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The development of hepatic stellate cells in normal and abnormal human fetuses – an immunohistochemical study
Author(s) -
Loo Christine K. C.,
Pereira Tamara N.,
Pozniak Katarzy.,
Ramsing Mette,
Vogel Ida,
Ramm Grant A.
Publication year - 2015
Publication title -
physiological reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.918
H-Index - 39
ISSN - 2051-817X
DOI - 10.14814/phy2.12504
Subject(s) - hepatic stellate cell , mesothelial cell , pathology , biology , fetus , mesothelium , mesenchymal stem cell , liver cytology , microbiology and biotechnology , medicine , endocrinology , pregnancy , liver metabolism , genetics
The precise embryological origin and development of hepatic stellate cells is not established. Animal studies and observations on human fetuses suggest that they derive from posterior mesodermal cells that migrate via the septum transversum and developing diaphragm to form submesothelial cells beneath the liver capsule, which give rise to mesenchymal cells including hepatic stellate cells. However, it is unclear if these are similar to hepatic stellate cells in adults or if this is the only source of stellate cells. We have studied hepatic stellate cells by immunohistochemistry, in developing human liver from autopsies of fetuses with and without malformations and growth restriction, using cellular Retinol Binding Protein‐1 ( cRBP ‐1), Glial Fibrillary Acidic Protein ( GFAP ), and α ‐Smooth Muscle Actin ( α SMA ) antibodies, to identify factors that influence their development. We found that hepatic stellate cells expressing cRBP ‐1 are present from the end of the first trimester of gestation and reduce in density throughout gestation. They appear abnormally formed and variably reduced in number in fetuses with abnormal mesothelial Wilms Tumor 1 ( WT 1) function, diaphragmatic hernia and in ectopic liver nodules without mesothelium. Stellate cells showed similarities to intravascular cells and their presence in a fetus with diaphragm agenesis suggests they may be derived from circulating stem cells. Our observations suggest circulating stem cells as well as mesothelium can give rise to hepatic stellate cells, and that they require normal mesothelial function for their development.

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