一种经蛋白酶成熟、二硫键稳定的人类免疫缺陷病毒1型gp140包膜糖蛋白的寡聚体和构象特性
Oligomeric and conformational properties of a proteolytically mature, disulfide-stabilized human immunodeficiency virus type 1 gp140 envelope glycoprotein.
作者信息
Schülke Norbert, Vesanen Mika S, Sanders Rogier W, Zhu Ping, Lu Min, Anselma Deborah J, Villa Anthony R, Parren Paul W H I, Binley James M, Roux Kenneth H, Maddon Paul J, Moore John P, Olson William C
机构信息
Progenics Pharmaceuticals Inc., Tarrytown, New York 10591, USA.
出版信息
J Virol. 2002 Aug;76(15):7760-76. doi: 10.1128/jvi.76.15.7760-7776.2002.
We describe the further properties of a protein, designated SOS gp140, wherein the association of the gp120 and gp41 subunits of the human immunodeficiency virus type 1 (HIV-1) envelope glycoprotein is stabilized by an intersubunit disulfide bond. HIV-1(JR-FL) SOS gp140, proteolytically uncleaved gp140 (gp140(UNC)), and gp120 were expressed in stably transfected Chinese hamster ovary cells and analyzed for antigenic and structural properties before and after purification. Compared with gp140(UNC), SOS gp140 reacted more strongly in surface plasmon resonance and radioimmunoprecipitation assays with the neutralizing monoclonal antibodies (MAbs) 2G12 (anti-gp120), 2F5 (anti-gp41), and 17b (to a CD4-induced epitope that overlaps the CCR5-binding site). In contrast, gp140(UNC) displayed the greater reactivity with nonneutralizing anti-gp120 and anti-gp41 MAbs. Immunoelectron microscopy studies suggested a model for SOS gp140 wherein the gp41 ectodomain (gp41(ECTO)) occludes the "nonneutralizing" face of gp120, consistent with the antigenic properties of this protein. We also report the application of Blue Native polyacrylamide gel electrophoresis (BN-PAGE), a high-resolution molecular sizing method, to the study of viral envelope proteins. BN-PAGE and other biophysical studies demonstrated that SOS gp140 was monomeric, whereas gp140(UNC) comprised a mixture of noncovalently associated and disulfide-linked dimers, trimers, and tetramers. The oligomeric and conformational properties of SOS gp140 and gp140(UNC) were largely unaffected by purification. An uncleaved gp140 protein containing the SOS cysteine mutations (SOS gp140(UNC)) was also oligomeric. Surprisingly, variable-loop-deleted SOS gp140 proteins were expressed (although not yet purified) as cleaved, noncovalently associated oligomers that were significantly more stable than the full-length protein. Overall, our findings have relevance for rational vaccine design.
我们描述了一种名为SOS gp140的蛋白质的更多特性,其中1型人类免疫缺陷病毒(HIV-1)包膜糖蛋白的gp120和gp41亚基通过亚基间二硫键稳定结合。HIV-1(JR-FL)SOS gp140、未被蛋白酶切割的gp140(gp140(UNC))和gp120在稳定转染的中国仓鼠卵巢细胞中表达,并在纯化前后分析其抗原和结构特性。与gp140(UNC)相比,SOS gp140在表面等离子体共振和放射免疫沉淀试验中与中和单克隆抗体(MAb)2G12(抗gp120)、2F5(抗gp41)和17b(针对与CCR5结合位点重叠的CD4诱导表位)反应更强。相反,gp140(UNC)与非中和抗gp120和抗gp41 MAb反应性更强。免疫电子显微镜研究提出了一个SOS gp140的模型,其中gp41胞外域(gp41(ECTO))遮盖了gp120的“非中和”面,这与该蛋白质的抗原特性一致。我们还报告了蓝色原胶聚丙烯酰胺凝胶电泳(BN-PAGE)(一种高分辨率分子大小测定方法)在病毒包膜蛋白研究中的应用。BN-PAGE和其他生物物理研究表明,SOS gp140是单体,而gp140(UNC)由非共价结合和二硫键连接的二聚体、三聚体和四聚体混合物组成。SOS gp140和gp140(UNC)的寡聚和构象特性在很大程度上不受纯化影响。含有SOS半胱氨酸突变的未切割gp140蛋白(SOS gp140(UNC))也是寡聚体。令人惊讶的是,可变环缺失的SOS gp140蛋白以切割后的非共价结合寡聚体形式表达(尽管尚未纯化),其稳定性明显高于全长蛋白。总体而言,我们的发现与合理的疫苗设计相关。
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