Bacterial protease alleviate chronic liver fibrosis induced by thioacetamide through suppression of hepatic stellate cells consequently decrease its proliferative index

In chronic liver diseases, liver fibrosis occurs due to excessive extracellular matrix (ECM) protein accumulation. Approximately 2 million deaths occur yearly due to liver disease, while cirrhosis is the 11th most common cause of death. Therefore, newer compounds or biomolecules must be synthesized...

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Published in:International journal of biological macromolecules 2023-06, Vol.239, p.124243-124243, Article 124243
Main Authors: Salem, Gad Elsayed Mohamed, Azzam, Shaimaa M., Nasser, Mona A.F., El Malah, Tamer, Abd El-Latief, Hanan M., Khan, Rizwan Hasan, Chavanich, Suchana, Anwar, Hend Mohamed
Format: Article
Language:English
Subjects:
adjuvants
Animals
Anti-Inflammatory Agents - pharmacology
antioxidants
Bacillus cereus
collagen
death
Endopeptidases - metabolism
extracellular matrix
Fibrosis
Hepatic Stellate Cells
histology
histopathology
interleukin-6
Liver
liver cirrhosis
Liver Cirrhosis - chemically induced
Liver Cirrhosis - drug therapy
Liver Cirrhosis - metabolism
liver function
Male
males
mutants
Nrf2/MCP-1
Oxidative Stress
Peptide Hydrolases - metabolism
Protease
proteinases
Rats
therapeutics
Thioacetamide
Thioacetamide - toxicity
Vascular Endothelial Growth Factor A - metabolism
VEGF
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Summary:In chronic liver diseases, liver fibrosis occurs due to excessive extracellular matrix (ECM) protein accumulation. Approximately 2 million deaths occur yearly due to liver disease, while cirrhosis is the 11th most common cause of death. Therefore, newer compounds or biomolecules must be synthesized to treat chronic liver diseases. In this aspect, the present study focuses on the assessment of the anti-inflammatory and antioxidant impact of Bacterial Protease (BP) produced by a new mutant strain of bacteria (Bacillus cereus S6-3/UM90) and 4,4′-(2,5-dimethoxy-1,4-phenylene) bis (1-(3-ethoxy phenyl)-1H-1,2,3-triazole) (DPET) in the treatment of early stage of liver fibrosis induced by thioacetamide (TAA). Sixty male rats were divided into six groups, ten rats each as follows: (1) Control group, (2) BP group, (3) TAA group, (4) TAA-Silymarin (S) group, (5) TAA-BP group, and (6) TAA-DPET group. Liver fibrosis significantly elevated liver function ALT, AST, and ALP, as well as anti-inflammatory interleukin 6 (IL-6) and VEGF. The oxidative stress parameters (MDA, SOD, and NO) were significantly increased with a marked reduction in GSH. Expression of MAPK and MCP-1 was unregulated in the TAA group, with downregulation of Nrf2 was observed. TAA caused histopathological alterations associated with hepatic vacuolation and fibrosis, increasing collagen fibers and high immuno-expression of VEGF. On the other hand, treatment with BP successfully improved the severe effects of TAA on the liver and restored histological architecture. Our study concluded the protective potentials of BP for attenuating liver fibrosis and could be used as adjuvant therapy for treating hepatic fibrosis. [Display omitted]
ISSN:0141-8130
1879-0003
DOI:10.1016/j.ijbiomac.2023.124243