首页> 美国卫生研究院文献>Clinical and Diagnostic Laboratory Immunology >Humoral immune response against human cytomegalovirus (HCMV)-specific proteins after HCMV infection in lung transplantation as detected with recombinant and naturally occurring proteins.
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Humoral immune response against human cytomegalovirus (HCMV)-specific proteins after HCMV infection in lung transplantation as detected with recombinant and naturally occurring proteins.

机译:用重组蛋白和天然存在的蛋白检测到的肺移植中HCMV感染后针对人巨细胞病毒(HCMV)特异性蛋白的体液免疫应答。

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摘要

The humoral immune response to four intracellularly located cytomegalovirus (CMV) proteins was studied in 15 lung transplant recipients experiencing active CMV infections. Five patients had primary infections, and 10 had secondary infections. Antibodies of the immunoglobulin M (IgM) and IgG classes were measured in an enzyme-linked immunosorbent assay (ELISA) system in which procaryotically expressed recombinant proteins were used as a substrate and also in a monoclonal antibody-based capture ELISA which uses naturally occurring proteins as a substrate. The proteins investigated were the lower matrix protein pp65 (ppUL83), the major DNA-binding protein p52 (ppUL44), and the two immediate early proteins IE1 and IE2 (different splicing products of UL123). Higher levels of antibodies were found to pp65 and especially to p52 than to the immediate early antigens. Antibody levels detected in the recombinant protein-based ELISAs were generally lower than antibody responses detected with the matching antigen capture ELISA. Moreover, some patients appeared to have antibodies mainly to epitopes present on naturally occurring proteins. The antibody responses detected in both assays were related to the viral load during infection as assessed by the CMV antigenemia test, which is a quantitative marker for CMV load. It was found that although epitopes on naturally occurring proteins induce higher antibody responses and responses in more patients, antibodies directed to epitopes present on the recombinant proteins were inversely related to the viral load during a CMV infection. Therefore, antibodies to epitopes on the recombinant proteins might be more clinically relevant in this group of lung transplant recipients.
机译:在经历活动性CMV感染的15位肺移植受者中研究了对四种细胞内定位的巨细胞病毒(CMV)蛋白的体液免疫应答。五名患者患有原发性感染,十名患有继发性感染。在酶联免疫吸附测定(ELISA)系统中测量了免疫球蛋白M(IgM)和IgG类的抗体,在该系统中,原核表达的重组蛋白被用作底物,在基于单克隆抗体的捕获ELISA中也使用天然存在的蛋白作为基材。研究的蛋白质是较低的基质蛋白质pp65(ppUL83),主要的DNA结合蛋白p52(ppUL44)和两个立即早期蛋白质IE1和IE2(UL123的不同剪接产物)。发现针对pp65尤其是p52的抗体水平要高于立即早期抗原。在基于重组蛋白的ELISA中检测到的抗体水平通常低于使用匹配的抗原捕获ELISA检测到的抗体反应。而且,一些患者似乎具有主要针对天然存在的蛋白质上存在的表位的抗体。两种测定法中检测到的抗体反应均与感染期间的病毒载量有关,这是通过CMV抗原血症测试评估的,该测试是CMV载量的定量标记。已经发现,尽管天然存在的蛋白质上的表位诱导更高的抗体应答,并且在更多的患者中产生应答,但是针对重组蛋白上存在的表位的抗体与CMV感染期间的病毒载量成反比。因此,在这组肺移植受者中,针对重组蛋白上表位的抗体可能在临床上更相关。

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