Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology

BACKGROUND & AIMS: Glisson’s capsule is the interstitial connective tissue that surrounds the liver. As part of its normal physiology, it withstands significant daily changes in liver size. The pathophysiology of the capsule in disease is not well understood. The aim of this study was to charact...

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Autores principales: Llewellyn, Jessica, Fede, Caterina, Loneker, Abigail E., Friday, Chet S., Hast, Michael W., Theise, Neil D., Furth, Emma E., Guido, Maria, Stecco, Carla, Wells, Rebecca G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10393548/
https://www.ncbi.nlm.nih.gov/pubmed/37534230
http://dx.doi.org/10.1016/j.jhepr.2023.100760
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author Llewellyn, Jessica
Fede, Caterina
Loneker, Abigail E.
Friday, Chet S.
Hast, Michael W.
Theise, Neil D.
Furth, Emma E.
Guido, Maria
Stecco, Carla
Wells, Rebecca G.
author_facet Llewellyn, Jessica
Fede, Caterina
Loneker, Abigail E.
Friday, Chet S.
Hast, Michael W.
Theise, Neil D.
Furth, Emma E.
Guido, Maria
Stecco, Carla
Wells, Rebecca G.
author_sort Llewellyn, Jessica
collection PubMed
description BACKGROUND & AIMS: Glisson’s capsule is the interstitial connective tissue that surrounds the liver. As part of its normal physiology, it withstands significant daily changes in liver size. The pathophysiology of the capsule in disease is not well understood. The aim of this study was to characterise the changes in capsule matrix, cellular composition, and mechanical properties that occur in liver disease and to determine whether these correlate with disease severity or aetiology. METHODS: Samples from ten control patients, and six with steatosis, seven with moderate fibrosis, and 37 with cirrhosis were collected from autopsies, intraoperative biopsies, and liver explants. Matrix proteins and cell markers were assessed by staining and second harmonic generation imaging. Mechanical tensile testing was performed on a test frame. RESULTS: Capsule thickness was significantly increased in cirrhotic samples compared with normal controls irrespective of disease aetiology (70.12 ± 14.16 μm and 231.58 ± 21.82 μm, respectively), whereas steatosis and moderate fibrosis had no effect on thickness (90.91 ± 11.40 μm). Changes in cirrhosis included an increase in cell number (fibroblasts, vascular cells, infiltrating immune cells, and biliary epithelial cells). Key matrix components (collagens 1 and 3, hyaluronan, versican, and elastin) were all deposited in the lower capsule, although only the relative amounts per area of hyaluronan and versican were increased. Organisational features, including crimping and alignment of collagen fibres, were also altered in cirrhosis. Unexpectedly, capsules from cirrhotic livers had decreased resistance to loading compared with controls. CONCLUSIONS: The liver capsule, similar to the parenchyma, is an active site of disease, demonstrating changes in matrix and cell composition as well as mechanical properties. IMPACT AND IMPLICATIONS: We assessed the changes in composition and response to stretching of the liver outer sheath, the capsule, in human liver disease. We found an increase in key structural components and numbers of cells as well as a change in matrix organisation of the capsule during the later stages of disease. This allows the diseased capsule to stretch more under any given force, suggesting that it is less stiff than healthy tissue.
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spelling pubmed-103935482023-08-02 Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology Llewellyn, Jessica Fede, Caterina Loneker, Abigail E. Friday, Chet S. Hast, Michael W. Theise, Neil D. Furth, Emma E. Guido, Maria Stecco, Carla Wells, Rebecca G. JHEP Rep Research Article BACKGROUND & AIMS: Glisson’s capsule is the interstitial connective tissue that surrounds the liver. As part of its normal physiology, it withstands significant daily changes in liver size. The pathophysiology of the capsule in disease is not well understood. The aim of this study was to characterise the changes in capsule matrix, cellular composition, and mechanical properties that occur in liver disease and to determine whether these correlate with disease severity or aetiology. METHODS: Samples from ten control patients, and six with steatosis, seven with moderate fibrosis, and 37 with cirrhosis were collected from autopsies, intraoperative biopsies, and liver explants. Matrix proteins and cell markers were assessed by staining and second harmonic generation imaging. Mechanical tensile testing was performed on a test frame. RESULTS: Capsule thickness was significantly increased in cirrhotic samples compared with normal controls irrespective of disease aetiology (70.12 ± 14.16 μm and 231.58 ± 21.82 μm, respectively), whereas steatosis and moderate fibrosis had no effect on thickness (90.91 ± 11.40 μm). Changes in cirrhosis included an increase in cell number (fibroblasts, vascular cells, infiltrating immune cells, and biliary epithelial cells). Key matrix components (collagens 1 and 3, hyaluronan, versican, and elastin) were all deposited in the lower capsule, although only the relative amounts per area of hyaluronan and versican were increased. Organisational features, including crimping and alignment of collagen fibres, were also altered in cirrhosis. Unexpectedly, capsules from cirrhotic livers had decreased resistance to loading compared with controls. CONCLUSIONS: The liver capsule, similar to the parenchyma, is an active site of disease, demonstrating changes in matrix and cell composition as well as mechanical properties. IMPACT AND IMPLICATIONS: We assessed the changes in composition and response to stretching of the liver outer sheath, the capsule, in human liver disease. We found an increase in key structural components and numbers of cells as well as a change in matrix organisation of the capsule during the later stages of disease. This allows the diseased capsule to stretch more under any given force, suggesting that it is less stiff than healthy tissue. Elsevier 2023-04-07 /pmc/articles/PMC10393548/ /pubmed/37534230 http://dx.doi.org/10.1016/j.jhepr.2023.100760 Text en © 2023 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Article
Llewellyn, Jessica
Fede, Caterina
Loneker, Abigail E.
Friday, Chet S.
Hast, Michael W.
Theise, Neil D.
Furth, Emma E.
Guido, Maria
Stecco, Carla
Wells, Rebecca G.
Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
title Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
title_full Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
title_fullStr Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
title_full_unstemmed Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
title_short Glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
title_sort glisson’s capsule matrix structure and function is altered in patients with cirrhosis irrespective of aetiology
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10393548/
https://www.ncbi.nlm.nih.gov/pubmed/37534230
http://dx.doi.org/10.1016/j.jhepr.2023.100760
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