Regenerative and fibrotic pathways in canine hepatic portosystemic shunt and portal vein hypoplasia, new models for clinical hepatocyte growth factor treatment 英文参考文献.docVIP
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Regenerative and fibrotic pathways in canine hepatic portosystemic shunt and portal vein hypoplasia, new models for clinical hepatocyte growth factor treatment 英文参考文献
Comparative Hepatology
BioMedCentral
Research
Open Access
Regenerative and fibrotic pathways in canine hepatic portosystemic
shunt and portal vein hypoplasia, new models for clinical hepatocyte
growth factor treatment
Bart Spee*1, Louis C Penning1, Ted SGAM van den Ingh2, Brigitte Arends1,
Jooske IJzer2, Frederik J van Sluijs1 and Jan Rothuizen1
Address: 1Department of Clinical Sciences of Companion Animals, Faculty of Veterinary Medicine, Utrecht University, Utrecht, The Netherlands
and 2Department of Pathobiology, Faculty of Veterinary Medicine, Utrecht University, Utrecht, The Netherlands
Email: Bart Spee* - b.spee@vet.uu.nl; Louis C Penning - l.c.penning@vet.uu.nl; Ted SGAM van den Ingh - t.s.g.a.m.vandenIngh@wanadoo.nl;
Brigitte Arends - b.arends@vet.uu.nl; Jooske IJzer - j.ijzer@vet.uu.nl; Frederik J van Sluijs - f.j.vansluijs@vet.uu.nl;
Jan Rothuizen - j.rothuizen@vet.uu.nl
* Corresponding author
Published: 07 December 2005
Received: 10 February 2005
Accepted: 07 December 2005
Comparative Hepatology 2005, 4:7
doi:10.1186/1476-5926-4-7
This article is available from: /content/4/1/7
? 2005 Spee et al; licensee BioMed Central Ltd.
This is an Open Access article distributed under the terms of the Creative Commons Attribution License (/licenses/by/2.0),
which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
Abstract
Background: We analyzed two spontaneous dog diseases characterized by subnormal portal
perfusion and reduced liver growth: (i) congenital portosystemic shunts (CPSS) without fibrosis and
(ii) primary portal vein hypoplasia (PPVH), a disease associated with fibrosis. These pathologies,
that lack inflammation or cholestasis, may represent simplified models to study liver growth and
fibrosis. To investigate the possible use of those models for hepatocyte growth factor (HGF)
treatment, we studied the functionality of HGF signaling in CPSS and PP
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