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A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests

Background: Alzheimer’s disease (AD), along with other neurodegenerative disorders, remains a challenge for clinicians, mainly because of the incomplete knowledge surrounding its etiology and inefficient therapeutic options. Considering the central role of amyloid beta (Aβ) in the onset and evolutio...

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Autores principales: Schreiner, Thomas Gabriel, Menéndez-González, Manuel, Adam, Maricel, Popescu, Bogdan Ovidiu, Szilagyi, Andrei, Stanciu, Gabriela Dumitrita, Tamba, Bogdan Ionel, Ciobanu, Romeo Cristian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10669467/
https://www.ncbi.nlm.nih.gov/pubmed/38002427
http://dx.doi.org/10.3390/bioengineering10111303
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author Schreiner, Thomas Gabriel
Menéndez-González, Manuel
Adam, Maricel
Popescu, Bogdan Ovidiu
Szilagyi, Andrei
Stanciu, Gabriela Dumitrita
Tamba, Bogdan Ionel
Ciobanu, Romeo Cristian
author_facet Schreiner, Thomas Gabriel
Menéndez-González, Manuel
Adam, Maricel
Popescu, Bogdan Ovidiu
Szilagyi, Andrei
Stanciu, Gabriela Dumitrita
Tamba, Bogdan Ionel
Ciobanu, Romeo Cristian
author_sort Schreiner, Thomas Gabriel
collection PubMed
description Background: Alzheimer’s disease (AD), along with other neurodegenerative disorders, remains a challenge for clinicians, mainly because of the incomplete knowledge surrounding its etiology and inefficient therapeutic options. Considering the central role of amyloid beta (Aβ) in the onset and evolution of AD, Aβ-targeted therapies are among the most promising research directions. In the context of decreased Aβ elimination from the central nervous system in the AD patient, the authors propose a novel therapeutic approach based on the “Cerebrospinal Fluid Sink Therapeutic Strategy” presented in previous works. This article aims to demonstrate the laborious process of the development and testing of an effective nanoporous ceramic filter, which is the main component of an experimental device capable of filtrating Aβ from the cerebrospinal fluid in an AD mouse model. Methods: First, the authors present the main steps needed to create a functional filtrating nanoporous ceramic filter, which represents the central part of the experimental filtration device. This process included synthesis, functionalization, and quality control of the functionalization, which were performed via various spectroscopy methods and thermal analysis, selectivity measurements, and a biocompatibility assessment. Subsequently, the prototype was implanted in APP/PS1 mice for four weeks, then removed, and the nanoporous ceramic filter was tested for its filtration capacity and potential structural damages. Results: In applying the multi-step protocol, the authors developed a functional Aβ-selective filtration nanoporous ceramic filter that was used within the prototype. All animal models survived the implantation procedure and had no significant adverse effects during the 4-week trial period. Post-treatment analysis of the nanoporous ceramic filter showed significant protein loading, but no complete clogging of the pores. Conclusions: We demonstrated that a nanoporous ceramic filter-based system that filtrates Aβ from the cerebrospinal fluid is a feasible and safe treatment modality in the AD mouse model. The presented prototype has a functional lifespan of around four weeks, highlighting the need to develop advanced nanoporous ceramic filters with anti-biofouling properties to ensure the long-term action of this therapy.
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spelling pubmed-106694672023-11-10 A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests Schreiner, Thomas Gabriel Menéndez-González, Manuel Adam, Maricel Popescu, Bogdan Ovidiu Szilagyi, Andrei Stanciu, Gabriela Dumitrita Tamba, Bogdan Ionel Ciobanu, Romeo Cristian Bioengineering (Basel) Article Background: Alzheimer’s disease (AD), along with other neurodegenerative disorders, remains a challenge for clinicians, mainly because of the incomplete knowledge surrounding its etiology and inefficient therapeutic options. Considering the central role of amyloid beta (Aβ) in the onset and evolution of AD, Aβ-targeted therapies are among the most promising research directions. In the context of decreased Aβ elimination from the central nervous system in the AD patient, the authors propose a novel therapeutic approach based on the “Cerebrospinal Fluid Sink Therapeutic Strategy” presented in previous works. This article aims to demonstrate the laborious process of the development and testing of an effective nanoporous ceramic filter, which is the main component of an experimental device capable of filtrating Aβ from the cerebrospinal fluid in an AD mouse model. Methods: First, the authors present the main steps needed to create a functional filtrating nanoporous ceramic filter, which represents the central part of the experimental filtration device. This process included synthesis, functionalization, and quality control of the functionalization, which were performed via various spectroscopy methods and thermal analysis, selectivity measurements, and a biocompatibility assessment. Subsequently, the prototype was implanted in APP/PS1 mice for four weeks, then removed, and the nanoporous ceramic filter was tested for its filtration capacity and potential structural damages. Results: In applying the multi-step protocol, the authors developed a functional Aβ-selective filtration nanoporous ceramic filter that was used within the prototype. All animal models survived the implantation procedure and had no significant adverse effects during the 4-week trial period. Post-treatment analysis of the nanoporous ceramic filter showed significant protein loading, but no complete clogging of the pores. Conclusions: We demonstrated that a nanoporous ceramic filter-based system that filtrates Aβ from the cerebrospinal fluid is a feasible and safe treatment modality in the AD mouse model. The presented prototype has a functional lifespan of around four weeks, highlighting the need to develop advanced nanoporous ceramic filters with anti-biofouling properties to ensure the long-term action of this therapy. MDPI 2023-11-10 /pmc/articles/PMC10669467/ /pubmed/38002427 http://dx.doi.org/10.3390/bioengineering10111303 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Schreiner, Thomas Gabriel
Menéndez-González, Manuel
Adam, Maricel
Popescu, Bogdan Ovidiu
Szilagyi, Andrei
Stanciu, Gabriela Dumitrita
Tamba, Bogdan Ionel
Ciobanu, Romeo Cristian
A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests
title A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests
title_full A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests
title_fullStr A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests
title_full_unstemmed A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests
title_short A Nanostructured Protein Filtration Device for Possible Use in the Treatment of Alzheimer’s Disease—Concept and Feasibility after In Vivo Tests
title_sort nanostructured protein filtration device for possible use in the treatment of alzheimer’s disease—concept and feasibility after in vivo tests
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10669467/
https://www.ncbi.nlm.nih.gov/pubmed/38002427
http://dx.doi.org/10.3390/bioengineering10111303
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