Department of Chemistry, Hunter College, 695 Park Avenue, New York, NY 10021, USA.
Bioorg Med Chem. 2011 Aug 15;19(16):4803-11. doi: 10.1016/j.bmc.2011.06.078. Epub 2011 Jul 1.
Inspired by the anti-human immunodeficiency virus (HIV) activity of analogues of β-galactosylceramide (GalCer), a set of mono- and di-saccharide fatty acid esters were designed as GalCer mimetics and their binding to the V3 loop peptide of HIV-1 and anti-HIV activity evaluated. 1,1-linked Gal-Man and Glu-Man disaccharides with an ester on the Man subunit bound the V3 loop peptide and inhibited HIV infectivity in single round infection assays with the TZM-bl cell line. IC(50)'s were in the 50 μM range with no toxicity to the cells at concentrations up to 200 μM. These compounds appear to inhibit virus entry at early steps in viral infection since they were inactive if added post viral entry. Although these compounds were found to bind to the V3 loop peptide of gp120, it is not clear that this interaction is responsible for their anti-HIV activity because the relative binding affinity of closely related analogues did not correlate with their antiviral behavior. The low cytotoxicity of these 1,1-linked disaccharide fatty acid esters, combined with the easy accessibility to structurally diverse analogues make these molecules attractive leads for new topical anti-viral agents.
受β-半乳糖神经酰胺(GalCer)类似物抗人类免疫缺陷病毒(HIV)活性的启发,设计了一系列单糖和二糖脂肪酸酯作为 GalCer 模拟物,并评估了它们与 HIV-1 V3 环肽的结合和抗 HIV 活性。在与 TZM-bl 细胞系的单次感染实验中,具有位于 Man 亚基上的酯的 1,1 连接的 Gal-Man 和 Glu-Man 二糖与 V3 环肽结合,并抑制 HIV 感染性。IC(50)值在 50 μM 范围内,在高达 200 μM 的浓度下对细胞没有毒性。这些化合物似乎在病毒感染的早期步骤中抑制病毒进入,因为如果在病毒进入后添加,它们就没有活性。尽管这些化合物被发现与 gp120 的 V3 环肽结合,但尚不清楚这种相互作用是它们抗 HIV 活性的原因,因为密切相关的类似物的相对结合亲和力与它们的抗病毒行为没有相关性。这些 1,1 连接的二糖脂肪酸酯的低细胞毒性,加上对结构多样的类似物的容易获得性,使这些分子成为新型局部抗病毒药物的有吸引力的先导化合物。