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Structure-Analgesic Activity Relationship Studies on the C18- and C19-Diterpenoid Alkaloids

Jianli WangDepartment of Chemistry of Medicinal Natural Products, West China of Pharmacy, Sichuan UniversityXiang-Li ShenWest China Second Hospital, Sichuan UniversityQiao‐Hong ChenDepartment of Chemistry of Medicinal Natural Products, West China of Pharmacy, Sichuan UniversityQi GongState Key Laboratory of Drug Research, Shanghai Institute of Materia Medica, Shanghai Institute for Biological SciencesWei WangState Key Laboratory of Drug Research, Shanghai Institute of Materia Medica, Shanghai Institute for Biological SciencesFeng‐Peng WangDepartment of Chemistry of Medicinal Natural Products, West China of Pharmacy, Sichuan University
2009en
ABI

Аннотация

For evaluation of C(18)- and C(19)-diterpenoid alkaloids as analgesics, three C(19)-diterpenoid alkaloids were isolated from the roots of Aconitum hemsleyanum var. circinatum and A. transsecutum; and twenty-five semisynthetic C(18)- or C(19)-diterpenoid alkaloids were prepared from lappaconitine, crassicauline A or yunaconitine. In a mice acetic acid-induced abdominal constriction assay, four crassicauline A analogs and three yunaconitine analogs exhibited good analgesic activities with 77.8-94.1% inhibition range in 0.1-10 mg/kg subcutaneous (s.c.) dose range at the point of 20 min after drug administration. Among them, 8-O-deacetyl-8-O-ethylcrassicauline A (ED(50)=0.0972 mg/kg) and 8-O-ethylyunaconitine (ED(50)=0.0591 mg/kg) were the most potent analgesics relative to the reference drugs lappaconitine (ED(50)=3.50 mg/kg) and crassicauline A (ED(50)=0.0480 mg/kg). Analgesic activity data of these C(18)- and C(19)-diterpenoid alkaloids indicate that a tertiary amine in ring A, an acetoxyl or an ethoxyl group at C-8, an aromatic ester at C-14, and the saturation state of the ring D are important structural features necessary to the analgesic activity of the C(19)-diterpenoid alkaloids.

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