3-Hydroxymorphinan, a Metabolite of Dextromethorphan, Protects Nigrostriatal Pathway Against MPTP-elicited Damage Both in Vivo and in Vitro

Overview

Journal FASEB J

Specialties Biology
Physiology

Date 2006 Dec 5

PMID 17142799

Citations 36

Authors

Wei Zhang

Eun-Joo Shin

Tongguang Wang

Phil Ho Lee

Hao Pang

Myung-Bok Wie

Won-Ki Kim

Seong-Jin Kim

Wen-Hsin Huang

Yongjun Wang

Wanqin Zhang

Jau-Shyong Hong

Hyoung-Chun Kim

Affiliations

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Abstract

We investigated the neuroprotective property of analogs of dextromethorphan (DM) in lipopolysaccharide (LPS) and 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) models to identify neuroprotective drugs for Parkinson's disease (PD). In vivo studies showed that daily injections with DM analogs protected dopamine (DA) neurons in substantia nigra pars compacta and restored DA levels in striatum using two different models for PD. Of the five analogs studied, 3-hydroxymorphinan (3-HM), a metabolite of DM, was the most potent, and restored DA neuronal loss and DA depletion up to 90% of the controls. Behavioral studies showed an excellent correlation between potency for preventing toxin-induced decrease in motor activities and neuroprotective effects among the DM analogs studied, of which 3-HM was the most potent in attenuating behavioral damage. In vitro studies revealed two glia-dependent mechanisms for the neuroprotection by 3-HM. First, astroglia mediated the 3-HM-induced neurotrophic effect by increasing the gene expression of neurotrophic factors, which was associated with the increased acetylation of histone H3. Second, microglia participated in 3-HM-mediated neuroprotection by reducing MPTP-elicited reactive microgliosis as evidenced by the decreased production of reactive oxygen species. In summary, we show the potent neuroprotection by 3-HM in LPS and MPTP PD models investigated. With its high efficacy and low toxicity, 3-HM may be a novel therapy for PD.

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