侵袭性肺炎球菌疾病患儿中肺炎球菌表面毒力蛋白免疫显性B细胞表位的发现
Discovery of Immunodominant B Cell Epitopes within Surface Pneumococcal Virulence Proteins in Pediatric Patients with Invasive Pneumococcal Disease.
作者信息
Lagousi Theano, Routsias John, Piperi Christina, Tsakris Athanassios, Chrousos George, Theodoridou Maria, Spoulou Vana
机构信息
From the First Department of Paediatrics, "Aghia Sophia" Children's Hospital, Immunobiology Research Laboratory and Infectious Diseases Department "MAKKA," and Departments of Microbiology and
Departments of Microbiology and.
出版信息
J Biol Chem. 2015 Nov 13;290(46):27500-10. doi: 10.1074/jbc.M115.666818. Epub 2015 Sep 22.
The identification of immunodominant B cell epitopes within surface pneumococcal virulence proteins in pediatric patients with invasive pneumococcal disease (IPD) is a valuable approach to define novel vaccine candidates. To this aim, we evaluated sera from children with IPD and age-matched controls against 141 20-mer synthetic peptides covering the entire sequence of major antigenic fragments within pneumococcal virulence proteins; namely, choline-binding protein D (CbpD), pneumococcal histidine triad proteins (PhtD and PhtE), pneumococcal surface protein A (PspA), plasminogen and fibronectin binding protein B (PfbB), and zinc metalloproteinase B (ZmpB). Ten immunodominant B cell epitopes were identified: CbpD-pep4 (amino acids (aa) 291-310), PhtD-pep11 (aa 88-107), PhtD-pep17 (aa 172-191), PhtD-pep19 (aa 200-219), PhtE-pep32 (aa 300-319), PhtE-pep40 (aa 79-98), PfbB-pep76 (aa 180-199), PfbB-pep79 (aa 222-241), PfbB-pep90 (aa 484-503), and ZmpB-pep125 (aa 431-450). All epitopes were highly conserved among different pneumococcal serotypes, and four of them were located within the functional zinc-binding domain of the histidine triad proteins PhtD and PhtE. Peptides CbpD-pep4, PhtD-pep19, and PhtE-pep40 were broadly recognized by IPD patient sera with prevalences of 96.4%, 92.9%, and 71.4%, respectively, whereas control sera exhibited only minor reactivities (<10.7%). Their specificities for IPD were 93.3%, 95%, and 96.7%; their sensitivities were 96.4%, 92.9%, and 71.4% and their positivity likelihood ratios for IPD were 14.5, 18.6, and 21.4, respectively. Furthermore, purified antibodies against CbpD-pep4, PhtD-pep19, and PhtE-pep40 readily bound on the surfaces of different pneumococcal serotypes, as assessed by FACS and immunofluorescence analysis. The identified immunodominant B cell epitopes provide a better understanding of immune response in IPD and are worth evaluation in additional studies as potential vaccine candidates.
在侵袭性肺炎球菌疾病(IPD)患儿中鉴定肺炎球菌表面毒力蛋白内的免疫显性B细胞表位是确定新型候选疫苗的一种有价值的方法。为此,我们用覆盖肺炎球菌毒力蛋白内主要抗原片段全序列的141个20肽合成肽评估了IPD患儿和年龄匹配对照的血清;即胆碱结合蛋白D(CbpD)、肺炎球菌组氨酸三联蛋白(PhtD和PhtE)、肺炎球菌表面蛋白A(PspA)、纤溶酶原和纤连蛋白结合蛋白B(PfbB)以及锌金属蛋白酶B(ZmpB)。鉴定出10个免疫显性B细胞表位:CbpD - pep4(氨基酸(aa)291 - 310)、PhtD - pep11(aa 88 - 107)、PhtD - pep17(aa 172 - 191)、PhtD - pep19(aa 200 - 219)、PhtE - pep32(aa 300 - 319)、PhtE - pep40(aa 79 - 98)、PfbB - pep76(aa 180 - 199)、PfbB - pep79(aa 222 - 241)、PfbB - pep90(aa 484 - 503)和ZmpB - pep125(aa 431 - 450)。所有表位在不同肺炎球菌血清型中高度保守,其中四个位于组氨酸三联蛋白PhtD和PhtE的功能性锌结合域内。肽CbpD - pep4、PhtD - pep19和PhtE - pep40被IPD患者血清广泛识别,患病率分别为96.4%、92.9%和71.4%,而对照血清仅表现出轻微反应性(<10.7%)。它们对IPD的特异性分别为93.3%、95%和96.7%;敏感性分别为96.4%、92.9%和71.4%,IPD的阳性似然比分别为14.5、18.6和21.4。此外,可以通过FACS和免疫荧光分析评估,针对CbpD - pep4、PhtD - pep19和PhtE - pep40的纯化抗体能轻易结合在不同肺炎球菌血清型的表面。鉴定出的免疫显性B细胞表位有助于更好地理解IPD中的免疫反应,作为潜在的候选疫苗值得在更多研究中进行评估。
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