Schwann cells, acutely dissociated from a predegenerated nerve trunk, can be applied into a matrix used to bridge nerve defects in rats
Dahlin, Lars LU
; Brandt, Jerker
LU
; Nilsson, A
; Lundborg, Göran
LU
and Kanje, M
(2007)
In Acta Neurochirurgica. Supplementum
100.
p.57-60
- Abstract
- BACKGROUND: The gold standard to reconstruct a nerve defect is a conventional autologous nerve graft. There may be a lack of such grafts in severe nerve injuries. Alternatives to autologous nerve grafts are needed. METHODS: We have developed a technique where mainly Schwann cells are acutely dissociated from the ends of the severed nerve trunk after nerve injury. The technique does not require long-term cell culture procedures. The obtained cells, which can be dissociated within a few hours, are applied to a silicone tube or a tendon autograft used to bridge a nerve defect. FINDINGS: Dissociated cells from the ends of the severed nerve ends consist of more than 85% of Schwann cells. The remaining cells are ED1 stained macrophages. The... (More)
- BACKGROUND: The gold standard to reconstruct a nerve defect is a conventional autologous nerve graft. There may be a lack of such grafts in severe nerve injuries. Alternatives to autologous nerve grafts are needed. METHODS: We have developed a technique where mainly Schwann cells are acutely dissociated from the ends of the severed nerve trunk after nerve injury. The technique does not require long-term cell culture procedures. The obtained cells, which can be dissociated within a few hours, are applied to a silicone tube or a tendon autograft used to bridge a nerve defect. FINDINGS: Dissociated cells from the ends of the severed nerve ends consist of more than 85% of Schwann cells. The remaining cells are ED1 stained macrophages. The cells survive transfer to a silicone tube or a tendon autograft which bridge the nerve defect. Axons do grow through such a graft filled with dissociated cells. CONCLUSION: Our novel model to obtain mainly Schwann cells by dissociation of the cells from the severed nerve ends after injury and add them to a matrix, thereby creating an artificial nerve graft, may be a new technique with potential clinical application in nerve reconstruction. (Less)
Please use this url to cite or link to this publication:
https://lup.lub.lu.se/record/1139690
- author
- Dahlin, Lars
LU
; Brandt, Jerker
LU
; Nilsson, A
; Lundborg, Göran
LU
and Kanje, M
- organization
- publishing date
- 2007
- type
- Contribution to journal
- publication status
- published
- subject
- in
- Acta Neurochirurgica. Supplementum
- volume
- 100
- pages
- 57 - 60
- publisher
- Springer
- external identifiers
-
- pmid:17985546
- scopus:38449107449
- ISSN
- 0065-1419
- language
- English
- LU publication?
- yes
- id
- 218c228d-8986-421c-80df-d5649b3c1fa9 (old id 1139690)
- date added to LUP
- 2016-04-01 16:19:47
- date last changed
- 2022-01-28 18:55:54
@article{218c228d-8986-421c-80df-d5649b3c1fa9,
abstract = {{BACKGROUND: The gold standard to reconstruct a nerve defect is a conventional autologous nerve graft. There may be a lack of such grafts in severe nerve injuries. Alternatives to autologous nerve grafts are needed. METHODS: We have developed a technique where mainly Schwann cells are acutely dissociated from the ends of the severed nerve trunk after nerve injury. The technique does not require long-term cell culture procedures. The obtained cells, which can be dissociated within a few hours, are applied to a silicone tube or a tendon autograft used to bridge a nerve defect. FINDINGS: Dissociated cells from the ends of the severed nerve ends consist of more than 85% of Schwann cells. The remaining cells are ED1 stained macrophages. The cells survive transfer to a silicone tube or a tendon autograft which bridge the nerve defect. Axons do grow through such a graft filled with dissociated cells. CONCLUSION: Our novel model to obtain mainly Schwann cells by dissociation of the cells from the severed nerve ends after injury and add them to a matrix, thereby creating an artificial nerve graft, may be a new technique with potential clinical application in nerve reconstruction.}},
author = {{Dahlin, Lars and Brandt, Jerker and Nilsson, A and Lundborg, Göran and Kanje, M}},
issn = {{0065-1419}},
language = {{eng}},
pages = {{57--60}},
publisher = {{Springer}},
series = {{Acta Neurochirurgica. Supplementum}},
title = {{Schwann cells, acutely dissociated from a predegenerated nerve trunk, can be applied into a matrix used to bridge nerve defects in rats}},
volume = {{100}},
year = {{2007}},
}