ALCAR completely prevented mechanical hyperalgesia and provoked in the nerve a c-Jun increment only. In the lumbar tract of the spinal cord, higher levels of activated PKCgamma, ERK 1,2, p38, SAP/JNK and c-Jun proteins were detected in the ipsilateral side in respect of sham. ALCAR was able to stimulate this expression profile. At the transcriptional level c-Jun mRNA was increased in the ipsilateral side of spinal cord of CCI saline-treated rats, whereas c-Fos mRNA was unchanged. ALCAR had a stimulatory effect on both these early genes.

Het bleek dus dat ALCAR niet alleen de neuropathische pijn verminderde, maar ook duidelijk neurobiologische veranderingen teweeg bracht in het zenuwweefsel. Bepaalde genen worden door ALCAR meer tot expressie gebracht en dat zou de basis kunnen zijn van neuroregeneratie. 

These findings may represent a different approach in the study of the complex balance between pain and neuroregeneration and could constitute the basis for developing new disease modifying agents in the treatment of neuropathic pain. ^[1]

November 2009: prof.dr. Jan M. Keppel Hesselink 

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