approach allowed similar growth characteristics of organoids from different mammalian tissue sources. The protocol requires 2–4 weeks to establish a stable organoid growth system. Organoids could be stably passaged, cryopreserved, and recovered under protocol guidance. Besides, the organoids of cholangiocytes and small intestines retained their original tissue characteristics, such as tissue-specific marker expression, which prepares them for further experiments such as preclinical in vitro trials and mechanism research studies. [ABSTRACT FROM AUTHOR]

Published

2022

50. Rescue of chloride and bicarbonate transport by elexacaftor-ivacaftor-tezacaftor in organoid-derived CF intestinal and cholangiocyte monolayers.

Author

Bijvelds, Marcel J.C., Roos, Floris J.M., Meijsen, Kelly F., Roest, Henk P., Verstegen, Monique M.A., Janssens, Hettie M., van der Laan, Luc J.W., and de Jonge, Hugo R.

Abstract

• Intestinal and biliary epithelia were cultured from cystic fibrosis organoids. • Elexacaftor/ivacaftor/tezacaftor rescued chloride transport in both epithelia. • CFTR modulators enhanced bicarbonate transport only in intestinal cells. • Biliary cells secrete bicarbonate and chloride via anoctamin-1, independent of CFTR. In cystic fibrosis (CF), loss of CF transmembrane conductance regulator (CFTR)-dependent bicarbonate secretion precipitates the accumulation of viscous mucus in the lumen of respiratory and gastrointestinal epithelial tissues. We investigated whether the combination of elexacaftor (ELX), ivacaftor (IVA) and tezacaftor (TEZ), apart from its well-documented effect on chloride transport, also restores Phe508del-CFTR-mediated bicarbonate transport. Epithelial monolayers were cultured from intestinal and biliary (cholangiocyte) organoids of homozygous Phe508del-CFTR patients and controls. Transcriptome sequencing was performed, and bicarbonate and chloride transport were assessed in the presence or absence of ELX/IVA/TEZ, using the intestinal current measurement technique. ELX/IVA/TEZ markedly enhanced bicarbonate and chloride transport across intestinal epithelium. In biliary epithelium, it failed to enhance CFTR-mediated bicarbonate transport but effectively rescued CFTR-mediated chloride transport, known to be requisite for bicarbonate secretion through the chloride-bicarbonate exchanger AE2 (SLC4A2), which was highly expressed by cholangiocytes. Biliary but not intestinal epithelial cells expressed an alternative anion channel, anoctamin-1/TMEM16A (ANO1), and secreted bicarbonate and chloride upon purinergic receptor stimulation. ELX/IVA/TEZ has the potential to restore both chloride and bicarbonate secretion across CF intestinal and biliary epithelia and may counter luminal hyper-acidification in these tissues. Graphical abstract [Display omitted]. [ABSTRACT FROM AUTHOR]

Published

2022