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Screening of an Echinococcus granulosus cDNA library with IgG4 from patients with cystic echinococcosis identifies a new tegumental protein involved in the immune escape

机译:从囊性棘球co虫病患者中用IgG4筛选细粒棘球oc虫cDNA文库,鉴定出一种新的被皮膜蛋白参与免疫逃逸

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摘要

The worldwide problem of chronic Echinococcus granulosus disease calls for new parasite-derived immunomodulatory molecules. By screening an E. granulosus cDNA library with IgG4 from patients with active cystic echinococcosis, we identified a cDNA that encodes a predicted partial protein that immunofluorescence studies localized in the protoscolex tegument and on the germinal layer of cyst wall. We named this protein EgTeg because the 105 amino acid sequence scored highest against a family of Schistosoma tegumental proteins. Evaluating the role of EgTeg in the human early inflammatory response we found that EgTeg significantly inhibited polymorphonuclear cell (PMN) chemotaxis. Cytometric analysis of intracellular cytokines disclosed a significantly higher percentage of cells producing IL-4 than IFN-γ (P = 0·001, Student's t-test) in T lymphocytes from patients with cystic echinococcosis stimulated with EgTeg. EgTeg induced weak Th1-dependent proliferation in 42% of patients' peripheral blood mononuclear cells. In immunoblotting (IB) analysis of total IgG and IgG subclass responses to EgTeg in patients with cystic echinococcosis, patients with other parasitoses, patients with cystic lesions and healthy controls, total IgG specific to EgTeg yielded high sensitivity (73%) but low specificity (44%) precluding its use in immunodiagnosis. Conversely, IgG4 specific to EgTeg gave acceptable sensitivity (65%) and high specificity (89%) suggesting its use in immunodiagnosis to confirm ultrasound documented cysts suggestive of E. granulosus. Because the new tegumental antigen EgTeg inhibits chemotaxis, induces IL-4-positive T lymphocytes and noncomplement fixing antibodies (IgG4) it is an immunomodulatory molecule associated with chronic infection.
机译:慢性粒棘球oc病的全球性问题要求新的寄生虫来源的免疫调节分子。通过筛选具有活动性囊性棘球co虫病患者的IgG4的大肠杆菌颗粒cDNA文库,我们鉴定了一个cDNA,该cDNA编码一种预测的部分蛋白,免疫荧光研究位于该蛋白的原皮和囊壁生发层。我们将这种蛋白质命名为EgTeg,是因为针对一个血吸虫外皮蛋白质家族的105个氨基酸序列得分最高。评价EgTeg在人类早期炎症反应中的作用,我们发现EgTeg显着抑制了多形核细胞(PMN)趋化性。细胞内细胞因子的细胞计数分析显示,在用EgTeg刺激的囊性包虫病患者的T淋巴细胞中,产生IL-4的细胞百分比显着高于IFN-γ(P = 0·001,Student's t检验)。 EgTeg在42%的患者外周血单核细胞中诱导弱的Th1依赖性增殖。在对囊性包虫病,其他寄生虫病,囊性病变和健康对照的患者中对EgTeg的总IgG和IgG亚类应答的免疫印迹(IB)分析中,对EgTeg特异的总IgG产生高灵敏度(73%)但特异性低( 44%)排除了其在免疫诊断中的用途。相反,对EgTeg特异的IgG4具有可接受的灵敏度(65%)和高特异性(89%),表明其可用于免疫诊断以确认超声记录的提示粒状大肠杆菌的囊肿。由于新的外皮抗原EgTeg抑制趋化性,诱导IL-4阳性T淋巴细胞和非补体固定抗体(IgG4),因此它是一种与慢性感染相关的免疫调节分子。

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