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Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation

Systemically delivered NEL-like molecule-1 (NELL-1), a potent pro-osteogenic protein, promotes bone formation in healthy and osteoporotic mouse models. PEGylation of NELL-1 (NELL-PEG) increases the half-life of the protein in a mouse model without compromising its osteogenic potential, thereby impro...

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Autores principales: Tanjaya, Justine, Zhang, Yulong, Lee, Soonchul, Shi, Jiayu, Chen, Eric, Ang, Pia, Zhang, Xinli, Tetradis, Sotirios, Ting, Kang, Wu, Benjamin, Soo, Chia, Kwak, Jin Hee
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Mary Ann Liebert, Inc. 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4921932/
https://www.ncbi.nlm.nih.gov/pubmed/27354930
http://dx.doi.org/10.1089/biores.2016.0018
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author Tanjaya, Justine
Zhang, Yulong
Lee, Soonchul
Shi, Jiayu
Chen, Eric
Ang, Pia
Zhang, Xinli
Tetradis, Sotirios
Ting, Kang
Wu, Benjamin
Soo, Chia
Kwak, Jin Hee
author_facet Tanjaya, Justine
Zhang, Yulong
Lee, Soonchul
Shi, Jiayu
Chen, Eric
Ang, Pia
Zhang, Xinli
Tetradis, Sotirios
Ting, Kang
Wu, Benjamin
Soo, Chia
Kwak, Jin Hee
author_sort Tanjaya, Justine
collection PubMed
description Systemically delivered NEL-like molecule-1 (NELL-1), a potent pro-osteogenic protein, promotes bone formation in healthy and osteoporotic mouse models. PEGylation of NELL-1 (NELL-PEG) increases the half-life of the protein in a mouse model without compromising its osteogenic potential, thereby improving its pharmacokinetics upon systemic delivery. This study consists of a twofold approach: a biodistribution test and an in vivo osteogenic potential test. The biodistribution test compared two commonly used administration methods for drug delivery other than intravenous—intraperitoneal (IP) and subcutaneous (SC)—to examine NELL-PEG biodistribution in mice. Compared to a single-dose SC injection (1.25 mg/kg), a single-dose IP administration yielded a higher protein uptake in the targeted bone sites. When the IP injection dose was doubled to 2.5 mg/kg, the protein remained in the femurs, tibias, and vertebrae for up to 72 h. Next, based on the results of the biodistribution study, IP administration was selected to further investigate the in vivo osteogenic effects of weekly NELL-PEG injection (q7d). In vivo, the IP administered NELL-PEG group showed significantly greater bone mineral density, bone volume fraction, and trabecular bone formation in the targeted bone sites compared to the phosphate-buffered saline control. In summary, weekly NELL-PEG injection via IP administration successfully enhanced the overall bone quality. These findings demonstrate that systemic delivery of NELL-PEG via IP administration may serve as an effective osteogenic therapy for preventing and treating osteoporosis.
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spelling pubmed-49219322016-06-28 Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation Tanjaya, Justine Zhang, Yulong Lee, Soonchul Shi, Jiayu Chen, Eric Ang, Pia Zhang, Xinli Tetradis, Sotirios Ting, Kang Wu, Benjamin Soo, Chia Kwak, Jin Hee Biores Open Access Original Research Article Systemically delivered NEL-like molecule-1 (NELL-1), a potent pro-osteogenic protein, promotes bone formation in healthy and osteoporotic mouse models. PEGylation of NELL-1 (NELL-PEG) increases the half-life of the protein in a mouse model without compromising its osteogenic potential, thereby improving its pharmacokinetics upon systemic delivery. This study consists of a twofold approach: a biodistribution test and an in vivo osteogenic potential test. The biodistribution test compared two commonly used administration methods for drug delivery other than intravenous—intraperitoneal (IP) and subcutaneous (SC)—to examine NELL-PEG biodistribution in mice. Compared to a single-dose SC injection (1.25 mg/kg), a single-dose IP administration yielded a higher protein uptake in the targeted bone sites. When the IP injection dose was doubled to 2.5 mg/kg, the protein remained in the femurs, tibias, and vertebrae for up to 72 h. Next, based on the results of the biodistribution study, IP administration was selected to further investigate the in vivo osteogenic effects of weekly NELL-PEG injection (q7d). In vivo, the IP administered NELL-PEG group showed significantly greater bone mineral density, bone volume fraction, and trabecular bone formation in the targeted bone sites compared to the phosphate-buffered saline control. In summary, weekly NELL-PEG injection via IP administration successfully enhanced the overall bone quality. These findings demonstrate that systemic delivery of NELL-PEG via IP administration may serve as an effective osteogenic therapy for preventing and treating osteoporosis. Mary Ann Liebert, Inc. 2016-06-01 /pmc/articles/PMC4921932/ /pubmed/27354930 http://dx.doi.org/10.1089/biores.2016.0018 Text en © Justine Tanjaya et al. 2016; Published by Mary Ann Liebert, Inc. This Open Access article is distributed under the terms of the Creative Commons License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited.
spellingShingle Original Research Article
Tanjaya, Justine
Zhang, Yulong
Lee, Soonchul
Shi, Jiayu
Chen, Eric
Ang, Pia
Zhang, Xinli
Tetradis, Sotirios
Ting, Kang
Wu, Benjamin
Soo, Chia
Kwak, Jin Hee
Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation
title Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation
title_full Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation
title_fullStr Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation
title_full_unstemmed Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation
title_short Efficacy of Intraperitoneal Administration of PEGylated NELL-1 for Bone Formation
title_sort efficacy of intraperitoneal administration of pegylated nell-1 for bone formation
topic Original Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4921932/
https://www.ncbi.nlm.nih.gov/pubmed/27354930
http://dx.doi.org/10.1089/biores.2016.0018
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