Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes
Abstract Background Altered neuronal connectivity in peri-infarct tissue is an important contributor to both the spontaneous recovery of neurological function that commonly develops after stroke and improvements in recovery that have been induced by experimental treatments in animal models. Microgli...
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doaj-2eb285fca8424af68c3dc6cb954671ad2020-11-24T21:18:59ZengBMCJournal of Neuroinflammation1742-20942019-01-0116111910.1186/s12974-018-1379-yEarly treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytesWai Ping Yew0Natalia D. Djukic1Jaya S. P. Jayaseelan2Frederick R. Walker3Karl A. A. Roos4Timothy K. Chataway5Hakan Muyderman6Neil R. Sims7Centre for Neuroscience, College of Medicine and Public Health, Flinders UniversityCentre for Neuroscience, College of Medicine and Public Health, Flinders UniversityCentre for Neuroscience, College of Medicine and Public Health, Flinders UniversityHunter Medical Research Institute; School of Biomedical Medical Sciences and Pharmacy, University of Newcastle Priority Research Centre in Stroke and Traumatic Brain InjuryHunter Medical Research Institute; School of Biomedical Medical Sciences and Pharmacy, University of Newcastle Priority Research Centre in Stroke and Traumatic Brain InjuryCentre for Neuroscience, College of Medicine and Public Health, Flinders UniversityCentre for Neuroscience, College of Medicine and Public Health, Flinders UniversityCentre for Neuroscience, College of Medicine and Public Health, Flinders UniversityAbstract Background Altered neuronal connectivity in peri-infarct tissue is an important contributor to both the spontaneous recovery of neurological function that commonly develops after stroke and improvements in recovery that have been induced by experimental treatments in animal models. Microglia and astrocytes are primary determinants of the environment in peri-infarct tissue and hence strongly influence the potential for neuronal plasticity. However, the specific roles of these cells and the timing of critical changes in their function are not well understood. Minocycline can protect against ischemic damage and promote recovery. These effects are usually attributed, at least partially, to the ability of this drug to suppress microglial activation. This study tested the ability of minocycline treatment early after stroke to modify reactive responses in microglia and astrocytes and improve recovery. Methods Stroke was induced by photothrombosis in the forelimb sensorimotor cortex of Sprague-Dawley rats. Minocycline was administered for 2 days after stroke induction and the effects on forelimb function assessed up to 28 days. The responses of peri-infarct Iba1-positive cells and astrocytes were evaluated using immunohistochemistry and Western blots. Results Initial characterization showed that the numbers of Iba1-positive microglia and macrophages decreased in peri-infarct tissue at 24 h then increased markedly over the next few days. Morphological changes characteristic of activation were readily apparent by 3 h and increased by 24 h. Minocycline treatment improved the rate of recovery of motor function as measured by a forelimb placing test but did not alter infarct volume. At 3 days, there were only minor effects on core features of peri-infarct microglial reactivity including the morphological changes and increased density of Iba1-positive cells. The treatment caused a decrease of 57% in the small subpopulation of cells that expressed CD68, a marker of phagocytosis. At 7 days, the expression of glial fibrillary acidic protein and vimentin was markedly increased by minocycline treatment, indicating enhanced reactive astrogliosis. Conclusions Early post-stroke treatment with minocycline improved recovery but had little effect on key features of microglial activation. Both the decrease in CD68-positive cells and the increased activation of astrogliosis could influence neuronal plasticity and contribute to the improved recovery.http://link.springer.com/article/10.1186/s12974-018-1379-yStrokeFocal ischemiaMicrogliaAstrocytesMinocyclineFunctional recovery |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Wai Ping Yew Natalia D. Djukic Jaya S. P. Jayaseelan Frederick R. Walker Karl A. A. Roos Timothy K. Chataway Hakan Muyderman Neil R. Sims |
spellingShingle |
Wai Ping Yew Natalia D. Djukic Jaya S. P. Jayaseelan Frederick R. Walker Karl A. A. Roos Timothy K. Chataway Hakan Muyderman Neil R. Sims Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes Journal of Neuroinflammation Stroke Focal ischemia Microglia Astrocytes Minocycline Functional recovery |
author_facet |
Wai Ping Yew Natalia D. Djukic Jaya S. P. Jayaseelan Frederick R. Walker Karl A. A. Roos Timothy K. Chataway Hakan Muyderman Neil R. Sims |
author_sort |
Wai Ping Yew |
title |
Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes |
title_short |
Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes |
title_full |
Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes |
title_fullStr |
Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes |
title_full_unstemmed |
Early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes |
title_sort |
early treatment with minocycline following stroke in rats improves functional recovery and differentially modifies responses of peri-infarct microglia and astrocytes |
publisher |
BMC |
series |
Journal of Neuroinflammation |
issn |
1742-2094 |
publishDate |
2019-01-01 |
description |
Abstract Background Altered neuronal connectivity in peri-infarct tissue is an important contributor to both the spontaneous recovery of neurological function that commonly develops after stroke and improvements in recovery that have been induced by experimental treatments in animal models. Microglia and astrocytes are primary determinants of the environment in peri-infarct tissue and hence strongly influence the potential for neuronal plasticity. However, the specific roles of these cells and the timing of critical changes in their function are not well understood. Minocycline can protect against ischemic damage and promote recovery. These effects are usually attributed, at least partially, to the ability of this drug to suppress microglial activation. This study tested the ability of minocycline treatment early after stroke to modify reactive responses in microglia and astrocytes and improve recovery. Methods Stroke was induced by photothrombosis in the forelimb sensorimotor cortex of Sprague-Dawley rats. Minocycline was administered for 2 days after stroke induction and the effects on forelimb function assessed up to 28 days. The responses of peri-infarct Iba1-positive cells and astrocytes were evaluated using immunohistochemistry and Western blots. Results Initial characterization showed that the numbers of Iba1-positive microglia and macrophages decreased in peri-infarct tissue at 24 h then increased markedly over the next few days. Morphological changes characteristic of activation were readily apparent by 3 h and increased by 24 h. Minocycline treatment improved the rate of recovery of motor function as measured by a forelimb placing test but did not alter infarct volume. At 3 days, there were only minor effects on core features of peri-infarct microglial reactivity including the morphological changes and increased density of Iba1-positive cells. The treatment caused a decrease of 57% in the small subpopulation of cells that expressed CD68, a marker of phagocytosis. At 7 days, the expression of glial fibrillary acidic protein and vimentin was markedly increased by minocycline treatment, indicating enhanced reactive astrogliosis. Conclusions Early post-stroke treatment with minocycline improved recovery but had little effect on key features of microglial activation. Both the decrease in CD68-positive cells and the increased activation of astrogliosis could influence neuronal plasticity and contribute to the improved recovery. |
topic |
Stroke Focal ischemia Microglia Astrocytes Minocycline Functional recovery |
url |
http://link.springer.com/article/10.1186/s12974-018-1379-y |
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