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利用十种人源单克隆抗体对1型人类免疫缺陷病毒跨膜蛋白gp41的两个免疫显性结构域进行表位作图。

Epitope mapping of two immunodominant domains of gp41, the transmembrane protein of human immunodeficiency virus type 1, using ten human monoclonal antibodies.

作者信息

Xu J Y, Gorny M K, Palker T, Karwowska S, Zolla-Pazner S

机构信息

Department of Pathology, New York University School of Medicine, New York 10016.

出版信息

J Virol. 1991 Sep;65(9):4832-8. doi: 10.1128/JVI.65.9.4832-4838.1991.

Abstract

Immunogenic regions of the gp41 transmembrane protein of human immunodeficiency virus type 1 (HIV-1) were previously mapped by examining polyclonal sera from HIV-infected patients and rodent polyclonal and monoclonal antibodies (MAbs) to peptides of gp41. To define the epitopes within these regions to which infected humans respond during the course of infection, the specificity of human MAbs to these regions had to be studied. Using 10 human MAbs identified initially by their reactivity to whole gp41 in HIV-1 lysates, the epitopes within the immunodominant region of gp41 and within a second immunogenic region of gp41 have been mapped. Thus, five MAbs (from five different patients) to the immunodominant domain of gp41 in the vicinity of the cysteines at positions 598 and 604 (hereinafter designated cluster I) reacted with a stretch of 11 amino acids from positions 590 to 600. Four of these five MAbs were reactive with linear epitopes, while one MAb required the conformation conferred by the disulfide bridge between the aforementioned cysteines. Three MAbs to cluster I revealed dissociation constants ranging from 10(-6) to 10(-8) M, depending on the MAb tested and the size of the synthetic or recombinant peptide used in the assay. Five additional MAbs reacted with a second immunogenic region between positions 644 and 663 (designated cluster II). Four of these five MAbs were specific for conformational determinants. Titration of sera from HIV-infected patients showed that there was about 100-fold more antibody to cluster I than to cluster II in patients' sera, confirming the immunodominance of cluster I.

摘要

1型人类免疫缺陷病毒(HIV-1)的gp41跨膜蛋白的免疫原性区域先前已通过检测HIV感染患者的多克隆血清以及针对gp41肽段的啮齿动物多克隆和单克隆抗体(MAb)进行了定位。为了确定在感染过程中受感染人类对这些区域内表位的反应,必须研究人源MAb对这些区域的特异性。利用最初通过对HIV-1裂解物中全gp41的反应性鉴定出的10种人源MAb,已对gp41免疫显性区域内以及gp41的第二个免疫原性区域内的表位进行了定位。因此,针对gp41在598位和604位半胱氨酸附近免疫显性结构域(以下称为簇I)的5种MAb(来自5名不同患者)与590位至600位的一段11个氨基酸发生反应。这5种MAb中有4种与线性表位反应,而1种MAb需要上述半胱氨酸之间二硫键赋予的构象。针对簇I的3种MAb显示解离常数范围为10^(-6)至10^(-8)M,这取决于所测试的MAb以及测定中使用的合成或重组肽的大小。另外5种MAb与644位和663位之间的第二个免疫原性区域(称为簇II)发生反应。这5种MAb中有4种对构象决定簇具有特异性。对HIV感染患者血清的滴定显示,患者血清中针对簇I的抗体比对簇II的抗体多约100倍,证实了簇I的免疫显性。

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