Your search keyword '"Ghufran, Shaikh Maryam"' showing total 3 results

1. Survivin expression is essential for early activation of hepatic stellate cells and fibrosis progression in chronic liver injury.

Author

Sharma S, Ghufran SM, Das B, Roy B, Ghose S, and Biswas S

Subjects

Animals, Cells, Cultured, Dose-Response Relationship, Drug, End Stage Liver Disease genetics, End Stage Liver Disease pathology, Hepatic Stellate Cells drug effects, Hepatic Stellate Cells pathology, Imidazoles pharmacology, Liver Cirrhosis genetics, Liver Cirrhosis pathology, Male, Mice, Mice, Inbred BALB C, Naphthoquinones pharmacology, Survivin antagonists & inhibitors, Survivin genetics, Disease Progression, End Stage Liver Disease metabolism, Hepatic Stellate Cells metabolism, Liver Cirrhosis metabolism, Survivin biosynthesis

Abstract

Aim: Hepatic fibrosis in injured liver is characterized by the activation of hepatic stellate cells (HSCs) from their quiescent state. Survivin (BIRC5) is one of the key genes that are upregulated during activation of HSCs but their role in HSC activation and fibrosis progression is unknown. Here, we have investigated the role of survivin protein in early fibrogenic activation of HSCs and fibrosis progression in chronic liver injury., Materials & Methods: Primary quiescent HSCs were isolated from healthy mice liver through perfusion and cultured for fibrogenic activation. Survivin expression was suppressed by its pharmacological suppressant, YM155. We developed chronic liver injury induced fibrotic mice model through administrating repeated dose of CCl 4 for 2 weeks and 4 weeks. Mice were pre-treated with YM155 a week before CCl 4 administration till 2nd week of dosing and then discontinued. Hepatic parameters were characterized and underlying mechanisms were investigated., Key Findings: Survivin expression gradually increased along with the expression of αSMA, collagen I activation maker in HSCs during their activation from quiescent state. Survivin suppression through YM155 downregulated αSMA, collagen I. Pre-treatment of YM155 in mice ceased the early activation of HSCs and onset of fibrosis in injured liver. However, discontinuation of YM155 initiated the activation of HSCs and fibrosis progression that shows survivin expression in HSCs is essential for their early activation and onset of liver fibrosis., Significance: Survivin expression induces with activation of HSCs and drives onset of liver fibrosis in injured liver. Targeting survivin protein in activated HSCs could be a potential anti-fibrotic therapeutic approach in chronic liver injury., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

2. Divergent effect of Birinapant, and BV6 SMAC mimetic on TNFα induced NF-κB signaling and cell viability in activated hepatic stellate cells

Author

Ghufran, Shaikh Maryam, Sharma, Sachin, Ghose, Sampa, and Biswas, Subhrajit

Published

2023

3. Survivin inhibition ameliorates liver fibrosis by inducing hepatic stellate cell senescence and depleting hepatic macrophage population.

Author

Sharma, Sachin, Ghufran, Shaikh Maryam, Aftab, Mehreen, Bihari, Chhagan, Ghose, Sampa, and Biswas, Subhrajit

Abstract

Persistent activation of hepatic stellate cells (HSCs) in the injured liver leads to the progression of liver injury from fibrosis to detrimental cirrhosis. In a previous study, we have shown that survivin protein is upregulated during the early activation of HSCs, which triggers the onset of liver fibrosis. However, the therapeutic potential of targeting survivin in a fully established fibrotic liver needs to be investigated. In this study, we chemically induced hepatic fibrosis in mice using carbon tetrachloride (CCl4) for 6 weeks, which was followed by treatment with a survivin suppressant (YM155). We also evaluated survivin expression in fibrotic human liver tissues, primary HSCs, and HSC cell line by histological analysis. αSMA+ HSCs in human and mice fibrotic liver tissues showed enhanced survivin expression, whereas the hepatocytes and quiescent (qHSCs) displayed minimal expression. Alternatively, activated M2 macrophage subtype induced survivin expression in HSCs through the TGF‐β‐TGF‐β receptor‐I/II signaling. Inhibition of survivin in HSCs promoted cell cycle arrest and senescence, which eventually suppressed their activation. In vivo, YM155 treatment increased the expression of cell senescence makers in HSCs around fibrotic septa such as p53, p21, and β‐galactosidase. YM155 treatment in vivo also reduced the hepatic macrophage population and inflammatory cytokine expression in the liver. In conclusion, downregulation of survivin in the fibrotic liver decreases HSC activation by inducing cellular senescence and modulating macrophage cytokine expression that collectively ameliorates liver fibrosis. [ABSTRACT FROM AUTHOR]

Published

2024