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Safety of Autologous Human Schwann Cell Transplantation in Subacute Thoracic Spinal Cord Injury
by
Green, Barth A.
, Wood, Patrick
, Widerström-Noga, Eva
, Saraf-Lavi, Efrat
, Guest, James D.
, Dietrich, W. Dalton
, Anderson, Kim D.
, Pearse, Damien D.
, Levi, Allan D.
, Dididze, Marine
, Curiel, Rosie
, Bartlett Bunge, Mary
, Khan, Aisha
in
Adult
/ Autografts
/ Axonal plasticity
/ Axons
/ Cell adhesion & migration
/ Clinical outcomes
/ Clinical significance
/ Clinical trials
/ Humans
/ Male
/ Neurological complications
/ Neuroprotection
/ Neurosciences
/ Pain
/ Peripheral neuropathy
/ Rehabilitation
/ Safety
/ Schwann cells
/ Schwann Cells - transplantation
/ Spasticity
/ Spinal cord injuries
/ Spinal Cord Injuries - therapy
/ Stem cells
/ Sural nerve
/ Thorax
/ Transplantation
/ Transplantation, Autologous - adverse effects
/ Transplantation, Autologous - methods
/ Trauma
/ Young Adult
2017
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Safety of Autologous Human Schwann Cell Transplantation in Subacute Thoracic Spinal Cord Injury
by
Green, Barth A.
, Wood, Patrick
, Widerström-Noga, Eva
, Saraf-Lavi, Efrat
, Guest, James D.
, Dietrich, W. Dalton
, Anderson, Kim D.
, Pearse, Damien D.
, Levi, Allan D.
, Dididze, Marine
, Curiel, Rosie
, Bartlett Bunge, Mary
, Khan, Aisha
in
Adult
/ Autografts
/ Axonal plasticity
/ Axons
/ Cell adhesion & migration
/ Clinical outcomes
/ Clinical significance
/ Clinical trials
/ Humans
/ Male
/ Neurological complications
/ Neuroprotection
/ Neurosciences
/ Pain
/ Peripheral neuropathy
/ Rehabilitation
/ Safety
/ Schwann cells
/ Schwann Cells - transplantation
/ Spasticity
/ Spinal cord injuries
/ Spinal Cord Injuries - therapy
/ Stem cells
/ Sural nerve
/ Thorax
/ Transplantation
/ Transplantation, Autologous - adverse effects
/ Transplantation, Autologous - methods
/ Trauma
/ Young Adult
2017
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Safety of Autologous Human Schwann Cell Transplantation in Subacute Thoracic Spinal Cord Injury
by
Green, Barth A.
, Wood, Patrick
, Widerström-Noga, Eva
, Saraf-Lavi, Efrat
, Guest, James D.
, Dietrich, W. Dalton
, Anderson, Kim D.
, Pearse, Damien D.
, Levi, Allan D.
, Dididze, Marine
, Curiel, Rosie
, Bartlett Bunge, Mary
, Khan, Aisha
in
Adult
/ Autografts
/ Axonal plasticity
/ Axons
/ Cell adhesion & migration
/ Clinical outcomes
/ Clinical significance
/ Clinical trials
/ Humans
/ Male
/ Neurological complications
/ Neuroprotection
/ Neurosciences
/ Pain
/ Peripheral neuropathy
/ Rehabilitation
/ Safety
/ Schwann cells
/ Schwann Cells - transplantation
/ Spasticity
/ Spinal cord injuries
/ Spinal Cord Injuries - therapy
/ Stem cells
/ Sural nerve
/ Thorax
/ Transplantation
/ Transplantation, Autologous - adverse effects
/ Transplantation, Autologous - methods
/ Trauma
/ Young Adult
2017
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Safety of Autologous Human Schwann Cell Transplantation in Subacute Thoracic Spinal Cord Injury
Journal Article
Safety of Autologous Human Schwann Cell Transplantation in Subacute Thoracic Spinal Cord Injury
2017
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Overview
The rationale for implantation of autologous human Schwann cells (SCs) in persons with subacute spinal cord injury (SCI) is based on evidence that transplanted SCs are neuroprotective, support local axonal plasticity, and are capable of myelinating axons. A Phase I clinical trial was conducted to evaluate the safety of autologous human SC transplantation into the injury epicenter of six subjects with subacute SCI. The trial was an open-label, unblinded, non-randomized, non-placebo controlled study with a dose escalation design and standard medical rehabilitation. Participants were paraplegics with neurologically complete, trauma-induced spinal lesions. Autologous SCs were cultured in vitro from a sural nerve harvested from each participant and injected into the epicenter of the spinal lesion. Outcome measures for safety were protocol compliance, feasibility, adverse events, stability of neurological level, absence of detectable mass lesion, and the emergence of clinically significant neuropathic pain or muscle spasticity no greater than expected for a natural course cohort. One year post-transplantation, there were no surgical, medical, or neurological complications to indicate that the timing or procedure for the cell transplantation was unsafe. There were no adverse events or serious adverse events related to the cell therapy. There was no evidence of additional spinal cord damage, mass lesion, or syrinx formation. We conclude that it is feasible to identify eligible candidates, appropriately obtain informed consent, perform a peripheral nerve harvest to obtain SCs within 5–30 days of injury, and perform an intra-spinal transplantation of highly purified autologous SCs within 4–7 weeks of injury.
Publisher
SAGE Publications,Mary Ann Liebert, Inc
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