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Schistosoma mansoni Phosphoenolpyruvate Carboxykinase a Novel Egg Antigen: Immunological Properties of the Recombinant Protein and Identification of a T-Cell Epitope

机译:曼氏血吸虫磷酸烯醇式丙酮酸羧激酶一种新型卵抗原:重组蛋白的免疫学性质和T细胞表位的鉴定

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摘要

In schistosomiasis mansoni, hepatic granulomatous inflammation surrounding parasite eggs is mediated by CD4+ T helper (Th) cells sensitized to schistosomal egg antigens (SEA). We previously showed that a prominent lymphoproliferative response of CD4+ Th cells from schistosome-infected C57BL/6 (BL/6) mice was directed against a 62-kDa component of SEA. A partial amino acid sequence of the 62-kDa component was found to be identical with one present in the enzyme phosphoenolpyruvate carboxykinase (PEPCK). Based on this sequence, a cDNA clone containing the entire coding region of PEPCK was identified, and the full recombinant Schistosoma mansoni PEPCK (rSm-PEPCK) of 626 amino acids was purified from a prokaryotic expression system. rSm-PEPCK strongly stimulated a specific T-cell hybridoma, 4E6, as well as CD4+ Th cells from SEA-immunized BL/6 mice and from infected BL/6, CBA, and BALB/c mice. In the infected mice, rSm-PEPCK elicited significant gamma interferon production as well as, to a lesser extent, production of interleukin-2 and -5. In BL/6 and BALB/c mice, the CD4+ Th cell response to rSm-PEPCK was greater than that directed against the egg antigen Sm-p40; conversely, CBA mice responded better to Sm-p40 than to Sm-PEPCK. A 12-amino-acid region (residues 398 to 409: DKSKDPKAHPNS) was demonstrated to contain a T-cell epitope; synthetic peptides containing this epitope significantly stimulated specific hybridoma 4E6 and polyclonal CD4+ Th cells. The identification and characterization of immunogenic egg components will contribute to the understanding and possible control of T-cell-mediated schistosomal disease.
机译:在曼氏血吸虫病中,寄生虫卵周围的肝肉芽肿性炎症是由对血吸虫卵抗原(SEA)敏感的CD4 + T辅助细胞(Th)介导的。我们以前表明,血吸虫感染的C57BL / 6(BL / 6)小鼠的CD4 + Th细胞具有显着的淋巴增生反应,是针对SEA的62 kDa成分。发现62-kDa组分的部分氨基酸序列与磷酸烯醇丙酮酸羧化激酶(PEPCK)中存在的氨基酸序列相同。基于该序列,鉴定了包含PEPCK的整个编码区的cDNA克隆,并从原核表达系统中纯化了626个氨基酸的完整重组曼氏血吸虫PEPCK(rSm-PEPCK)。 rSm-PEPCK强烈刺激了SEA免疫BL / 6小鼠以及感染的BL / 6,CBA和BALB / c小鼠的特定T细胞杂交瘤,4E6以及CD4 + Th细胞。在受感染的小鼠中,rSm-PEPCK引起大量的γ干扰素产生,并在较小程度上引起白介素2和-5的产生。在BL / 6和BALB / c小鼠中,对rSm-PEPCK的CD4 + Th细胞应答大于针对卵抗原Sm-p40的应答。相反,CBA小鼠对Sm-p40的反应优于对Sm-PEPCK的反应。证实一个12个氨基酸的区域(398至409残基:DKSKDPKAHPNS)含有一个T细胞表位。含有该表位的合成肽能显着刺激特异性杂交瘤细胞4E6和多克隆CD4 + Th细胞。免疫原性卵成分的鉴定和表征将有助于理解和可能控制T细胞介导的血吸虫病。

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