Neuroprotective and behavioral efficacy of nerve growth factor-transfected hippocampal progenitor cell transplants after experimental traumatic brain injury

Philips, Matthew F.; Mattiasson, Gustav; Wieloch, Tadeusz; Björklund, Anders; Johansson, Barbro; Tomasevic, Gregor; Martinez-Serrano, Alberto; Lenzlinger, Philipp M.; Sinson, Grant; Grady, M. Sean; McIntosh, Tracy K.

Neuroprotective and behavioral efficacy of nerve growth factor-transfected hippocampal progenitor cell transplants after experimental traumatic brain injury

Mark

Philips, Matthew F. ; Mattiasson, Gustav ^LU ; Wieloch, Tadeusz ^LU ; Björklund, Anders ^LU

; Johansson, Barbro ^LU ; Tomasevic, Gregor ^LU ; Martinez-Serrano, Alberto ; Lenzlinger, Philipp M. ; Sinson, Grant and Grady, M. Sean , et al. (2001) In Journal of Neurosurgery 94(5). p.765-765

Abstract: OBJECT: Immortalized neural progenitor cells derived from embryonic rat hippocampus (HiB5), were transduced ex vivo with the gene for mouse nerve growth factor (NGF) to secrete NGF (NGF-HiB5) at 2 ng/hr/10(5) cells in culture. METHODS: Fifty-nine male Wistar rats weighing 300 to 370 g each were anesthetized with 60 mg/kg sodium pentobarbital and subjected to lateral fluid-percussion brain injury of moderate severity (2.3-2.4 atm, 34 rats) or sham injury (25 rats). At 24 hours postinjury, 2 microl (150,000 cells/microl) of [3H]thymidine-labeled NGF-HiB5 cells were transplanted stereotactically into three individual sites in the cerebral cortex adjacent to the injury site (14 rats). Separate groups of brain-injured rats received... (More); OBJECT: Immortalized neural progenitor cells derived from embryonic rat hippocampus (HiB5), were transduced ex vivo with the gene for mouse nerve growth factor (NGF) to secrete NGF (NGF-HiB5) at 2 ng/hr/10(5) cells in culture. METHODS: Fifty-nine male Wistar rats weighing 300 to 370 g each were anesthetized with 60 mg/kg sodium pentobarbital and subjected to lateral fluid-percussion brain injury of moderate severity (2.3-2.4 atm, 34 rats) or sham injury (25 rats). At 24 hours postinjury, 2 microl (150,000 cells/microl) of [3H]thymidine-labeled NGF-HiB5 cells were transplanted stereotactically into three individual sites in the cerebral cortex adjacent to the injury site (14 rats). Separate groups of brain-injured rats received nontransfected (naive [n])-HiB5 cells (12 animals) or cell suspension vehicle (eight animals). One week postinjury, animals underwent neurological evaluation for motor function and cognition (Morris water maze) and were killed for histological, autoradiographic, and immunocytochemical analysis. Viable HiB5 cell grafts were identified in all animals, together with reactive microglia and macrophages located throughout the periinjured parenchyma and grafts (OX-42 immunohistochemistry). Brain-injured animals transplanted with either NGF-HiB5 or n-HiB5 cells displayed significantly improved neuromotor function (p < 0.05) and spatial learning behavior (p < 0.005) compared with brain-injured animals receiving microinjections of vehicle alone. A significant reduction in hippocampal CA3 cell death was observed in brain-injured animals receiving transplants of NGF-HiB5 cells compared with those receiving n-HiB5 cells or vehicle (p < 0.025). CONCLUSIONS: This study demonstrates that immortalized neural stem cells that have been retrovirally transduced to produce NGF can markedly improve cognitive and neuromotor function and rescue hippocampal CA3 neurons when transplanted into the injured brain during the acute posttraumatic period. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1120004

author

Philips, Matthew F. ; Mattiasson, Gustav ^LU ; Wieloch, Tadeusz ^LU ; Björklund, Anders ^LU

; Johansson, Barbro ^LU ; Tomasevic, Gregor ^LU ; Martinez-Serrano, Alberto ; Lenzlinger, Philipp M. ; Sinson, Grant and Grady, M. Sean , et al. (More)

Philips, Matthew F. ; Mattiasson, Gustav ^LU ; Wieloch, Tadeusz ^LU ; Björklund, Anders ^LU

; Johansson, Barbro ^LU ; Tomasevic, Gregor ^LU ; Martinez-Serrano, Alberto ; Lenzlinger, Philipp M. ; Sinson, Grant ; Grady, M. Sean and McIntosh, Tracy K. (Less)

organization

publishing date

2001

type

Contribution to journal

publication status

published

subject

keywords

stem cell, growth factor, traumatic brain injury, transplantation, neuroprotection, gene therapy, rat

in

Journal of Neurosurgery

volume

94

issue

5

pages

765 - 765

publisher

American Association of Neurosurgeons

external identifiers

pmid:11354408
scopus:0034873680

ISSN

0022-3085

language

English

LU publication?

yes

additional info

The information about affiliations in this record was updated in December 2015. The record was previously connected to the following departments: Neurology, Lund (013027000), Laboratory for Experimental Brain Research (013041000), Neurobiology (013212024), Neurosurgery (013026000)

id

21923bb0-4f0a-4f2d-befe-a5bc1d4529ce (old id 1120004)

date added to LUP

2016-04-01 15:41:54

date last changed

2022-03-07 00:57:19

@article{21923bb0-4f0a-4f2d-befe-a5bc1d4529ce,
  abstract     = {{OBJECT: Immortalized neural progenitor cells derived from embryonic rat hippocampus (HiB5), were transduced ex vivo with the gene for mouse nerve growth factor (NGF) to secrete NGF (NGF-HiB5) at 2 ng/hr/10(5) cells in culture. METHODS: Fifty-nine male Wistar rats weighing 300 to 370 g each were anesthetized with 60 mg/kg sodium pentobarbital and subjected to lateral fluid-percussion brain injury of moderate severity (2.3-2.4 atm, 34 rats) or sham injury (25 rats). At 24 hours postinjury, 2 microl (150,000 cells/microl) of [3H]thymidine-labeled NGF-HiB5 cells were transplanted stereotactically into three individual sites in the cerebral cortex adjacent to the injury site (14 rats). Separate groups of brain-injured rats received nontransfected (naive [n])-HiB5 cells (12 animals) or cell suspension vehicle (eight animals). One week postinjury, animals underwent neurological evaluation for motor function and cognition (Morris water maze) and were killed for histological, autoradiographic, and immunocytochemical analysis. Viable HiB5 cell grafts were identified in all animals, together with reactive microglia and macrophages located throughout the periinjured parenchyma and grafts (OX-42 immunohistochemistry). Brain-injured animals transplanted with either NGF-HiB5 or n-HiB5 cells displayed significantly improved neuromotor function (p &lt; 0.05) and spatial learning behavior (p &lt; 0.005) compared with brain-injured animals receiving microinjections of vehicle alone. A significant reduction in hippocampal CA3 cell death was observed in brain-injured animals receiving transplants of NGF-HiB5 cells compared with those receiving n-HiB5 cells or vehicle (p &lt; 0.025). CONCLUSIONS: This study demonstrates that immortalized neural stem cells that have been retrovirally transduced to produce NGF can markedly improve cognitive and neuromotor function and rescue hippocampal CA3 neurons when transplanted into the injured brain during the acute posttraumatic period.}},
  author       = {{Philips, Matthew F. and Mattiasson, Gustav and Wieloch, Tadeusz and Björklund, Anders and Johansson, Barbro and Tomasevic, Gregor and Martinez-Serrano, Alberto and Lenzlinger, Philipp M. and Sinson, Grant and Grady, M. Sean and McIntosh, Tracy K.}},
  issn         = {{0022-3085}},
  keywords     = {{stem cell; growth factor; traumatic brain injury; transplantation; neuroprotection; gene therapy; rat}},
  language     = {{eng}},
  number       = {{5}},
  pages        = {{765--765}},
  publisher    = {{American Association of Neurosurgeons}},
  series       = {{Journal of Neurosurgery}},
  title        = {{Neuroprotective and behavioral efficacy of nerve growth factor-transfected hippocampal progenitor cell transplants after experimental traumatic brain injury}},
  volume       = {{94}},
  year         = {{2001}},
}

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Neuroprotective and behavioral efficacy of nerve growth factor-transfected hippocampal progenitor cell transplants after experimental traumatic brain injury