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Merck
  • Potent inhibition of HIV replication in primary human cells by novel synthetic polyketides inspired by Aureothin.

Potent inhibition of HIV replication in primary human cells by novel synthetic polyketides inspired by Aureothin.

Scientific reports (2020-01-30)
Alexander Herrmann, Manfred Roesner, Thomas Werner, Stefanie M Hauck, Alisha Koch, Amelie Bauer, Martha Schneider, Ruth Brack-Werner
摘要

Overcoming the global health threat of HIV infection requires continuous pipelines of novel drug candidates. We identified the γ-pyrone polyketides Aureothin/Neoaureothin as potent hits by anti-HIV screening of an extensive natural compound collection. Total synthesis of a structurally diverse group of Aureothin-derivatives successfully identified a lead compound (#7) superior to Aureothin that combines strong anti-HIV activity (IC90<45 nM), photostability and improved cell safety. Compound #7 inhibited de novo virus production from integrated proviruses by blocking the accumulation of HIV RNAs that encode the structural components of virions and include viral genomic RNAs. Thus, the mode-of-action displayed by compound #7 is different from those of all current clinical drugs. Proteomic analysis indicated that compound #7 does not affect global protein expression in primary blood cells and may modulate cellular pathways linked to HIV infection. Compound #7 inhibited multiple HIV genotypes, including HIV-type 1 and 2 and synergistically inhibited HIV in combination with clinical reverse transcriptase and integrase inhibitors. We conclude that compound #7 represents a promising new class of HIV inhibitors that will facilitate the identification of new virus-host interactions exploitable for antiviral attack and holds promise for further drug development.

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Sigma-Aldrich
Enfuvirtide acetate salt, ≥95% (HPLC)
Sigma-Aldrich
Fumitremorgin C, from Neosartorya fischeri, film
Sigma-Aldrich
1,3-二邻甲苯胍, 99%