Publications by authors named "H Altinova"

Schwann cell (SC) transplantation represents a promising therapeutic approach for traumatic spinal cord injury but is frustrated by barrier formation, preventing cell migration, and axonal regeneration at the interface between grafted SCs and reactive resident astrocytes (ACs). Although regenerating axons successfully extend into SC grafts, only a few cross the SC-AC interface to re-enter lesioned neuropil. To date, research has focused on identifying and modifying the molecular mechanisms underlying such scarring cell-cell interactions, while the influence of substrate topography remains largely unexplored.

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Article Synopsis
  • Researchers have developed various strategies to enhance tissue repair after spinal cord injuries, focusing on using bioengineered scaffolds to bridge damaged areas.
  • The study utilized light and electron microscopy to analyze the scarring process after implantation of a collagen scaffold in rat spinal cords, revealing tightly packed, uniform cells present at both the repair site and scaffold-host interface.
  • These findings suggest that the scarring tissue contains specialized cells resembling perineurial cells, emphasizing the complexity of the healing process following spinal cord injuries and the challenges tied to scaffold integration.
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Background: Molecular composition and topography of the extracellular matrix (ECM) influence regenerative cell migration following peripheral nerve injury (PNI). Advanced tissue engineering strategies for the repair of neurotmesis-type PNI include the development of nanofiber-containing implantable scaffolds that mimic features of the ECM to orchestrate regenerative growth. Reliable and quantifiable in vitro assays are required to assess the ability of such substrates to influence migration of the cell types of interest.

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Severe spinal cord injury (SCI) results in permanent functional deficits, which despite pre-clinical advances, remain untreatable. Combinational approaches, including the implantation of bioengineered scaffolds are likely to promote significant tissue repair. However, this critically depends on the extent to which host tissue can integrate with the implant.

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