Depression-like behavior in the forced swimming test in PACAP-deficient mice: amelioration by the atypical antipsychotic risperidone |
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| Authors: | Hitoshi Hashimoto† Ryota Hashimoto†‡§ Norihito Shintani Kazuhiro Tanaka Akiko Yamamoto Michiyoshi Hatanaka Xiaohong Guo Yoshiko Morita Mamoru Tanida¶ Katsuya Nagai¶ Masatoshi Takeda†‡ Akemichi Baba |
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| Institution: | Department of Pathology, Hope Center for Neurological Disorders, Washington University School of Medicine, St Louis, Missouri, USA |
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| Abstract: | Axonal degeneration is a key component of many neurodegenerative diseases. Injured axons undergo a program of self-destruction termed Wallerian degeneration that is an active, well-regulated process. The pathways leading to axon fragmentation are uncharacterized, but experiments with wld s mutant mice led to the discovery that over-expression of NMN adenylyltransferase 1 or treatment with NAD+ can inhibit axonal degeneration. In this study, we show that the purine nucleosides adenosine and guanosine, but not inosine, inhibit injury-induced axonal degeneration in cultured dorsal root ganglia neurons. Axons can be preserved by adding adenosine within 6 h of the axonal injury. The presence of adenosine was required continuously after the injury to maintain axonal protection. Together these results suggest that adenosine does not alter the neuronal response to injury, but instead inhibits a local axonal pathway necessary for the commitment and/or execution of the axon destructive program. |
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| Keywords: | adenosine axonal degeneration guanosine purine nucleosides Wallerian degeneration |
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