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Query: UMLS:C0239946 (
liver fibrosis
)
8,268
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Liver biopsy, owing to its limitations and risks, is an imperfect gold standard for assessing the severity of the most frequent chronic liver diseases chronic hepatitis C (HCV), B (HBV) non alcoholic (NAFLD) and alcoholic (
ALD
) fatty liver diseases. This review summarizes the advantages and the limits of the available biomarkers of
liver fibrosis
. Among a total of 2,237 references, a total of 14 validated serum biomarkers have been identified between 1991 and 2008. Nine were not patented and five were patented. Two alternatives to liver biopsy were the most evaluated FibroTest and Fibroscan. For FibroTest, there was a total of 38 different populations including 7,985 subjects with both FibroTest and biopsy (4,600 HCV, 1,580 HBV, 267 NAFLD, 524
ALD
, and 1014 mixed). For Fibroscan, there was a total of 11 published studies including 2,260 subjects (1,466 HCV, 95 cholestatic liver disease, and 699 mixed). For FibroTest, the mean diagnostic value for the diagnosis of advanced fibrosis assessed using standardized area under the ROC curves was 0.84 (95% confidence interval 0.83-0.86), without a significant difference between the causes of liver disease, hepatitis C, hepatitis B, and alcoholic or non alcoholic fatty liver disease. High-risk profiles of false negative/false positive of FibroTest, mainly Gilbert syndrome, hemolysis and acute inflammation, are present in 3% of the populations. In case of discordance between biopsy and FibroTest, half of the failures can be due to biopsy; the prognostic value of FibroTest is at least similar to that of biopsy in HCV, HBV and
ALD
. In conclusion this overview of evidence-based data suggests that biomarkers could be used as an alternative to liver biopsy for the first line assessment of fibrosis stage in the four most common chronic liver diseases, namely HCV, HBV, NAFLD and
ALD
. Neither biomarkers nor biopsy alone is sufficient for taking a definite decision in a given patient; all the clinical and biological data must be taken into account. There is no evidence based data justifying biopsy as a first line estimate of
liver fibrosis
. Health authorities in some countries have already approved validated biomarkers as the first line procedure for the staging of
liver fibrosis
.
...
PMID:Assessment of liver fibrosis: noninvasive means. 1956 32
Metabolic and alcoholic liver injuries result in nonalcoholic (NAFLD) or alcoholic (
ALD
) fatty liver disease, respectively. In particular, presence of fibrosis in NAFLD and
ALD
requires treatment, but development of drugs is hampered by the lack of suitable models with significant fibrosis. The carbon tetrachloride (CCl
4
)
liver fibrosis
model does not reflect human NAFLD or
ALD
, but CCl
4
may serve as a fibrosis accelerator in addition to another injury. Ethanol in drinking water (16%) or Western diet (WD) were administered for 7 wk in mice either alone or in combination with CCl
4
intoxications. Extent of fibrosis, steatosis, and inflammation was assessed by histology, transcription, and biochemistry. Furthermore, transcription of fibrosis, proliferation, and inflammation-related genes was studied on human liver samples with fibrosis resulting from hepatitis C virus infection (
n
= 7), NAFLD (
n
= 8), or
ALD
(
n
= 7). WD or ethanol alone induced only mild steatosis and inflammation. Combination of CCl
4
and WD induced the most severe steatosis together with significant
liver fibrosis
and moderate inflammation. Combination of CCl
4
and ethanol induced the strongest inflammation, with significant
liver fibrosis
and moderate steatosis. The relationship pattern between fibrosis, proliferation, and inflammation of human
ALD
was mostly similar in mice treated with CCl
4
and ethanol. The combination of CCl
4
intoxication with WD validates previous data suggesting it as an appropriate model for human nonalcoholic steatohepatitis. Especially, CCl
4
plus ethanol for 7 wk induces
ALD
in mice, providing a model suitable for further basic research and drug testing.
NEW & NOTEWORTHY
Alcoholic fatty liver disease with significant fibrosis is generated within 7 wk using carbon tetrachloride as a fibrosis accelerator and administering gradually ethanol (up to 16%) in mice. The similarity in the pattern of steatosis, inflammation, and fibrosis involved in alcoholic fatty liver disease to those of the human condition renders this mouse model suitable as a preclinical model for drug development.
...
PMID:Combination of CCl
4
with alcoholic and metabolic injuries mimics human liver fibrosis. 3118 34
