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Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment

Tendon and ligament injuries are the most common musculoskeletal injuries, which not only impact the quality of life but result in a massive economic burden. Surgical interventions for tendon/ligament injuries utilize biological and/or engineered grafts to reconstruct damaged tissue, but these have...

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Autores principales: Abdulmalik, Sama, Gallo, Jack, Nip, Jonathan, Katebifar, Sara, Arul, Michael, Lebaschi, Amir, Munch, Lucas N., Bartly, Jenna M., Choudhary, Shilpa, Kalajzic, Ivo, Banasavadi-Siddegowdae, Yeshavanth Kumar, Nukavarapu, Syam P., Kumbar, Sangamesh G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: KeAi Publishing 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9876843/
https://www.ncbi.nlm.nih.gov/pubmed/36733930
http://dx.doi.org/10.1016/j.bioactmat.2023.01.013
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author Abdulmalik, Sama
Gallo, Jack
Nip, Jonathan
Katebifar, Sara
Arul, Michael
Lebaschi, Amir
Munch, Lucas N.
Bartly, Jenna M.
Choudhary, Shilpa
Kalajzic, Ivo
Banasavadi-Siddegowdae, Yeshavanth Kumar
Nukavarapu, Syam P.
Kumbar, Sangamesh G.
author_facet Abdulmalik, Sama
Gallo, Jack
Nip, Jonathan
Katebifar, Sara
Arul, Michael
Lebaschi, Amir
Munch, Lucas N.
Bartly, Jenna M.
Choudhary, Shilpa
Kalajzic, Ivo
Banasavadi-Siddegowdae, Yeshavanth Kumar
Nukavarapu, Syam P.
Kumbar, Sangamesh G.
author_sort Abdulmalik, Sama
collection PubMed
description Tendon and ligament injuries are the most common musculoskeletal injuries, which not only impact the quality of life but result in a massive economic burden. Surgical interventions for tendon/ligament injuries utilize biological and/or engineered grafts to reconstruct damaged tissue, but these have limitations. Engineered matrices confer superior physicochemical properties over biological grafts but lack desirable bioactivity to promote tissue healing. While incorporating drugs can enhance bioactivity, large matrix surface areas and hydrophobicity can lead to uncontrolled burst release and/or incomplete release due to binding. To overcome these limitations, we evaluated the delivery of a peptide growth factor (exendin-4; Ex-4) using an enhanced nanofiber matrix in a tendon injury model. To overcome drug surface binding due to matrix hydrophobicity of poly(caprolactone) (PCL)—which would be expected to enhance cell-material interactions—we blended PCL and cellulose acetate (CA) and electrospun nanofiber matrices with fiber diameters ranging from 600 to 1000 nm. To avoid burst release and protect the drug, we encapsulated Ex-4 in the open lumen of halloysite nanotubes (HNTs), sealed the HNT tube endings with a polymer blend, and mixed Ex-4-loaded HNTs into the polymer mixture before electrospinning. This reduced burst release from ∼75% to ∼40%, but did not alter matrix morphology, fiber diameter, or tensile properties. We evaluated the bioactivity of the Ex-4 nanofiber formulation by culturing human mesenchymal stem cells (hMSCs) on matrix surfaces for 21 days and measuring tenogenic differentiation, compared with nanofiber matrices in basal media alone. Strikingly, we observed that Ex-4 nanofiber matrices accelerated the hMSC proliferation rate and elevated levels of sulfated glycosaminoglycan, tendon-related genes (Scx, Mkx, and Tnmd), and ECM-related genes (Col-I, Col-III, and Dcn), compared to control. We then assessed the safety and efficacy of Ex-4 nanofiber matrices in a full-thickness rat Achilles tendon defect with histology, marker expression, functional walking track analysis, and mechanical testing. Our analysis confirmed that Ex-4 nanofiber matrices enhanced tendon healing and reduced fibrocartilage formation versus nanofiber matrices alone. These findings implicate Ex-4 as a potentially valuable tool for tendon tissue engineering.
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spelling pubmed-98768432023-02-01 Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment Abdulmalik, Sama Gallo, Jack Nip, Jonathan Katebifar, Sara Arul, Michael Lebaschi, Amir Munch, Lucas N. Bartly, Jenna M. Choudhary, Shilpa Kalajzic, Ivo Banasavadi-Siddegowdae, Yeshavanth Kumar Nukavarapu, Syam P. Kumbar, Sangamesh G. Bioact Mater Article Tendon and ligament injuries are the most common musculoskeletal injuries, which not only impact the quality of life but result in a massive economic burden. Surgical interventions for tendon/ligament injuries utilize biological and/or engineered grafts to reconstruct damaged tissue, but these have limitations. Engineered matrices confer superior physicochemical properties over biological grafts but lack desirable bioactivity to promote tissue healing. While incorporating drugs can enhance bioactivity, large matrix surface areas and hydrophobicity can lead to uncontrolled burst release and/or incomplete release due to binding. To overcome these limitations, we evaluated the delivery of a peptide growth factor (exendin-4; Ex-4) using an enhanced nanofiber matrix in a tendon injury model. To overcome drug surface binding due to matrix hydrophobicity of poly(caprolactone) (PCL)—which would be expected to enhance cell-material interactions—we blended PCL and cellulose acetate (CA) and electrospun nanofiber matrices with fiber diameters ranging from 600 to 1000 nm. To avoid burst release and protect the drug, we encapsulated Ex-4 in the open lumen of halloysite nanotubes (HNTs), sealed the HNT tube endings with a polymer blend, and mixed Ex-4-loaded HNTs into the polymer mixture before electrospinning. This reduced burst release from ∼75% to ∼40%, but did not alter matrix morphology, fiber diameter, or tensile properties. We evaluated the bioactivity of the Ex-4 nanofiber formulation by culturing human mesenchymal stem cells (hMSCs) on matrix surfaces for 21 days and measuring tenogenic differentiation, compared with nanofiber matrices in basal media alone. Strikingly, we observed that Ex-4 nanofiber matrices accelerated the hMSC proliferation rate and elevated levels of sulfated glycosaminoglycan, tendon-related genes (Scx, Mkx, and Tnmd), and ECM-related genes (Col-I, Col-III, and Dcn), compared to control. We then assessed the safety and efficacy of Ex-4 nanofiber matrices in a full-thickness rat Achilles tendon defect with histology, marker expression, functional walking track analysis, and mechanical testing. Our analysis confirmed that Ex-4 nanofiber matrices enhanced tendon healing and reduced fibrocartilage formation versus nanofiber matrices alone. These findings implicate Ex-4 as a potentially valuable tool for tendon tissue engineering. KeAi Publishing 2023-01-20 /pmc/articles/PMC9876843/ /pubmed/36733930 http://dx.doi.org/10.1016/j.bioactmat.2023.01.013 Text en © 2023 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Abdulmalik, Sama
Gallo, Jack
Nip, Jonathan
Katebifar, Sara
Arul, Michael
Lebaschi, Amir
Munch, Lucas N.
Bartly, Jenna M.
Choudhary, Shilpa
Kalajzic, Ivo
Banasavadi-Siddegowdae, Yeshavanth Kumar
Nukavarapu, Syam P.
Kumbar, Sangamesh G.
Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment
title Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment
title_full Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment
title_fullStr Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment
title_full_unstemmed Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment
title_short Nanofiber matrix formulations for the delivery of Exendin-4 for tendon regeneration: In vitro and in vivo assessment
title_sort nanofiber matrix formulations for the delivery of exendin-4 for tendon regeneration: in vitro and in vivo assessment
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9876843/
https://www.ncbi.nlm.nih.gov/pubmed/36733930
http://dx.doi.org/10.1016/j.bioactmat.2023.01.013
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