期刊
JOURNAL OF NATURAL MEDICINES
卷 71, 期 4, 页码 579-589出版社
SPRINGER JAPAN KK
DOI: 10.1007/s11418-017-1104-7
关键词
Viral protein R; TREx-HeLa-Vpr cells; K. pulchra; P. javanica; Isopimarane diterpenoids; Picrasane quassinoids
资金
- Ministry of Education, Culture, Sports, Science and Technology, Japan
- Tokyo Biochemical Research Foundation
- Japan Society for the Promotion of Science
- Kobayashi International Scholarship Foundation
- Tokyo Biochemical Research Foundation [TBRF-RF-14-84]
Human immunodeficiency virus type-1 (HIV-1) is a lentiviral family member that encodes the retroviral Gag, Pol, and Env proteins, along with six additional accessory proteins, Tat, Rev, Vpu, Vif, Nef, and Vpr. The currently approved anti-HIV drugs target the Pol and Env encoded proteins. However, these drugs are only effective in reducing viral replication. Furthermore, the drugs' toxicities and the emergence of drug-resistant strains have become serious worldwide problems. Resistance eventually arises to all of the approved anti-HIV drugs, including the newly approved drugs that target HIV integrase (IN). Drug resistance likely emerges because of spontaneous mutations that occur during viral replication. Therefore, new drugs that effectively block other viral components must be developed to reduce the rate of resistance and suppress viral replication with little or no long-term toxicity. The accessory proteins may expand treatment options. Viral protein R (Vpr) is one of the promising drug targets among the HIV accessory proteins. However, the search for inhibitors continues in anti-HIV drug discovery. In this review, we summarize the naturally occurring compounds discovered from two Myanmar medicinal plants as well as their structure-activity relationships. A total of 49 secondary metabolites were isolated from Kaempferia pulchra rhizomes and Picrasama javanica bark, and the types of compounds were identified as isopimarane diterpenoids and picrasane quassinoids, respectively. Among the isolates, 7 diterpenoids and 15 quassinoids were found to be Vpr inhibitors lacking detectable toxicity, and their potencies varied according to their respective functionalities.
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