Research on the mechanism of Zuogui Pill and Yougui Pill in promoting axonal regeneration in model rats of autoimmune encephalomyelitis.

Abstract	OBJECTIVE: To study the molecular mechanism of Zuogui Pill (ZGP) and Yougui Pill (YGP) on axonal regeneration in rats with experimental autoimmune encephalomyelitis (EAE). METHODS: EAE rat model was established by bilateral rear pedes subcutaneous injection of antigen made by mixing myelin basic protein (MBP) and complete Freud's adjuvant (CFA) in the volume ratio of 1:1. The pathological changes of axonal injury and regeneration in the brain and the spinal cord were observed on the 14th (the acute stage) and the 28th day (the remission stage) after modeling, with hematoxylin-eosin (HE) staining, silver stain, and immunohistochemical staining. The rats treated with prednisone acetate were taken as controls. RESULTS: Observation under the light microscope with HE staining showed a sleeve-like change in rats' cerebrospinal parenchyma with inflammatory cell infiltration around the small vessels and neuronic denaturation, while silver staining showed excessive tumefaction and abscission of axon, and immunohistochemical analysis showed decreasing of nerve growth factor (NGF) expression at the acute stage of EAE, which was even more remarkable at the remission stage, showing significant difference as compared with the normal control (P<0.05). And the expressions of Nogo A, an axon growth inhibitor, and its receptor (Nogo-66 receptor, Ng R) were significantly higher than those in the normal control at the acute stage (P<0.01). However, after the intervention of ZGP and YGP, the pathological changes and axon damage in rats' brain and spinal cord were much more alleviated, and the NGF expression was significantly higher than that in the model group at the acute stage (P<0.05). The expression of NGF was even stronger during the remission stage, and a better effect was shown by YGP. As for Nogo A and Ng R expressions, they were significantly lower than those in the model group at the acute stage (P<0.05), but a better effect was shown by ZGP. CONCLUSIONS: ZGP and YGP can prevent axonal injury and promote the axonal regeneration in rats of EAE, and the possible mechanism is to increase the expression of NGF and reduce the expression of Nogo A and its receptor. However, some differences are observed between the two Chinese preparations in their acting times and points, which provides a certain basis for revealing the modern connotation of the Chinese medicine theory on tonifying Shen ()-yin and Shen-yang.
Authors	Lei Wang, Hui Zhao, Yong-ping Fan, Hai-yang Gong, Ming Li, Fang Qi, Yan Liu
Journal	Chinese journal of integrative medicine (Chin J Integr Med) Vol. 16 Issue 2 Pg. 167-72 (Apr 2010) ISSN: 1672-0415 [Print] China
PMID	20473744 (Publication Type: Journal Article, Research Support, Non-U.S. Gov't)
Chemical References	Drugs, Chinese Herbal GPI-Linked Proteins Myelin Proteins Nogo Proteins Nogo Receptor 1 Receptors, Cell Surface Receptors, Peptide Rtn4 protein, rat Rtn4r protein, rat Tablets yougui zuogui Nerve Growth Factor
Topics	Animals Axons (drug effects, metabolism, pathology, physiology) Brain (drug effects, metabolism, pathology) Disease Models, Animal Drug Evaluation, Preclinical Drugs, Chinese Herbal (administration & dosage, pharmacology) Encephalomyelitis, Autoimmune, Experimental (drug therapy, metabolism, pathology) GPI-Linked Proteins Male Myelin Proteins (metabolism) Nerve Growth Factor (metabolism) Nerve Regeneration (drug effects) Nogo Proteins Nogo Receptor 1 Rats Rats, Inbred Lew Receptors, Cell Surface Receptors, Peptide (metabolism) Research Signal Transduction (drug effects) Tablets

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