Division of Infectious Diseases and Immunology, Department of Medicine, University of Massachusetts Medical School, Worcester, Massachusetts, USA.
Viral Immunol. 2012 Oct;25(5):348-59. doi: 10.1089/vim.2012.0010. Epub 2012 Aug 30.
Dengue, caused by the four serotypes of dengue virus (DENV), represents an expanding global health challenge. The potential for serotype-cross-reactive antibodies to exacerbate disease during a secondary infection with a heterologous DENV serotype has driven efforts to study human DENV-specific antibodies. Most DENV-specific antibodies generated in humans are serotype-cross-reactive, weakly neutralizing, and directed against the immature pre-membrane (prM), envelope (E), and nonstructural 1 (NS1) proteins. To broaden the characterization of human DENV-specific antibodies, we assessed B-cell responses by ELISpot assays and isolated B cells from the peripheral blood of a human subject with previous DENV infection. Forty-eight human IgG monoclonal antibodies (hMAbs) were initially characterized by their potential to bind to an inactivated lysate of DENV-infected cells. Subsequently, most DENV-specific hMAbs were found to bind soluble, recombinant E protein (rE). Two hMAbs were unable to bind rE, despite strongly binding to the DENV-infected cell lysate. Further analyses showed that these two hMAbs bound conformation-dependent, reduction-sensitive epitopes on E protein. These data shed light on the breadth of DENV-specific hMAbs generated within a single immune donor.
登革热是由四种登革病毒血清型(DENV)引起的,是一项日益严峻的全球健康挑战。在感染异型 DENV 血清型时,血清型交叉反应性抗体可能会加重疾病,这推动了人们对人类登革病毒特异性抗体的研究。在人类中产生的大多数登革病毒特异性抗体是血清型交叉反应性的、弱中和性的,针对不成熟的前膜(prM)、包膜(E)和非结构蛋白 1(NS1)。为了更广泛地描述人类登革病毒特异性抗体,我们通过 ELISpot 测定评估了 B 细胞反应,并从先前感染过登革病毒的人类受试者的外周血中分离出 B 细胞。最初,我们通过潜在的结合能力来鉴定 48 种人 IgG 单克隆抗体(hMAb)是否能与灭活的登革病毒感染细胞裂解物结合。随后,发现大多数登革病毒特异性 hMAb 能与可溶性重组 E 蛋白(rE)结合。然而,有两种 hMAb 不能结合 rE,尽管它们能与登革病毒感染细胞裂解物强烈结合。进一步的分析表明,这两种 hMAb 结合了 E 蛋白上构象依赖性、还原敏感性的表位。这些数据阐明了在单个免疫供体中产生的登革病毒特异性 hMAb 的广泛范围。
