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多重调理吞噬作用测定法(MOPA):一种用于监测7价肺炎球菌结合疫苗的有用工具。

Multiplex opsonophagocytosis assay (MOPA): a useful tool for the monitoring of the 7-valent pneumococcal conjugate vaccine.

作者信息

Bogaert D, Sluijter M, De Groot R, Hermans P W M

机构信息

University Medical Center Rotterdam, 3000 DR Rotterdam, The Netherlands.

出版信息

Vaccine. 2004 Sep 28;22(29-30):4014-20. doi: 10.1016/j.vaccine.2004.03.049.

Abstract

Pneumococcal conjugate vaccination is highly efficacious against invasive diseases in young children. Since host protection is mainly mediated by opsonin-dependent phagocytosis, the in vitro measurement of opsonophagocytic activity of the anti-capsular antibodies is assumed to be a reliable correlate of protection to monitor vaccine efficacy. Unfortunately, the methods used so far are all tedious to perform and material-consuming. Therefore, we modified the multi-specificity opsonophagocytosis killing assay (MSOPKA) into a high-throughput method, which simultaneously measures the opsonophagocytosis against the seven serotypes covered by the current conjugate vaccine in a single assay. In the so-called multiplex opsonophagocytosis assay (MOPA), a mixture containing equal numbers of colony forming units (CFUs) of chloramphenicol-resistant serotype 4, spectinomycin-resistant serotype 6B, streptomycin-resistant serotype 9V, erythromycin-resistant serotype 14, rifampicin-resistant serotype 18C, tetracycline-resistant serotype 19F, and trimethoprim-resistant serotype 23F pneumococci was used as a target mixture and incubated with serial dilutions of test serum. After opsonophagocytosis by differentiated HL-60 cells in the presence of complement, the samples were spotted onto different blood agar plates containing the seven selective antibiotics, respectively. Opsonophagocytosis was calculated as the highest serum dilution resulting in 90% or more reduction in CFUs. The data obtained by this assay correlated well with the data obtained by the MSOPKA. In conclusion, the MOPA simultaneously measures opsonophagocytosis capacity of serum against the capsular serotypes included in the 7-valent pneumococcal conjugate vaccine in a high-throughput fashion, requiring low volumes of patient sera.

摘要

肺炎球菌结合疫苗对幼儿侵袭性疾病具有高度有效性。由于宿主保护主要通过调理素依赖性吞噬作用介导,因此抗荚膜抗体的调理吞噬活性的体外测量被认为是监测疫苗效力的可靠保护相关性指标。不幸的是,迄今为止使用的方法操作都很繁琐且消耗材料。因此,我们将多特异性调理吞噬杀伤试验(MSOPKA)改进为一种高通量方法,该方法可在一次试验中同时测量针对当前结合疫苗所涵盖的七种血清型的调理吞噬作用。在所谓的多重调理吞噬试验(MOPA)中,使用含有等量耐氯霉素血清型4、耐壮观霉素血清型6B、耐链霉素血清型9V、耐红霉素血清型14、耐利福平血清型18C、耐四环素血清型19F和耐甲氧苄啶血清型23F肺炎球菌的菌落形成单位(CFU)的混合物作为靶标混合物,并与试验血清的系列稀释液孵育。在补体存在下由分化的HL-60细胞进行调理吞噬后,将样品分别点样到含有七种选择性抗生素的不同血琼脂平板上。调理吞噬作用计算为导致CFU减少90%或更多的最高血清稀释度。该试验获得的数据与MSOPKA获得的数据相关性良好。总之,MOPA以高通量方式同时测量血清对7价肺炎球菌结合疫苗中包含的荚膜血清型的调理吞噬能力,所需患者血清量少。

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