Ultrastructural studies of an immune-mediated inflammatory response in the CNS parenchyma directed against a non-CNS antigen
Ultrastructural studies of an immune-mediated inflammatory response in the CNS parenchyma directed against a non-CNS antigen
We have shown previously that heat-killed bacillus Calmette-Guerin injected into the brain parenchyma becomes sequestered behind the blood-brain barrier for months undetected by the immune system. However, independent peripheral sensitization of the immune system to bacillus Calmette-Guerin results in recognition of bacillus Calmette-Guerin in the brain and the induction of focal chronic lesions [Matyszak M.K. and Perry V.H. (1995) Neuroscience 64, 967-977]. We carried out ultrastructural studies of these lesions. Prior to subcutaneous challenge we used immunohistochemistry to detect bacillus Calmette-Guerin which was found in cells with the morphology of macrophages/microglia and in perivascular macrophages. Eight to 14 days after subcutaneous challenge there was a conspicuous leucocyte infiltration at the site of bacillus Calmette-Guerin deposits within the brain parenchyma. The majority of these cells were macrophages and lymphocytes, with some lymphocytes showing characteristic blast morphology. Dendritic cells in close contact with lymphocytes were prominent. Inflammatory cells were found in perivascular cuffs and within the brain parenchyma. The tissue was oedematous and some axons were undergoing Wallerian degeneration with associated myelin degeneration. Throughout the lesions, but more commonly at the edges, we detected macrophages containing myelin in their cytoplasm close to intact axons and axons with evidence of remyelinating sheaths, suggestive of primary demyelination. In older lesions, two to three months after the peripheral challenge, the oedema was less pronounced and there was little evidence of Wallerian degeneration. There were still many macrophages, lymphocytes and dendritic cells, although the number of these cells was lower than in earlier lesions. Late lesions also contained many plasma cells which were not present in early lesions. In these late lesions there were bundles of axons with no myelin or a few axons with thin myelin sheaths, suggestive of persistent or ongoing demyelination or remyelination. These observations show that, during a delayed-type hypersensitivity lesion in the CNS, the leucocyte populations change with time, and suggest that the mechanisms and type of tissue damage are different in the early and late stages of the lesion.
BCG, demyelination, dendrite cell, DTH, inflammation, macrophage
549-560
Matyszak, M.K.
20d1a24b-f94d-4065-8340-916e42e8bfc8
Townsend, M.J.
3311c8f1-835a-4d38-becb-894430fae4bd
Perry, V.H.
8f29d36a-8e1f-4082-8700-09483bbaeae4
10 March 1997
Matyszak, M.K.
20d1a24b-f94d-4065-8340-916e42e8bfc8
Townsend, M.J.
3311c8f1-835a-4d38-becb-894430fae4bd
Perry, V.H.
8f29d36a-8e1f-4082-8700-09483bbaeae4
Matyszak, M.K., Townsend, M.J. and Perry, V.H.
(1997)
Ultrastructural studies of an immune-mediated inflammatory response in the CNS parenchyma directed against a non-CNS antigen.
Neuroscience, 78 (2), .
(doi:10.1016/S0306-4522(96)00578-7).
Abstract
We have shown previously that heat-killed bacillus Calmette-Guerin injected into the brain parenchyma becomes sequestered behind the blood-brain barrier for months undetected by the immune system. However, independent peripheral sensitization of the immune system to bacillus Calmette-Guerin results in recognition of bacillus Calmette-Guerin in the brain and the induction of focal chronic lesions [Matyszak M.K. and Perry V.H. (1995) Neuroscience 64, 967-977]. We carried out ultrastructural studies of these lesions. Prior to subcutaneous challenge we used immunohistochemistry to detect bacillus Calmette-Guerin which was found in cells with the morphology of macrophages/microglia and in perivascular macrophages. Eight to 14 days after subcutaneous challenge there was a conspicuous leucocyte infiltration at the site of bacillus Calmette-Guerin deposits within the brain parenchyma. The majority of these cells were macrophages and lymphocytes, with some lymphocytes showing characteristic blast morphology. Dendritic cells in close contact with lymphocytes were prominent. Inflammatory cells were found in perivascular cuffs and within the brain parenchyma. The tissue was oedematous and some axons were undergoing Wallerian degeneration with associated myelin degeneration. Throughout the lesions, but more commonly at the edges, we detected macrophages containing myelin in their cytoplasm close to intact axons and axons with evidence of remyelinating sheaths, suggestive of primary demyelination. In older lesions, two to three months after the peripheral challenge, the oedema was less pronounced and there was little evidence of Wallerian degeneration. There were still many macrophages, lymphocytes and dendritic cells, although the number of these cells was lower than in earlier lesions. Late lesions also contained many plasma cells which were not present in early lesions. In these late lesions there were bundles of axons with no myelin or a few axons with thin myelin sheaths, suggestive of persistent or ongoing demyelination or remyelination. These observations show that, during a delayed-type hypersensitivity lesion in the CNS, the leucocyte populations change with time, and suggest that the mechanisms and type of tissue damage are different in the early and late stages of the lesion.
This record has no associated files available for download.
More information
Accepted/In Press date: 14 October 1996
Published date: 10 March 1997
Keywords:
BCG, demyelination, dendrite cell, DTH, inflammation, macrophage
Identifiers
Local EPrints ID: 489605
URI: http://eprints.soton.ac.uk/id/eprint/489605
ISSN: 0306-4522
PURE UUID: 285f68d6-6aeb-4f48-b137-508c11b2a74b
Catalogue record
Date deposited: 29 Apr 2024 16:46
Last modified: 05 Jun 2024 19:14
Export record
Altmetrics
Contributors
Author:
M.K. Matyszak
Author:
M.J. Townsend
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics