Silvia Cagnin scite author profile

The extracellular matrix is a highly reactive scaffold formed by a wide array of multifunctional molecules, encompassing collagens and noncollagenous glycoproteins, proteoglycans, glycosaminoglycans, and polysaccharides. Besides outlining the tissue borders, the extracellular matrix profoundly regulates the behavior of resident cells by transducing mechanical signals, and by integrating multiple cues derived from the microenvironment. Evidence is mounting that changes in the biostructure of the extracellular matrix are instrumental for biliary repair. Following biliary damage and eventually, malignant transformation, the extracellular matrix undergoes several quantitative and qualitative modifications, which direct interactions among hepatic progenitor cells, reactive ductular cells, activated myofibroblasts and macrophages, to generate the ductular reaction. Herein, we will give an overview of the main molecular factors contributing to extracellular matrix remodeling in cholangiopathies. Then, we will discuss the structural alterations in terms of biochemical composition and physical stiffness featuring the “desmoplastic matrix” of cholangiocarcinoma along with their pro-oncogenic effects.

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The ATRA-dependent overexpression of the glutamate transporter EAAC1 requires RARβ induction

Bianchi

Gazzola

Cagnin

et al. 2009

Biochimica et Biophysica Acta (BBA) - Biomembranes

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The mechanisms underlying trafficking and membrane targeting of EAAC1, the rodent counterpart of the human EAAT3 carrier for anionic amino acids, are well characterized. In contrast, much less is known on the regulation of Slc1a1, the gene that encodes for the transporter. We have recently found that all-trans retinoic acid (ATRA) stimulates EAAC1 expression and anionic amino acid transport in C6 rat glioma cells. We report here that the ATRA effect on EAAC1 activity was inhibited by the specific RAR antagonist LE540 and mimicked by Am80, a RAR agonist, but not by the RXR agonist HX630. Moreover, the ATRA-dependent induction of Slc1a1 mRNA required the synthesis of a protein intermediate and was not associated with changes in the messenger half-life. ATRA treatment induced the expression of both Rarb mRNA and RARbeta protein several hours before the induction of Slc1a1, while the mRNA for RFX1, a transcription factor recently involved in Slc1a1 transcription, was unchanged. In addition, Rarb silencing markedly inhibited the ATRA-dependent increase of both Rarb and Slc1a1 mRNAs. We conclude that in C6 glioma cells the induction of Slc1a1 by ATRA requires the synthesis of RARbeta, suggesting that the receptor is involved in the regulation of the transporter gene.

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PSC-Associated Cholangiocarcinoma: Diagnostic and Therapeutic Considerations

Cagnin

Tabibian

Fabris

2021

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PC.01.6 Modeling of Primary Sclerosing Cholangitis Using Biliary Spheroids Derived From Bile Fluid and Needle-Liver Biopsy Sample

Mariotti¹,

Fantin²,

Cadamuro³

et al. 2020

Digestive and Liver Disease

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Silvia Cagnin

Liver Matrix in Benign and Malignant Biliary Tract Disease

The ATRA-dependent overexpression of the glutamate transporter EAAC1 requires RARβ induction

PSC-Associated Cholangiocarcinoma: Diagnostic and Therapeutic Considerations

PC.01.6 Modeling of Primary Sclerosing Cholangitis Using Biliary Spheroids Derived From Bile Fluid and Needle-Liver Biopsy Sample

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