Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver

F. van Dijk; N. Teekamp; L. Beljaars; E. Post; J. Zuidema; R. Steendam; Y. O. Kim; H. W. Frijlink; D. Schuppand; K. Poelstra; W. L. J. Hinrichs; P. Olinga

doi:10.1016/j.jconrel.2017.11.029

Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver

F. van Dijk, N. Teekamp, L. Beljaars, E. Post, J. Zuidema, R. Steendam, Y. O. Kim, H. W. Frijlink, D. Schuppand, K. Poelstra, W. L. J. Hinrichs^*, P. Olinga

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Liver fibrogenesis is associated with excessive production of extracellular matrix by myofibroblasts that often leads to cirrhosis and consequently liver dysfunction and death. Novel protein-based antifibrotic drugs show high specificity and efficacy, but their use in the treatment of fibrosis causes a high burden for patients, since repetitive and long-term parenteral administration is required as most proteins and peptides are rapidly cleared from the circulation. Therefore, we developed biodegradable polymeric microspheres for the sustained release of proteinaceous drugs. We encapsulated the drug carrier pPB-HSA, which specifically binds to the PDGF beta R that is highly upregulated on activated myofibroblasts, into microspheres composed of hydrophilic multi-block copolymers composed of poly(L-lactide) and poly ethylene glycol/poly(is an element of-caprolactone), allowing diffusion-controlled release. Firstly, we estimated in mice with acute fibrogenesis induced by a single CCl4 injection the half-life of I-125-labeled pPB-HSA at 40 min and confirmed the preferential accumulation in fibrotic tissue. Subsequently, we determined in the Mdr2-/- mouse model of advanced biliary liver fibrosis how the subcutaneously injected microspheres released pPB-HSA into both plasma and fibrotic liver at 24 h after injection, which was maintained for six days. Although the microspheres still contained protein at day seven, pPB-HSA plasma and liver concentrations were decreased. This reduction was associated with an antibody response against the human albumin-based carrier protein, which was prevented by using a mouse albumin-based equivalent (pPB-MSA). In conclusion, this study shows that our polymeric microspheres are suitable as sustained release formulation for targeted protein constructs such as pPB-HSA. These formulations could be applied for the long-term treatment of chronic diseases such as liver fibrosis.

Original language	English
Pages (from-to)	258-265
Number of pages	8
Journal	Journal of Controlled Release
Volume	269
Early online date	20-Nov-2017
DOIs	https://doi.org/10.1016/j.jconrel.2017.11.029
Publication status	Published - 10-Jan-2018

Keywords

Controlled release
Biodegradable polymeric microspheres
PDGF beta-receptor targeted drug carrier
Protein delivery
in vitro in vivo correlation
Liver fibrosis
GROWTH-FACTOR RECEPTOR
DRUG-DELIVERY
ANTIFIBROTIC THERAPIES
POLYMERIC MICROSPHERES
MULTIBLOCK-COPOLYMER
INTERFERON-GAMMA
IN-VIVO
FIBROSIS
IMPLANTS
MICE

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van Dijk, F., Teekamp, N., Beljaars, L., Post, E., Zuidema, J., Steendam, R., Kim, Y. O., Frijlink, H. W., Schuppand, D., Poelstra, K., Hinrichs, W. L. J., & Olinga, P. (2018). Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver. Journal of Controlled Release, 269, 258-265. https://doi.org/10.1016/j.jconrel.2017.11.029

@article{5cfdb613f3554af0828c44a265783b79,

title = "Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver",

abstract = "Liver fibrogenesis is associated with excessive production of extracellular matrix by myofibroblasts that often leads to cirrhosis and consequently liver dysfunction and death. Novel protein-based antifibrotic drugs show high specificity and efficacy, but their use in the treatment of fibrosis causes a high burden for patients, since repetitive and long-term parenteral administration is required as most proteins and peptides are rapidly cleared from the circulation. Therefore, we developed biodegradable polymeric microspheres for the sustained release of proteinaceous drugs. We encapsulated the drug carrier pPB-HSA, which specifically binds to the PDGF beta R that is highly upregulated on activated myofibroblasts, into microspheres composed of hydrophilic multi-block copolymers composed of poly(L-lactide) and poly ethylene glycol/poly(is an element of-caprolactone), allowing diffusion-controlled release. Firstly, we estimated in mice with acute fibrogenesis induced by a single CCl4 injection the half-life of I-125-labeled pPB-HSA at 40 min and confirmed the preferential accumulation in fibrotic tissue. Subsequently, we determined in the Mdr2-/- mouse model of advanced biliary liver fibrosis how the subcutaneously injected microspheres released pPB-HSA into both plasma and fibrotic liver at 24 h after injection, which was maintained for six days. Although the microspheres still contained protein at day seven, pPB-HSA plasma and liver concentrations were decreased. This reduction was associated with an antibody response against the human albumin-based carrier protein, which was prevented by using a mouse albumin-based equivalent (pPB-MSA). In conclusion, this study shows that our polymeric microspheres are suitable as sustained release formulation for targeted protein constructs such as pPB-HSA. These formulations could be applied for the long-term treatment of chronic diseases such as liver fibrosis.",

keywords = "Controlled release, Biodegradable polymeric microspheres, PDGF beta-receptor targeted drug carrier, Protein delivery, in vitro in vivo correlation, Liver fibrosis, GROWTH-FACTOR RECEPTOR, DRUG-DELIVERY, ANTIFIBROTIC THERAPIES, POLYMERIC MICROSPHERES, MULTIBLOCK-COPOLYMER, INTERFERON-GAMMA, IN-VIVO, FIBROSIS, IMPLANTS, MICE",

author = "{van Dijk}, F. and N. Teekamp and L. Beljaars and E. Post and J. Zuidema and R. Steendam and Kim, {Y. O.} and Frijlink, {H. W.} and D. Schuppand and K. Poelstra and Hinrichs, {W. L. J.} and P. Olinga",

year = "2018",

month = jan,

day = "10",

doi = "10.1016/j.jconrel.2017.11.029",

language = "English",

volume = "269",

pages = "258--265",

journal = "Journal of Controlled Release",

issn = "0168-3659",

publisher = "Elsevier Bedrijfsinformatie b.v.",

}

van Dijk, F, Teekamp, N, Beljaars, L , Post, E, Zuidema, J, Steendam, R, Kim, YO, Frijlink, HW, Schuppand, D, Poelstra, K , Hinrichs, WLJ & Olinga, P 2018, 'Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver', Journal of Controlled Release, vol. 269, pp. 258-265. https://doi.org/10.1016/j.jconrel.2017.11.029

TY - JOUR

T1 - Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver

AU - van Dijk, F.

AU - Teekamp, N.

AU - Beljaars, L.

AU - Post, E.

AU - Zuidema, J.

AU - Steendam, R.

AU - Kim, Y. O.

AU - Frijlink, H. W.

AU - Schuppand, D.

AU - Poelstra, K.

AU - Hinrichs, W. L. J.

AU - Olinga, P.

PY - 2018/1/10

Y1 - 2018/1/10

N2 - Liver fibrogenesis is associated with excessive production of extracellular matrix by myofibroblasts that often leads to cirrhosis and consequently liver dysfunction and death. Novel protein-based antifibrotic drugs show high specificity and efficacy, but their use in the treatment of fibrosis causes a high burden for patients, since repetitive and long-term parenteral administration is required as most proteins and peptides are rapidly cleared from the circulation. Therefore, we developed biodegradable polymeric microspheres for the sustained release of proteinaceous drugs. We encapsulated the drug carrier pPB-HSA, which specifically binds to the PDGF beta R that is highly upregulated on activated myofibroblasts, into microspheres composed of hydrophilic multi-block copolymers composed of poly(L-lactide) and poly ethylene glycol/poly(is an element of-caprolactone), allowing diffusion-controlled release. Firstly, we estimated in mice with acute fibrogenesis induced by a single CCl4 injection the half-life of I-125-labeled pPB-HSA at 40 min and confirmed the preferential accumulation in fibrotic tissue. Subsequently, we determined in the Mdr2-/- mouse model of advanced biliary liver fibrosis how the subcutaneously injected microspheres released pPB-HSA into both plasma and fibrotic liver at 24 h after injection, which was maintained for six days. Although the microspheres still contained protein at day seven, pPB-HSA plasma and liver concentrations were decreased. This reduction was associated with an antibody response against the human albumin-based carrier protein, which was prevented by using a mouse albumin-based equivalent (pPB-MSA). In conclusion, this study shows that our polymeric microspheres are suitable as sustained release formulation for targeted protein constructs such as pPB-HSA. These formulations could be applied for the long-term treatment of chronic diseases such as liver fibrosis.

AB - Liver fibrogenesis is associated with excessive production of extracellular matrix by myofibroblasts that often leads to cirrhosis and consequently liver dysfunction and death. Novel protein-based antifibrotic drugs show high specificity and efficacy, but their use in the treatment of fibrosis causes a high burden for patients, since repetitive and long-term parenteral administration is required as most proteins and peptides are rapidly cleared from the circulation. Therefore, we developed biodegradable polymeric microspheres for the sustained release of proteinaceous drugs. We encapsulated the drug carrier pPB-HSA, which specifically binds to the PDGF beta R that is highly upregulated on activated myofibroblasts, into microspheres composed of hydrophilic multi-block copolymers composed of poly(L-lactide) and poly ethylene glycol/poly(is an element of-caprolactone), allowing diffusion-controlled release. Firstly, we estimated in mice with acute fibrogenesis induced by a single CCl4 injection the half-life of I-125-labeled pPB-HSA at 40 min and confirmed the preferential accumulation in fibrotic tissue. Subsequently, we determined in the Mdr2-/- mouse model of advanced biliary liver fibrosis how the subcutaneously injected microspheres released pPB-HSA into both plasma and fibrotic liver at 24 h after injection, which was maintained for six days. Although the microspheres still contained protein at day seven, pPB-HSA plasma and liver concentrations were decreased. This reduction was associated with an antibody response against the human albumin-based carrier protein, which was prevented by using a mouse albumin-based equivalent (pPB-MSA). In conclusion, this study shows that our polymeric microspheres are suitable as sustained release formulation for targeted protein constructs such as pPB-HSA. These formulations could be applied for the long-term treatment of chronic diseases such as liver fibrosis.

KW - Controlled release

KW - Biodegradable polymeric microspheres

KW - PDGF beta-receptor targeted drug carrier

KW - Protein delivery

KW - in vitro in vivo correlation

KW - Liver fibrosis

KW - GROWTH-FACTOR RECEPTOR

KW - DRUG-DELIVERY

KW - ANTIFIBROTIC THERAPIES

KW - POLYMERIC MICROSPHERES

KW - MULTIBLOCK-COPOLYMER

KW - INTERFERON-GAMMA

KW - IN-VIVO

KW - FIBROSIS

KW - IMPLANTS

KW - MICE

U2 - 10.1016/j.jconrel.2017.11.029

DO - 10.1016/j.jconrel.2017.11.029

M3 - Article

C2 - 29170138

SN - 0168-3659

VL - 269

SP - 258

EP - 265

JO - Journal of Controlled Release

JF - Journal of Controlled Release

ER -

Pharmacokinetics of a sustained release formulation of PDGFβ-receptor directed carrier proteins to target the fibrotic liver

Abstract

Keywords

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