TY - JOUR
T1 - Polycaprolactone/graphene oxide/acellular matrix nanofibrous scaffolds with antioxidant and promyelinating features for the treatment of peripheral demyelinating diseases
AU - Nagarajan, Aishwarya
AU - Rizwana, Nasera
AU - Abraham, Michelle
AU - Bhat, Mahima
AU - Vetekar, Aakanksha
AU - Thakur, Goutam
AU - Chakraborty, Uttara
AU - Agarwal, Vipul
AU - Nune, Manasa
N1 - Funding Information:
The authors VA and MN acknowledge the University of New South Wales-Manipal Academy of Higher Education (UNSW-MAHE) collaborative research seed funding. MN would also like to acknowledge the Department of Science & Technology, India for the SERB start-up research grant (SRG/2019/002130) and SERB-POWER research grants (SPG/2021/003703). We also thank Manipal Institute of Regenerative Medicine, MAHE for the infrastructural support. We thank Dr. Shounak De, Associate Professor, Manipal Institute of Technology, India for providing us with the Graphene oxide. The authors acknowledge the facilities and the scientific and technical assistance of Microscopy Australia at the Electron Microscope Unit (EMU) within the Mark Wainwright Analytical Center (MWAC) at UNSW Sydney. The authors acknowledge that the schematic illustrations were created with BioRender.com.
Funding Information:
The authors VA and MN acknowledge the University of New South Wales-Manipal Academy of Higher Education (UNSW-MAHE) collaborative research seed funding. MN would also like to acknowledge the Department of Science & Technology, India for the SERB start-up research grant (SRG/2019/002130) and SERB-POWER research grants (SPG/2021/003703). We also thank Manipal Institute of Regenerative Medicine, MAHE for the infrastructural support. We thank Dr. Shounak De, Associate Professor, Manipal Institute of Technology, India for providing us with the Graphene oxide. The authors acknowledge the facilities and the scientific and technical assistance of Microscopy Australia at the Electron Microscope Unit (EMU) within the Mark Wainwright Analytical Center (MWAC) at UNSW Sydney. The authors acknowledge that the schematic illustrations were created with BioRender.com.
Publisher Copyright:
© 2023, The Author(s).
PY - 2023/10/5
Y1 - 2023/10/5
N2 - Peripheral demyelinating diseases entail damage to axons and Schwann cells in the peripheral nervous system. Because of poor prognosis and lack of a cure, this group of diseases has a global impact. The primary underlying cause of these diseases involves the inability of Schwann cells to remyelinate the damaged insulating myelin around axons, resulting in neuronal death over time. In the past decade, extensive research has been directed in the direction of Schwann cells focusing on their physiological and neuroprotective effects on the neurons in the peripheral nervous system. One cause of dysregulation in the remyelinating function of Schwann cells has been associated with oxidative stress. Tissue-engineered biodegradable scaffolds that can stimulate remyelination response in Schwann cells have been proposed as a potential treatment strategy for peripheral demyelinating diseases. However, strategies developed to date primarily focussed on either remyelination or oxidative stress in isolation. Here, we have developed a multifunctional nanofibrous scaffold with material and biochemical cues to tackle both remyelination and oxidative stress in one matrix. We developed a nanofibrous scaffold using polycaprolactone (PCL) as a foundation loaded with antioxidant graphene oxide (GO) and coated this bioscaffold with Schwann cell acellular matrix. In vitro studies revealed both antioxidant and remyelination properties of the developed bioscaffold. Based on the results, the developed multifunctional bioscaffold approach can be a promising biomaterial approach for treating demyelinating diseases. Graphical Abstract: [Figure not available: see fulltext.].
AB - Peripheral demyelinating diseases entail damage to axons and Schwann cells in the peripheral nervous system. Because of poor prognosis and lack of a cure, this group of diseases has a global impact. The primary underlying cause of these diseases involves the inability of Schwann cells to remyelinate the damaged insulating myelin around axons, resulting in neuronal death over time. In the past decade, extensive research has been directed in the direction of Schwann cells focusing on their physiological and neuroprotective effects on the neurons in the peripheral nervous system. One cause of dysregulation in the remyelinating function of Schwann cells has been associated with oxidative stress. Tissue-engineered biodegradable scaffolds that can stimulate remyelination response in Schwann cells have been proposed as a potential treatment strategy for peripheral demyelinating diseases. However, strategies developed to date primarily focussed on either remyelination or oxidative stress in isolation. Here, we have developed a multifunctional nanofibrous scaffold with material and biochemical cues to tackle both remyelination and oxidative stress in one matrix. We developed a nanofibrous scaffold using polycaprolactone (PCL) as a foundation loaded with antioxidant graphene oxide (GO) and coated this bioscaffold with Schwann cell acellular matrix. In vitro studies revealed both antioxidant and remyelination properties of the developed bioscaffold. Based on the results, the developed multifunctional bioscaffold approach can be a promising biomaterial approach for treating demyelinating diseases. Graphical Abstract: [Figure not available: see fulltext.].
UR - https://www.scopus.com/pages/publications/85173174085
UR - https://www.scopus.com/pages/publications/85173174085#tab=citedBy
U2 - 10.1007/s10856-023-06750-2
DO - 10.1007/s10856-023-06750-2
M3 - Article
C2 - 37796399
AN - SCOPUS:85173174085
SN - 0957-4530
VL - 34
SP - 49
JO - Journal of materials science. Materials in medicine
JF - Journal of materials science. Materials in medicine
IS - 10
M1 - 49
ER -