Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis

CCN-2 (connective tissue growth factor; CTGF) is a key factor in fibrosis. Plasma CCN-2 has biomarker potential in numerous fibrotic disorders, but it is unknown which pathophysiological factors determine plasma CCN-2 levels. The proteolytic amino-terminal fragment of CCN-2 is primarily eliminated b...

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Autores principales: Gerritsen, K. G. F., Bovenschen, N., Nguyen, T. Q., Sprengers, D., Koeners, M. P., van Koppen, A. N., Joles, J. A., Goldschmeding, R., Kok, R. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Netherlands 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5143326/
https://www.ncbi.nlm.nih.gov/pubmed/27644406
http://dx.doi.org/10.1007/s12079-016-0354-6
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author Gerritsen, K. G. F.
Bovenschen, N.
Nguyen, T. Q.
Sprengers, D.
Koeners, M. P.
van Koppen, A. N.
Joles, J. A.
Goldschmeding, R.
Kok, R. J.
author_facet Gerritsen, K. G. F.
Bovenschen, N.
Nguyen, T. Q.
Sprengers, D.
Koeners, M. P.
van Koppen, A. N.
Joles, J. A.
Goldschmeding, R.
Kok, R. J.
author_sort Gerritsen, K. G. F.
collection PubMed
description CCN-2 (connective tissue growth factor; CTGF) is a key factor in fibrosis. Plasma CCN-2 has biomarker potential in numerous fibrotic disorders, but it is unknown which pathophysiological factors determine plasma CCN-2 levels. The proteolytic amino-terminal fragment of CCN-2 is primarily eliminated by the kidney. Here, we investigated elimination and distribution profiles of full length CCN-2 by intravenous administration of recombinant CCN-2 to rodents. After bolus injection in mice, we observed a large initial distribution volume (454 mL/kg) and a fast initial clearance (120 mL/kg/min). Immunosorbent assay and immunostaining showed that CCN-2 distributed mainly to the liver and was taken up by hepatocytes. Steady state clearance in rats, determined by continuous infusion of CCN-2, was fast (45 mL/kg/min). Renal CCN-2 clearance, determined by arterial and renal vein sampling, accounted for only 12 % of total clearance. Co-infusion of CCN-2 with receptor-associated protein (RAP), an antagonist of LDL-receptor family proteins, showed that RAP prolonged CCN-2 half-life and completely prevented CCN-2 internalization by hepatocytes. This suggests that hepatic uptake of CCN-2 is mediated by a RAP-sensitive mechanism most likely involving LRP1, a member of the LDL-receptor family involved in hepatic clearance of various plasma proteins. Surface plasmon resonance binding studies confirmed that CCN-2 is an LRP1 ligand. Co-infusion of CCN-2 with an excess of the heparan sulphate-binding protamine lowered the large initial distribution volume of CCN-2 by 88 % and reduced interstitial staining of CCN-2, suggesting binding of CCN-2 to heparan sulphate proteoglycans (HSPGs). Protamine did not affect clearance rate, indicating that RAP-sensitive clearance of CCN-2 is HSPG independent. In conclusion, unlike its amino-terminal fragment which is cleared by the kidney, full length CCN-2 is primarily eliminated by the liver via a fast RAP-sensitive, probably LRP1-dependent pathway.
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spelling pubmed-51433262016-12-22 Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis Gerritsen, K. G. F. Bovenschen, N. Nguyen, T. Q. Sprengers, D. Koeners, M. P. van Koppen, A. N. Joles, J. A. Goldschmeding, R. Kok, R. J. J Cell Commun Signal Research Article CCN-2 (connective tissue growth factor; CTGF) is a key factor in fibrosis. Plasma CCN-2 has biomarker potential in numerous fibrotic disorders, but it is unknown which pathophysiological factors determine plasma CCN-2 levels. The proteolytic amino-terminal fragment of CCN-2 is primarily eliminated by the kidney. Here, we investigated elimination and distribution profiles of full length CCN-2 by intravenous administration of recombinant CCN-2 to rodents. After bolus injection in mice, we observed a large initial distribution volume (454 mL/kg) and a fast initial clearance (120 mL/kg/min). Immunosorbent assay and immunostaining showed that CCN-2 distributed mainly to the liver and was taken up by hepatocytes. Steady state clearance in rats, determined by continuous infusion of CCN-2, was fast (45 mL/kg/min). Renal CCN-2 clearance, determined by arterial and renal vein sampling, accounted for only 12 % of total clearance. Co-infusion of CCN-2 with receptor-associated protein (RAP), an antagonist of LDL-receptor family proteins, showed that RAP prolonged CCN-2 half-life and completely prevented CCN-2 internalization by hepatocytes. This suggests that hepatic uptake of CCN-2 is mediated by a RAP-sensitive mechanism most likely involving LRP1, a member of the LDL-receptor family involved in hepatic clearance of various plasma proteins. Surface plasmon resonance binding studies confirmed that CCN-2 is an LRP1 ligand. Co-infusion of CCN-2 with an excess of the heparan sulphate-binding protamine lowered the large initial distribution volume of CCN-2 by 88 % and reduced interstitial staining of CCN-2, suggesting binding of CCN-2 to heparan sulphate proteoglycans (HSPGs). Protamine did not affect clearance rate, indicating that RAP-sensitive clearance of CCN-2 is HSPG independent. In conclusion, unlike its amino-terminal fragment which is cleared by the kidney, full length CCN-2 is primarily eliminated by the liver via a fast RAP-sensitive, probably LRP1-dependent pathway. Springer Netherlands 2016-09-19 2016-12 /pmc/articles/PMC5143326/ /pubmed/27644406 http://dx.doi.org/10.1007/s12079-016-0354-6 Text en © The Author(s) 2016 Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Research Article
Gerritsen, K. G. F.
Bovenschen, N.
Nguyen, T. Q.
Sprengers, D.
Koeners, M. P.
van Koppen, A. N.
Joles, J. A.
Goldschmeding, R.
Kok, R. J.
Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis
title Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis
title_full Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis
title_fullStr Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis
title_full_unstemmed Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis
title_short Rapid hepatic clearance of full length CCN-2/CTGF: a putative role for LRP1-mediated endocytosis
title_sort rapid hepatic clearance of full length ccn-2/ctgf: a putative role for lrp1-mediated endocytosis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5143326/
https://www.ncbi.nlm.nih.gov/pubmed/27644406
http://dx.doi.org/10.1007/s12079-016-0354-6
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