Literature DB >> 1446899

Role of mesenchymal cell populations in porcine serum-induced rat liver fibrosis.

E Bhunchet1, K Wake.   

Abstract

The role of liver mesenchymal cell populations in porcine serum-induced rat liver fibrosis were studied morphologically and immunohistochemically. Five-week-old rats were intraperitoneally injected with porcine serum twice a week and examined at various intervals between 3 and 24 wk after the initial injection. At an early phase, numbers of fibroblasts and extracellular matrix increased in the walls of central veins and in portal and capsular connective tissues. In the walls of central veins, the number of "second-layer cells" (i.e., the fibroblasts located at the second layer of the wall) increased. Connective tissue septa, accompanying some fibroblasts, extended from these interstitial tissues into the hepatic parenchyma, and their foremost edges came into direct contact with the perisinusoidal stellate cells. The sinusoids adjacent to the newly formed septa collapsed and later disappeared; this process resulted in the formation of hepatic limiting plates along the septa. At a more advanced stage, the interstitial fibroblasts and septal cells-which were derived from interstitial fibroblasts and the stellate cells-increased and became multilayered, constructing three-dimensional cell networks. These networks, together with increased collagen fibrils and elastic fibers, constitute the fibrotic dense connective tissue. In the control rat, smooth muscle cells were positive on vimentin, desmin and smooth muscle-alpha-actin staining. The stellate cells, second-layer cells, capsular and portal fibroblasts were shown to be vimentin and desmin positive and smooth muscle-alpha-actin negative. In the fibrotic liver, septal(fibroblastic) cells were vimentin and desmin positive and smooth muscle-alpha-actin negative. We conclude that not only the perisinusoidal stellate cells but also the interstitial fibroblasts, including the second-layer cells, play substantial role in the development of porcine serum-induced septal fibrosis in rat liver.

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Year:  1992        PMID: 1446899     DOI: 10.1002/hep.1840160623

Source DB:  PubMed          Journal:  Hepatology        ISSN: 0270-9139            Impact factor:   17.425


  37 in total

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2.  Lymphocyte-hepatic stellate cell proximity suggests a direct interaction.

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3.  miR-194 is a marker of hepatic epithelial cells and suppresses metastasis of liver cancer cells in mice.

Authors:  Zhipeng Meng; Xianghui Fu; Xiaosong Chen; Samuel Zeng; Yan Tian; Richard Jove; Rongzhen Xu; Wendong Huang
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4.  GFAP promoter directs lacZ expression specifically in a rat hepatic stellate cell line.

Authors:  Gunter Maubach; Michelle Chin Chia Lim; Chun-Yan Zhang; Lang Zhuo
Journal:  World J Gastroenterol       Date:  2006-02-07       Impact factor: 5.742

5.  Hepatomegaly in transgenic mice expressing the homeobox gene Cux-1.

Authors:  Gregory B Vanden Heuvel; Jennifer G Brantley; Neal I Alcalay; Madhulika Sharma; Gabor Kemeny; Joshua Warolin; Aric W Ledford; David M Pinson
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6.  Induction of tropomyosin during hepatic stellate cell activation and the progression of liver fibrosis.

Authors:  Kohji Otogawa; Tomohiro Ogawa; Ryoko Shiga; Kazuo Ikeda; Norifumi Kawada
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7.  Smoothelin, a new marker to determine the origin of liver fibrogenic cells.

Authors:  Sébastien Lepreux; Christelle Guyot; Fabrice Billet; Chantal Combe; Charles Balabaud; Paulette Bioulac-Sage; Alexis Desmoulière
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8.  Intralobular heterogeneity of perisinusoidal stellate cells in porcine liver.

Authors:  K Wake; T Sato
Journal:  Cell Tissue Res       Date:  1993-08       Impact factor: 5.249

Review 9.  The portal fibroblast: not just a poor man's stellate cell.

Authors:  Rebecca G Wells
Journal:  Gastroenterology       Date:  2014-05-09       Impact factor: 22.682

Review 10.  Bioconjugation of oligonucleotides for treating liver fibrosis.

Authors:  Zhaoyang Ye; Houssam S Hajj Houssein; Ram I Mahato
Journal:  Oligonucleotides       Date:  2007
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