Publication: A rationally designed self-immolative linker enhances the synergism between a polymer-rock inhibitor conjugate and neural progenitor cells in the treatment of spinal cord injury.
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Identifiers
Date
2021-07-24
Authors
Giraldo, E
Nebot, V J
Đorđević, S
Requejo-Aguilar, R
Alastrue-Agudo, A
Zagorodko, O
Armiñan, A
Martinez-Rojas, B
Vicent, M J
Moreno-Manzano, V
Advisors
Journal Title
Journal ISSN
Volume Title
Publisher
Elsevier
Abstract
Rho/ROCK signaling induced after spinal cord injury (SCI) contributes to secondary damage by promoting apoptosis, inflammation, and axon growth inhibition. The specific Rho-kinase inhibitor fasudil can contribute to functional regeneration after SCI, although inherent low stability has hampered its use. To improve the therapeutic potential of fasudil, we now describe a family of rationally-designed bioresponsive polymer-fasudil conjugates based on an understanding of the conditions after SCI, such as low pH, enhanced expression of specific proteases, and a reductive environment. Fasudil conjugated to poly-l-glutamate via a self-immolative redox-sensitive linker (PGA-SS-F) displays optimal release kinetics and, consequently, treatment with PGA-SS-F significantly induces neurite elongation and axon growth in dorsal root ganglia explants, spinal cord organotypic cultures, and neural precursor cells (NPCs). The intrathecal administration of PGA-SS-F after SCI in a rat model prevents early apoptosis and induces the expression of axonal growth- and neuroplasticity-associated markers to a higher extent than the free form of fasudil. Moreover, a combination treatment comprising the acute transplantation of NPCs pre-treated with PGA-SS-F leads to enhanced cell engraftment and reduced cyst formation after SCI. In chronic SCI, combinatory treatment increases the preservation of neuronal fibers. Overall, this synergistic combinatorial strategy may represent a potentially efficient clinical approach to SCI treatment.
Description
MeSH Terms
Animals
Neural stem cells
Polymers
Rats
Spinal cord injuries
rho-associated kinases
Neural stem cells
Polymers
Rats
Spinal cord injuries
rho-associated kinases
DeCS Terms
Animales
Células-madre neurales
Polímeros
Quinasas asociadas a rho
Ratas
Traumatismos de la médula espinal
Células-madre neurales
Polímeros
Quinasas asociadas a rho
Ratas
Traumatismos de la médula espinal
CIE Terms
Keywords
Axonal elongation, Fasudil, Neuroprotection, Polymer therapeutics, Polymer-drug conjugates, RhoA/ROCK Inhibitor, Spinal cord injury
Citation
Giraldo E, Nebot VJ, Đorđević S, Requejo-Aguilar R, Alastrue-Agudo A, Zagorodko O, et al. A rationally designed self-immolative linker enhances the synergism between a polymer-rock inhibitor conjugate and neural progenitor cells in the treatment of spinal cord injury. Biomaterials. 2021 Sep;276:121052