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Mannose-rich glycosylation patterns on HIV-1 subtype C gp120 and sensitivity to the lectins, Griffithsin, Cyanovirin-N and Scytovirin

机译:HIV-1 C亚型gp120上的富含甘露糖的糖基化模式以及对凝集素,格里菲素,氰维林N和Scytovirin的敏感性

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摘要

Griffithsin (GRFT), Cyanovirin-N (CV-N) and Scytovirin (SVN) are lectins that inhibit HIV-1 infection by binding to multiple mannose-rich glycans on the HIV-1 envelope glycoproteins (Env). Here we show that these lectins neutralize subtype C primary virus isolates in addition to Env-pseudotyped viruses obtained from plasma and cervical vaginal lavages. Among 15 subtype C pseudoviruses, the median IC50 values were 0.4, 1.8 and 20.1 nM for GRFT, CV-N and SVN, respectively, similar to what was found for subtype B and A. Analysis of Env sequences suggested that concomitant lack of glycans at positions 234 and 295 resulted in natural resistance to these compounds, which was confirmed by site-directed mutagenesis. Furthermore, the binding sites for these lectins overlapped that of the 2G12 monoclonal antibody epitope, which is generally absent on subtype C Env. This data support further research on these lectins as potential microbicides in the context of HIV-1 subtype C infection.
机译:Griffithsin(GRFT),Cyanovirin-N(CV-N)和Scytovirin(SVN)是通过与HIV-1包膜糖蛋白(Env)上的多个富含甘露糖的聚糖结合而抑制HIV-1感染的凝集素。在这里,我们显示这些凝集素除了可以从血浆和宫颈阴道灌洗液中获得Env假型病毒之外,还可以中和C型亚型病毒。在15种C型亚型伪病毒中,GRFT,CV-N和SVN的中位IC50值分别为0.4、1.8和20.1 nM,与B和A型亚型相似。对Env序列的分析表明,在234和295位产生了对这些化合物的天然抗性,这已通过定点诱变得到证实。此外,这些凝集素的结合位点与2G12单克隆抗体表位的结合位点重叠,后者通常在亚型C Env上不存在。该数据支持对这些凝集素作为HIV-1亚型C感染的潜在杀菌剂的进一步研究。

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