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Greatly improved neuroprotective efficiency of citicoline by stereotactic delivery in treatment of ischemic injury

  • Fangjingwei Xu
  • , Hongbin Han*
  • , Junhao Yan
  • , He Chen
  • , Qingyuan He
  • , Weiguo Xu
  • , Ning Zhu
  • , Hong Zhang
  • , Fugen Zhou
  • , Kejia Lee
  • *此作品的通讯作者
  • Peking University
  • SUNY Downstate Health Sciences University
  • Beihang University
  • Max Planck Institute for Radio Astronomy

科研成果: 期刊稿件文章同行评审

摘要

Limited penetration of neuroprotective drug citicoline into the central nervous system (CNS) by systemic administration led to poor efficiency. A novel method of stereotactic drug delivery was explored to make citicoline bypass the blood brain barrier (BBB) and take effect by direct contact with ischemic neurons. A permanent middle cerebral artery occlusion (pMCAO) model of rats was prepared. To get the optimal conditions for citicoline administration by the novel stereotactic delivery pathway, magnetic resonance imaging (MRI) tracer method was used, and a dose-dependent effect was given. Examinations of MRI, behavior evaluation, infarct volume assessment and histological staining were performed to evaluate the outcome. This MRI-guided stereotactic delivery of citicoline resulted in a notable reduction (>80%) in infarct size and a delayed ischemic injury in cortex 12 hours after onset of acute ischemia when compared with the systematic delivery. The improved neuroprotective efficiency was realized by a full distribution of citicoline in most of middle cerebral artery (MCA) territory and an adequate drug reaction in the involved areas of the brain. Brain lesions of treated rats by stereotactic delivery of citicoline were well predicted in the lateral ventricle and thalamus due to a limited drug deposition by MRI tracer method. Our study realized an improved neuroprotective efficiency of citicoline by stereotactic delivery, and an optimal therapeutic effect of this administration pathway can be achieved under MRI guidance.

源语言英语
页(从-至)461-467
页数7
期刊Drug Delivery
18
7
DOI
出版状态已出版 - 9月 2011

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