Enzyme-linked immunosorbent serum assay specific for the 7S domain of Collagen Type IV (P4NP 7S): A marker related to the extracellular matrix remodeling during liver fibrogenesis

Enzyme-linked immunosorbent serum assay specific for the 7S domain of Collagen Type IV (P4NP 7S): A marker related to the extracellular matrix remodeling during liver fibrogenesis

Aim:  The present study describes the ability of a newly developed N‐terminal pro‐peptides of type IV collagen 7S domain (P4NP 7S) competitive enzyme‐linked immunosorbent assay (ELISA) for describing liver fibrosis. The assay applies a monoclonal antibody specific for a PIVNP 7S epitope 100% homolog...

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Bibliographic Details
Published in:Hepatology research Vol. 42; no. 5; pp. 482 - 493
Main Authors: Leeming, Diana J., Nielsen, Mette J., Dai, Yueqin, Veidal, Sanne S., Vassiliadis, Efstathios, Zhang, Chen, He, Yi, Vainer, Ben, Zheng, Qinlong, Karsdal, Morten A.
Format: Journal Article
Language:English
Published: Melbourne, Australia Blackwell Publishing Asia 01-05-2012
Subjects:
bile duct ligation model
biochemical markers
CCl4
liver fibrosis
P4NP 7S domain
type IV collagen
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Summary:Aim:  The present study describes the ability of a newly developed N‐terminal pro‐peptides of type IV collagen 7S domain (P4NP 7S) competitive enzyme‐linked immunosorbent assay (ELISA) for describing liver fibrosis. The assay applies a monoclonal antibody specific for a PIVNP 7S epitope 100% homologous in the human, rat, and mouse species. Methods:  Monoclonal antibodies were raised against selected P4NP 7S specific sequences. Antibodies were screened and a competitive ELISA assay was developed using a selected antibody. The assay was evaluated in relation to technical performance, and in two preclinical liver fibrosis models; the bile duct ligation model (BDL) and the carbon tetrachloride model (CCL4) both performed in rats. Results:  A technically robust P4NP 7S ELISA assay using a monoclonal antibody was produced. In the BDL and CCL4 liver fibrosis models it was observed that the P4NP 7S levels were significantly elevated in rat with liver fibrosis as seen by histology (CCL4: 283% elevated in the highest quartile of total hepatic collagen compared with controls, P = 0.001; BDL: 183% elevated at week 4 compared with sham, P < 0.001) and correlated to the amount of hepatic type IV collagen expression in BDL rats (r = 0.49, P < 0.05) in contrast to sham (r = −0.12). P4NP 7S also correlated to total collagen in CCL4 treated livers (P < 0.001, r = 0.67), however, not in controls (r = 0.04). Conclusions:  This newly developed serum assay specific for P4NP 7S was highly related to liver fibrosis and correlated to extent of hepatic fibrosis. This assay may improve fibrosis quantification.
Bibliography:ArticleID:HEPR946
istex:0E85CAE533E6B6096BCBADF94498318423DEB23D
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DJ Leeming, Y Dai, SS Veidal, E Vassiliadis, Y Hi, Q Zheng, and MA Karsdal are full‐time employees of Nordic Bioscience.
Conflict of interest
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ISSN:1386-6346
1872-034X
DOI:10.1111/j.1872-034X.2011.00946.x