Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury

Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury

Intraspinal quisqualic acid (QUIS) injury induce (i) mechanical and thermal hyperalgesia, (ii) progressive self-injurious overgrooming of the affected dermatome. The latter is thought to resemble painful dysesthesia observed in spinal cord injury (SCI) patients. We have reported previously loss of...

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Main Authors: Jeung Woon eLee, Stanislava eJergova, Orion eFurmanski, Shyam eGajavelli, Jacqueline eSagen
Format: Article
Language:English
Published: Frontiers Media S.A. 2012-05-01
Series:Frontiers in Physiology
Subjects:
Quisqualic Acid
Transplantation
GABA
cortical progenitor cells
spinal cord injury
neuropathic pain
Online Access:http://journal.frontiersin.org/Journal/10.3389/fphys.2012.00167/full
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spelling doaj-ab000e43129d4010ad740620afbd9ced2020-11-24T23:00:51ZengFrontiers Media S.A.Frontiers in Physiology1664-042X2012-05-01310.3389/fphys.2012.0016724021Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injuryJeung Woon eLee0Jeung Woon eLee1Stanislava eJergova2Stanislava eJergova3Orion eFurmanski4Orion eFurmanski5Shyam eGajavelli6Jacqueline eSagen7University of Miami Miller School of MedicineWilliam Paterson UniversityUniversity of Miami Miller School of MedicineInstitute of Neurobiology, CE, Slovak Academy of ScienceUniversity of Miami Miller School of MedicineJohns Hopkins School of MedicineUniversity of Miami Miller School of MedicineUniversity of Miami Miller School of MedicineIntraspinal quisqualic acid (QUIS) injury induce (i) mechanical and thermal hyperalgesia, (ii) progressive self-injurious overgrooming of the affected dermatome. The latter is thought to resemble painful dysesthesia observed in spinal cord injury (SCI) patients. We have reported previously loss of endogenous GABA immunoreactive (IR) cells in the superficial dorsal horn of QUIS rats 2 weeks post-injury. Further histological evaluation showed that GABA-, glycine-, and synaptic vesicular transporter VIAAT-IR persisted but were substantially decreased in the injured spinal cord. In this study, partially-differentiated GABA-IR embryonic neural precursor cells (NPCs) were transplanted into the spinal cord of QUIS rats to reverse overgrooming by replenishing lost inhibitory circuitry. Rat E14 NPCs were predifferentiated in 0.1 ng/ml FGF-2 for 4 hrs prior to transplantation. In vitro immunocytochemistry of transplant cohort showed large population of GABA-IR NPCs that double labeled with nestin but few co-localized with NeuN, indicating partial maturation. Two weeks following QUIS lesion at T12-L1, and following the onset of overgrooming, NPCs were transplanted into the QUIS lesion sites; bovine adrenal fibroblast cells were used as control. Overgrooming was reduced in >55.5% of NPC grafted animals, with inverse relationship between the number of surviving GABA-IR cells and the size of overgrooming. Fibroblast-control animals showed a progressive worsening of overgrooming. At 3 weeks post-transplantation, numerous GABA-, nestin-, and GFAP-IR cells were present in the lesion site. Surviving grafted GABA-IR NPCs were NeuN+ and GFAP-. These results indicate that partially-differentiated NPCs survive and differentiate in vivo into neuronal cells following transplantation into an injured spinal cord. GABA-IR NPC transplants can restore lost dorsal horn inhibitory signaling and are useful in alleviating central pain following SCI.http://journal.frontiersin.org/Journal/10.3389/fphys.2012.00167/fullQuisqualic AcidTransplantationGABAcortical progenitor cellsspinal cord injuryneuropathic pain
collection DOAJ
language English
format Article
sources DOAJ
author Jeung Woon eLee
Jeung Woon eLee
Stanislava eJergova
Stanislava eJergova
Orion eFurmanski
Orion eFurmanski
Shyam eGajavelli
Jacqueline eSagen
spellingShingle Jeung Woon eLee
Jeung Woon eLee
Stanislava eJergova
Stanislava eJergova
Orion eFurmanski
Orion eFurmanski
Shyam eGajavelli
Jacqueline eSagen
Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
Frontiers in Physiology
Quisqualic Acid
Transplantation
GABA
cortical progenitor cells
spinal cord injury
neuropathic pain
author_facet Jeung Woon eLee
Jeung Woon eLee
Stanislava eJergova
Stanislava eJergova
Orion eFurmanski
Orion eFurmanski
Shyam eGajavelli
Jacqueline eSagen
author_sort Jeung Woon eLee
title Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
title_short Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
title_full Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
title_fullStr Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
title_full_unstemmed Pre-differentiated GABAergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
title_sort pre-differentiated gabaergic neural precursor transplants for alleviation of dysesthetic central pain following excitotoxic spinal cord injury
publisher Frontiers Media S.A.
series Frontiers in Physiology
issn 1664-042X
publishDate 2012-05-01
description Intraspinal quisqualic acid (QUIS) injury induce (i) mechanical and thermal hyperalgesia, (ii) progressive self-injurious overgrooming of the affected dermatome. The latter is thought to resemble painful dysesthesia observed in spinal cord injury (SCI) patients. We have reported previously loss of endogenous GABA immunoreactive (IR) cells in the superficial dorsal horn of QUIS rats 2 weeks post-injury. Further histological evaluation showed that GABA-, glycine-, and synaptic vesicular transporter VIAAT-IR persisted but were substantially decreased in the injured spinal cord. In this study, partially-differentiated GABA-IR embryonic neural precursor cells (NPCs) were transplanted into the spinal cord of QUIS rats to reverse overgrooming by replenishing lost inhibitory circuitry. Rat E14 NPCs were predifferentiated in 0.1 ng/ml FGF-2 for 4 hrs prior to transplantation. In vitro immunocytochemistry of transplant cohort showed large population of GABA-IR NPCs that double labeled with nestin but few co-localized with NeuN, indicating partial maturation. Two weeks following QUIS lesion at T12-L1, and following the onset of overgrooming, NPCs were transplanted into the QUIS lesion sites; bovine adrenal fibroblast cells were used as control. Overgrooming was reduced in >55.5% of NPC grafted animals, with inverse relationship between the number of surviving GABA-IR cells and the size of overgrooming. Fibroblast-control animals showed a progressive worsening of overgrooming. At 3 weeks post-transplantation, numerous GABA-, nestin-, and GFAP-IR cells were present in the lesion site. Surviving grafted GABA-IR NPCs were NeuN+ and GFAP-. These results indicate that partially-differentiated NPCs survive and differentiate in vivo into neuronal cells following transplantation into an injured spinal cord. GABA-IR NPC transplants can restore lost dorsal horn inhibitory signaling and are useful in alleviating central pain following SCI.
topic Quisqualic Acid
Transplantation
GABA
cortical progenitor cells
spinal cord injury
neuropathic pain
url http://journal.frontiersin.org/Journal/10.3389/fphys.2012.00167/full
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