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Immunization with recombinantly expressed glycan antigens from Schistosoma mansoni induces glycan-specific antibodies against the parasite

机译:用曼氏血吸虫重组表达的聚糖抗原免疫诱导针对寄生虫的聚糖特异性抗体

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摘要

Schistosomiasis caused by infection with parasitic helminths of Schistosoma spp. is a major global health problem due to inadequate treatment and lack of a vaccine. The immune response to schistosomes includes glycan antigens, which could be valuable diagnostic markers and vaccine targets. However, no precedent exists for how to design vaccines targeting eukaryotic glycoconjugates. The di- and tri-saccharide motifs LacdiNAc (GalNAcβ1,4GlcNAc; LDN) and fucosylated LacdiNAc (GalNAcβ1,4(Fucα1-3)GlcNAc; LDNF) are the basis for several important schistosome glycan antigens. They occur in monomeric form or as repeating units (poly-LDNF) and as part of a variety of different glycoconjugates. Because chemical synthesis and conjugation of such antigens is exceedingly difficult, we sought to develop a recombinant expression system for parasite glycans. We hypothesized that presentation of parasite glycans on the cell surface would induce glycan-specific antibodies. We generated Chinese hamster ovary (CHO) Lec8 cell lines expressing poly-LDN (L8-GT) and poly-LDNF (L8-GTFT) abundantly on their membrane glycoproteins. Sera from Schistosoma mansoni-infected mice were highly cross-reactive with the cells and with cell-surface N-glycans. Immunizing mice with L8-GT and L8-GTFT cells induced glycan-specific antibodies. The L8-GTFT cells induced a sustained booster response, with antibodies that bound to S. mansoni lysates and recapitulated the exquisite specificity of the anti-parasite response for particular presentations of LDNF antigen. In summary, this recombinant expression system promotes successful generation of antibodies to the glycans of S. mansoni, and it can be adapted to study the role of glycan antigens and anti-glycan immune responses in many other infections and pathologies.
机译:血吸虫病是由血吸虫寄生虫感染引起的。由于治疗不足和缺乏疫苗,是全球主要的健康问题。对血吸虫的免疫应答包括聚糖抗原,其可能是有价值的诊断标记和疫苗靶标。然而,如何设计针对真核糖缀合物的疫苗尚无先例。二糖和三糖基序LacdiNAc(GalNAcβ1,4GlcNAc; LDN)和岩藻糖基化的LacdiNAc(GalNAcβ1,4(Fucα1-3)GlcNAc; LDNF)是几种重要的血吸虫聚糖抗原的基础。它们以单体形式或作为重复单元(poly-LDNF)以及作为各种不同糖缀合物的一部分存在。由于此类抗原的化学合成和缀合极其困难,因此我们寻求开发一种用于寄生虫聚糖的重组表达系统。我们假设细胞表面上的寄生聚糖呈递会诱导聚糖特异性抗体。我们生成了中国仓鼠卵巢(CHO)Lec8细胞系,在其膜糖蛋白上大量表达了poly-LDN(L8-GT)和poly-LDNF(L8-GTFT)。曼氏血吸虫感染小鼠的血清与细胞和细胞表面N-聚糖具有高度的交叉反应性。用L8-GT和L8-GTFT细胞免疫小鼠诱导了聚糖特异性抗体。 L8-GTFT细胞诱导了持续的加强应答,其抗体结合了曼氏曼森酵母裂解物,并针对LDNF抗原的特定呈递概括了抗寄生虫应答的出色特异性。总之,该重组表达系统促进了曼氏沙门氏菌聚糖抗体的成功产生,并且可以适用于研究聚糖抗原和抗聚糖免疫反应在许多其他感染和病理中的作用。

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