Abstract
Liver fibrosis is the most common outcome of chronic liver diseases, and its progression to cirrhosis can only be effectively treated with liver transplantation. The amniotic membrane (AM) has been studied as an alternative therapy for fibrosis diseases mainly for its favorable properties, including anti-inflammatory, anti-scaring and immunomodulatory properties. It was recently demonstrated that the AM reduces the progression of biliary fibrosis to its advanced stage, cirrhosis, when applied on the liver for 6 weeks after fibrosis induction. Here, we investigated the effects of AM on rat fibrotic liver, during a prolonged period of time. Fibrosis was induced by bile duct ligation (BDL), and at the same time, a fragment of AM was applied around the liver. After 1, 3, 6, and 9 weeks, the degree of fibrosis was assessed by qualitative Knodell scoring, and by quantitative image analysis to quantify the area of collagen deposition in hepatic tissue. While fibrosis progressed rapidly in untreated BDL animals, leading to cirrhosis within 6 weeks, AM-treated livers showed confined fibrosis at the periportal area with few and thin fibrotic septa, but without cirrhosis. In addition, collagen deposition was reduced to about 36 and 55% of levels observed in BDL at 6 and 9 weeks after BDL, respectively, which shows that the longer the period of AM application, the lower the collagen deposition. These results suggested that AM applied as a patch onto the liver surface for longer periods attenuated the severity of biliary fibrosis and protected against liver degeneration caused by excessive collagen deposition.
Highlights
Fibrosis is the most common outcome of chronic liver diseases
Considering all rats, bile duct ligation (BDL) (n=32) and BDL+amniotic membrane (AM) (n=32), we observed the absence of bile duct dilatation in 7 rats (10.93%), 4 in the BDL group (12.5%) and 3 in the BDL+AM (9.3%)
Regarding the temporal progression of liver fibrosis with groups, the results showed no significant difference in disease progression between the first and third week (P40.05), i.e., the value of fibrosis score remained similar in the BDL group and in the BDL+AM group, (Figure 4)
Summary
Fibrosis is the most common outcome of chronic liver diseases. Fibrosis is characterized by an excessive accumulation of extracellular matrix in hepatic parenchyma, which distorts the normal liver architecture, forming scar tissue that encapsulates the injured area. Rings of scar tissue surround regenerative nodules of liver parenchyma, which characterizes the end stage of the disease known as cirrhosis [2]. Patients with cirrhosis have a high risk of irreversible liver failure or hepatocellular carcinoma in adulthood [3]. The only effective treatment for cirrhosis is organ transplantation, which still has several limitations, including scarce availability of donor livers, risk of immune rejection, immunosuppressive therapy for life, and the fact that many patients are not able to undergo transplantation [4]
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