Matei Elena, Basu Rohan, Furey William, Shi Jiong, Calnan Conor, Aiken Christopher, Gronenborn Angela M
From the Department of Structural Biology, University of Pittsburgh, School of Medicine, Pittsburgh, Pennsylvania 15260.
From the Department of Structural Biology, University of Pittsburgh, School of Medicine, Pittsburgh, Pennsylvania 15260, the Department of Chemistry, Pennsylvania State University, University Park, Pennsylvania 16802.
J Biol Chem. 2016 Sep 2;291(36):18967-76. doi: 10.1074/jbc.M116.740415. Epub 2016 Jul 7.
The HIV-1 envelope glycoprotein gp120 is heavily glycosylated and bears numerous high mannose sugars. These sugars can serve as targets for HIV-inactivating compounds, such as antibodies and lectins, which bind to the glycans and interfere with viral entry into the target cell. We determined the 1.6 Å x-ray structure of Cyt-CVNH, a recently identified lectin from the cyanobacterium Cyanothece(7424), and elucidated its glycan specificity by NMR. The Cyt-CVNH structure and glycan recognition profile are similar to those of other CVNH proteins, with each domain specifically binding to Manα(1-2)Manα units on the D1 and D3 arms of high mannose glycans. However, in contrast to CV-N, no cross-linking and precipitation of the cross-linked species in solution was observed upon Man-9 binding, allowing, for the first time, investigation of the interaction of Man-9 with a member of the CVNH family by NMR. HIV assays showed that Cyt-CVNH is able to inhibit HIV-1 with ∼4-fold higher potency than CV-N(P51G), a stabilized version of wild type CV-N. Therefore, Cyt-CVNH may qualify as a valuable lectin for potential microbicidal use.
HIV-1包膜糖蛋白gp120高度糖基化,带有大量高甘露糖。这些糖可作为HIV灭活化合物的作用靶点,如抗体和凝集素,它们与聚糖结合并干扰病毒进入靶细胞。我们确定了来自蓝细菌蓝藻(7424)的一种最近鉴定出的凝集素Cyt-CVNH的1.6 Å X射线结构,并通过核磁共振阐明了其聚糖特异性。Cyt-CVNH的结构和聚糖识别特征与其他CVNH蛋白相似,每个结构域特异性结合高甘露糖聚糖D1和D3臂上的Manα(1-2)Manα单元。然而,与CV-N不同,在结合Man-9后未观察到溶液中交联物种的交联和沉淀,这首次使得通过核磁共振研究Man-9与CVNH家族成员的相互作用成为可能。HIV检测表明,Cyt-CVNH抑制HIV-1的效力比野生型CV-N的稳定版本CV-N(P51G)高约4倍。因此,Cyt-CVNH可能是一种有价值的凝集素,有潜在的杀微生物用途。
