首页> 美国卫生研究院文献>Journal of Virology >Note: Comparison of the Antibody Repertoire Generated in Healthy Volunteers following Immunization with a Monomeric Recombinant gp120 Construct Derived from a CCR5/CXCR4-Using Human Immunodeficiency Virus Type 1 Isolate with Sera from Naturally Infected Individuals
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Note: Comparison of the Antibody Repertoire Generated in Healthy Volunteers following Immunization with a Monomeric Recombinant gp120 Construct Derived from a CCR5/CXCR4-Using Human Immunodeficiency Virus Type 1 Isolate with Sera from Naturally Infected Individuals

机译:注意:使用源自人类自然感染者血清的CCR5 / CXCR4单克隆重组gp120构建体(使用人类免疫缺陷病毒1型分离株)免疫后在健康志愿者中产生的抗体库的比较

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摘要

We have characterized sera from healthy volunteers immunized with a monomeric recombinant gp120 (rgp120) derived from a CCR5/CXCR4 (R5X4)-using subtype B isolate of human immunodeficiency virus type (HIV-1), HIV-1W61D, in comparison to sera from long-term HIV-1-infected individuals, using homologous reagents. Sera from vaccinees and HIV-1 positive subjects had similar binding titers to native monomeric rgp120W61D and showed a similar titer of antibodies inhibiting the binding of soluble CD4 (sCD4) to rgp120W61D. However, extensive peptide binding studies showed that the overall pattern of recognition of vaccinee and HIV-1-positive sera is different, with vaccinee sera displaying a wider and more potent recognition of linear V1/V2 and V3 domain epitopes. Neutralization of homologous HIV-1W61D or heterologous HIV-1M2424/4 peripheral blood mononuclear cell (PBMC)-derived virus lines by vaccinee sera could be achieved, but only after adaptation of the viruses to T-cell lines and was quickly lost on readaptation to growth in PBMC. Sera from HIV-positive individuals were able to neutralize both PBMC-grown and T-cell line-adapted viruses. Interestingly, rgp120W61D was recognized by monoclonal antibodies previously shown to neutralize primary HIV-1 isolates. The use of very potent adjuvants and R5X4 rgp120 led to an antibody response equivalent in binding activity and inhibition of binding of sCD4 to gp120 to that of HIV-positive individuals but did not lead to the induction of antibodies capable of neutralizing PBMC-grown virus.
机译:我们已经表征了健康志愿者的血清,与使用来自人类免疫缺陷病毒类型(HIV-1),HIV-1W61D的B亚型分离株的CCR5 / CXCR4(R5X4)衍生的单体重组gp120(rgp120)进行了免疫长期使用HIV-1感染的个体,使用同源试剂。来自疫苗接种者和HIV-1阳性受试者的血清具有与天然单体rgp120W61D相似的结合效价,并显示出相似的效价抑制可溶性CD4(sCD4)与rgp120W61D结合的抗体。但是,广泛的肽结合研究表明,被疫苗接种者和HIV-1阳性血清的整体识别模式是不同的,其中被疫苗接种者血清对线性V1 / V2和V3域表位的识别更加广泛和有效。可以通过疫苗接种血清中和同源HIV-1W61D或异源HIV-1M2424 / 4外周血单核细胞(PBMC)的病毒株,但只有在病毒适应T细胞株后,并在重新适应PBMC的增长。来自HIV阳性个体的血清能够中和PBMC生长的病毒和T细胞适应的病毒。有趣的是,rgp120W61D被先前显示出可中和主要HIV-1分离物的单克隆抗体所识别。非常有效的佐剂和R5X4 rgp120的使用可产生与HIV阳性个体相当的结合活性和sCD4与gp120的结合活性抑制抗体反应,但不会诱导能够中和PBMC生长的病毒的抗体。

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