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Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons

Cell therapy in experimental models of Parkinson's disease replaces the lost dopamine neurons (DAN), but we still need improved methods to guide dopaminergic axons (DAx) of grafted neurons to make proper connections. The protein Semaphorin 3C (Sema3C) attracts DAN axons and enhances their growt...

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Autores principales: Carballo-Molina, Oscar A., Sánchez-Navarro, Andrea, López-Ornelas, Adolfo, Lara-Rodarte, Rolando, Salazar, Patricia, Campos-Romo, Aurelio, Ramos-Mejía, Verónica, Velasco, Iván
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Mary Ann Liebert, Inc. 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4913502/
https://www.ncbi.nlm.nih.gov/pubmed/27174503
http://dx.doi.org/10.1089/ten.tea.2016.0008
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author Carballo-Molina, Oscar A.
Sánchez-Navarro, Andrea
López-Ornelas, Adolfo
Lara-Rodarte, Rolando
Salazar, Patricia
Campos-Romo, Aurelio
Ramos-Mejía, Verónica
Velasco, Iván
author_facet Carballo-Molina, Oscar A.
Sánchez-Navarro, Andrea
López-Ornelas, Adolfo
Lara-Rodarte, Rolando
Salazar, Patricia
Campos-Romo, Aurelio
Ramos-Mejía, Verónica
Velasco, Iván
author_sort Carballo-Molina, Oscar A.
collection PubMed
description Cell therapy in experimental models of Parkinson's disease replaces the lost dopamine neurons (DAN), but we still need improved methods to guide dopaminergic axons (DAx) of grafted neurons to make proper connections. The protein Semaphorin 3C (Sema3C) attracts DAN axons and enhances their growth. In this work, we show that the hydrogel PuraMatrix, a self-assembling peptide-based matrix, incorporates Sema3C and releases it steadily during 4 weeks. We also tested if hydrogel-delivered Sema3C attracts DAx using a system of rat midbrain explants embedded in collagen gels. We show that Sema3C released by this hydrogel attracts DAx, in a similar way to pretectum, which is known to attract growing DAN axons. We assessed the effect of Sema3C on the growth of DAx using microfluidic devices. DAN from rat midbrain or those differentiated from human embryonic stem cells showed enhanced axonal extension when exposed to hydrogel-released Sema3C, similar to soluble Sema3C. Notably, DAN of human origin express the cognate Sema3C receptors, Neuropilin1 and Neuropilin2. These results show that PuraMatrix is able to incorporate and release Sema3C, and such delivery guides and promotes the axonal growth of DAN. This biocompatible hydrogel might be useful as a Sema3C carrier for in vivo studies in parkinsonian animal models.
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spelling pubmed-49135022016-07-06 Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons Carballo-Molina, Oscar A. Sánchez-Navarro, Andrea López-Ornelas, Adolfo Lara-Rodarte, Rolando Salazar, Patricia Campos-Romo, Aurelio Ramos-Mejía, Verónica Velasco, Iván Tissue Eng Part A Original Articles Cell therapy in experimental models of Parkinson's disease replaces the lost dopamine neurons (DAN), but we still need improved methods to guide dopaminergic axons (DAx) of grafted neurons to make proper connections. The protein Semaphorin 3C (Sema3C) attracts DAN axons and enhances their growth. In this work, we show that the hydrogel PuraMatrix, a self-assembling peptide-based matrix, incorporates Sema3C and releases it steadily during 4 weeks. We also tested if hydrogel-delivered Sema3C attracts DAx using a system of rat midbrain explants embedded in collagen gels. We show that Sema3C released by this hydrogel attracts DAx, in a similar way to pretectum, which is known to attract growing DAN axons. We assessed the effect of Sema3C on the growth of DAx using microfluidic devices. DAN from rat midbrain or those differentiated from human embryonic stem cells showed enhanced axonal extension when exposed to hydrogel-released Sema3C, similar to soluble Sema3C. Notably, DAN of human origin express the cognate Sema3C receptors, Neuropilin1 and Neuropilin2. These results show that PuraMatrix is able to incorporate and release Sema3C, and such delivery guides and promotes the axonal growth of DAN. This biocompatible hydrogel might be useful as a Sema3C carrier for in vivo studies in parkinsonian animal models. Mary Ann Liebert, Inc. 2016-06-01 2016-06-01 /pmc/articles/PMC4913502/ /pubmed/27174503 http://dx.doi.org/10.1089/ten.tea.2016.0008 Text en © Oscar A. Carballo-Molina, et al., 2016; published by Mary Ann Liebert, Inc. This Open Access article is distributed under the terms of the Creative Commons Attribution Noncommercial License (http://creativecommons.org/licenses/by-nc/4.0/) which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and the source are credited.
spellingShingle Original Articles
Carballo-Molina, Oscar A.
Sánchez-Navarro, Andrea
López-Ornelas, Adolfo
Lara-Rodarte, Rolando
Salazar, Patricia
Campos-Romo, Aurelio
Ramos-Mejía, Verónica
Velasco, Iván
Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons
title Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons
title_full Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons
title_fullStr Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons
title_full_unstemmed Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons
title_short Semaphorin 3C Released from a Biocompatible Hydrogel Guides and Promotes Axonal Growth of Rodent and Human Dopaminergic Neurons
title_sort semaphorin 3c released from a biocompatible hydrogel guides and promotes axonal growth of rodent and human dopaminergic neurons
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4913502/
https://www.ncbi.nlm.nih.gov/pubmed/27174503
http://dx.doi.org/10.1089/ten.tea.2016.0008
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