Citicoline mechanisms and clinical efficacy in
cerebral ischemia.

Adibhatla RM, Hatcher JF.

Department of Neurological Surgery, 
Clinical Science Center, 
University of Wisconsin, Madison, WI, 53792. adibhatl@neurosurg.wisc.edu
J Neurosci Res 2002 Oct 15;70(2):133-9

Abstract

Citicoline (CDP-choline), an intermediate in the biosynthesis of phosphatidylcholine (PtdCho), has shown beneficial effects in various CNS injury models and neurodegenerative diseases. PtdCho hydrolysis by phospholipase A(2) (PLA(2)) after cerebral ischemia and reperfusion yields arachidonic acid (ArAc) and lyso-PtdCho. ArAc oxidative metabolism results in formation of reactive oxygen species and lipid peroxides. Lyso-PtdCho could inhibit activity of cytidine triphosphate-phosphocholine cytidylyltransferase (the rate-limiting enzyme in PtdCho biosynthesis), resulting in impaired PtdCho synthesis. Citicoline significantly increased glutathione levels and attenuated release of ArAc and the loss of PtdCho, cardiolipin, and sphingomyelin following transient cerebral ischemia. These effects could be explained by an effect of citicoline on PLA(2). Based on these observations, a mechanism has been hypothesized. This Mini-Review summarizes recent experimental data on the effects of citicoline in cerebral ischemia and evaluates several factors that might have hindered efficacy of citicoline in stroke clinical trials in the United States. Clinical stroke trials of citicoline in Europe and Japan have demonstrated beneficial effects. U.S. trials shown only marginal effects, which might be due to the 24 hr time window, the dose and route of administration, and the stringency of the primary outcome parameters. Recent evaluation of U.S. clinical data suggests that reduction of infarct growth may be a more sensitive measure of the citicoline effect than improvement on the NIH Stroke Scale (NIHSS) by > or =7 points. The citicoline neuroprotective mechanism has not been clearly identified, and its potential in stroke treatment might still be fully recognized in the United States. The clinical efficacy of citicoline (CDP-choline) should be examined further in light of the recent phase III stroke clinical trials and experimental data for cerebral ischemia.

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CDP Choline stroke research                                        www.cdpcholine.info
     CDP choline  in acute ischemic stroke
     CDP choline  randomized trial in acute ischemic stroke
     CDP choline  neural protection in stroke
     CDP choline  in acute ischemic stroke
     CDP choline  efficacy in stroke 
 
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Piracetam stroke research                                             www.piracetam.info
     piracetam  improvement in stroke
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     piracetam  in the treatment of acute stroke
     piracetam  evaluation in acute stroke
     piracetam  in stroke-unduced Aphasia
     piracetam  treatment in ischemic stroke
     piracetam  treatment of patients with an ischemic stroke
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     piracetam  effect on post-stroke recovery
     piracetam  adjuvant to language therapy for aphasia
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     vinpocetine  treatment in acute stroke
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