PLoS ONE (Jan 2010)

Semaphorin 6A improves functional recovery in conjunction with motor training after cerebral ischemia.

  • Andreas Rogalewski,
  • Tanjew Dittgen,
  • Matthias Klugmann,
  • Friederike Kirsch,
  • Carola Krüger,
  • Claudia Pitzer,
  • Jens Minnerup,
  • Wolf-Rüdiger Schäbitz,
  • Armin Schneider

DOI
https://doi.org/10.1371/journal.pone.0010737
Journal volume & issue
Vol. 5, no. 5
p. e10737

Abstract

Read online

BACKGROUND: We have previously identified Semaphorin 6a (Sema6A) as an upregulated gene product in a gene expression screen in cortical ischemia [1]. Semaphorin 6a was regulated during the recovery phase following ischemia in the cortex. Semaphorin 6a is a member of the superfamily of semaphorins involved in axon guidance and other functions. We hypothesized that the upregulation indicates a crucial role of this molecule in post-stroke rewiring of the brain. Here we have tested this hypothesis by overexpressing semaphorin 6a in the cortex by microinjection of a modified AAV2-virus. A circumscribed cortical infarct was induced, and the recovery of rats monitored for up to 4 weeks using a well-established test battery (accelerated rotarod training paradigm, cylinder test, adhesive tape removal). We observed a significant improvement in post-ischemic recovery of animals injected with the semaphorin 6a virus versus animals treated with a control virus. We conclude that semaphorin 6a overexpressed in the cortex enhances recovery after cerebral ischemia. Semaphorin 6a may represent a novel therapeutic candidate for the treatment of chronic stroke.