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Erschienen in: Translational Stroke Research 3/2011

01.09.2011 | Original Article

Recombinant T Cell Receptor Ligands Improve Outcome After Experimental Cerebral Ischemia

verfasst von: Kozaburo Akiyoshi, Suzan Dziennis, Julie Palmateer, Xuefang Ren, Arthur A. Vandenbark, Halina Offner, Paco S. Herson, Patricia D. Hurn

Erschienen in: Translational Stroke Research | Ausgabe 3/2011

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Abstract

A key target for novel stroke therapy is the regulation of post-ischemic inflammatory mechanisms. Recent evidence emphasizes the role of T lymphocytes of differing subtypes in the evolution is ischemic brain damage. We have recently demonstrated the benefit of myelin antigen-specific immunodulatory agents known as recombinant T cell receptor ligands (RTLs) in a standard murine model of focal stroke. The aim of the current study was to extend this initial observation to RTL treatment in a therapeutically relevant timing after middle cerebral artery occlusion (MCAO) and verify functional benefit to complement histological outcome measures. We observed that the administration of mouse-specific RTL551 reduced infarct size and improved sensorimotor outcome when administered within a 3 h post-ischemic therapeutic window. RTL551 treatment reduced cortical, caudate putamen, and total infarct volume as compared to vehicle-treated mice. Using a standard behavioral testing repertoire, we observed that RTL551 reduced sensorimotor impairment 3 days after MCAO. Humanized RTL1000 (HLA-DR2 moiety linked to hMOG-35-55 peptide) also reduced infarct size in HLA-DR2 transgenic mice. These data indicate that this neuroantigen-specific immunomodulatory agent reduces damage when administered in a therapeutically relevant reperfusion timeframe.
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Metadaten
Titel
Recombinant T Cell Receptor Ligands Improve Outcome After Experimental Cerebral Ischemia
verfasst von
Kozaburo Akiyoshi
Suzan Dziennis
Julie Palmateer
Xuefang Ren
Arthur A. Vandenbark
Halina Offner
Paco S. Herson
Patricia D. Hurn
Publikationsdatum
01.09.2011
Verlag
Springer-Verlag
Erschienen in
Translational Stroke Research / Ausgabe 3/2011
Print ISSN: 1868-4483
Elektronische ISSN: 1868-601X
DOI
https://doi.org/10.1007/s12975-011-0085-1

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