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Hepatoprotection of silymarin against thioacetamide-induced chronic liver fibrosis
Journal of the science of food and agriculture, 2012-05, Vol.92 (7), p.1441-1447
Chen, I-Shu
Chen, Yi-Chen
Chou, Chung-Hsi
Chuang, Ruei-Feng
Sheen, Lee-Yan
Chiu, Chih-Hsien
2012
Volltextzugriff (PDF)
Details
Autor(en) / Beteiligte
Chen, I-Shu
Chen, Yi-Chen
Chou, Chung-Hsi
Chuang, Ruei-Feng
Sheen, Lee-Yan
Chiu, Chih-Hsien
Titel
Hepatoprotection of silymarin against thioacetamide-induced chronic liver fibrosis
Ist Teil von
Journal of the science of food and agriculture, 2012-05, Vol.92 (7), p.1441-1447
Ort / Verlag
Chichester, UK: John Wiley & Sons, Ltd
Erscheinungsjahr
2012
Quelle
MEDLINE
Beschreibungen/Notizen
BACKGROUND: Liver fibrosis is chronic liver damage usually caused by alcohol, viruses or other toxins and is characterised by an excessive accumulation of extracellular matrix proteins such as collagen. The aim of this study was to establish an animal model of chronic liver damage and investigate molecular mechanisms of silymarin hepatoprotective effects. RESULTS: Thioacetamide (TAA; 100 mg kg−1 intraperitoneal (i.p.) injection three times weekly) effectively induced chronic liver fibrosis in male ICR mice. Then 24 ICR mice were randomly divided into four groups: (1) saline (i.p.) + water (gavage); (2) saline (i.p.) + 150 mg kg−1 silymarin (gavage); (3) 100 mg kg−1 TAA (i.p.) + water (gavage); (4) 100 mg kg−1 TAA (i.p.) + 150 mg kg−1 silymarin (gavage). Eight weeks of TAA treatment resulted in lower body weight, serum cholesterol and triglycerides as well as increased liver size, ALT, AST and LDH values (P < 0.05). These TAA‐induced effects were attenuated by silymarin (P < 0.05); therefore silymarin also ameliorated TAA‐induced liver lesions. Effects of silymarin on TAA‐induced chronic liver damage may be attributed to down‐regulation of hepatic MMP‐2, MMP‐13, TIMP‐1, TIMP‐2, AP‐1, KLF6, TGF‐β1, α‐SMA and COL‐α1. CONCLUSION: A mouse model of chronic liver fibrosis was successfully established by injecting 100 mg kg−1 TAA three times weekly in male ICR mice. Meanwhile, silymarin showed hepatoprotection against TAA‐induced damage. Copyright © 2011 Society of Chemical Industry
Sprache
Englisch
Identifikatoren
ISSN: 0022-5142
eISSN: 1097-0010
DOI: 10.1002/jsfa.4723
Titel-ID: cdi_proquest_journals_993561788
Format
–
Schlagworte
Animals
,
Body Weight - drug effects
,
Chemical and Drug Induced Liver Injury - drug therapy
,
Chemical and Drug Induced Liver Injury - metabolism
,
Chemical and Drug Induced Liver Injury - pathology
,
Cholesterol
,
Cholesterol - blood
,
Chronic Disease
,
chronic liver fibrosis
,
Disease Models, Animal
,
Down-Regulation
,
hepatic stellate cell activation
,
Liver - drug effects
,
Liver - metabolism
,
Liver - pathology
,
Liver Cirrhosis, Experimental - metabolism
,
Liver Cirrhosis, Experimental - pathology
,
Liver Cirrhosis, Experimental - prevention & control
,
Liver diseases
,
Male
,
Matrix Metalloproteinases - metabolism
,
Medical treatment
,
Mice
,
Mice, Inbred ICR
,
MMP/TIMP families
,
Organ Size - drug effects
,
Phytotherapy
,
Plant Extracts - pharmacology
,
Plant Extracts - therapeutic use
,
Proteins
,
Random Allocation
,
Rodents
,
Silybum marianum - chemistry
,
silymarin
,
Silymarin - pharmacology
,
Silymarin - therapeutic use
,
Thioacetamide
,
Tissue Inhibitor of Metalloproteinases - metabolism
,
Transcription Factor AP-1 - metabolism
,
Transforming Growth Factor beta1 - metabolism
,
Triglycerides - blood
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