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VH3 Gene Usage in Neutralizing Human Antibodies Specific for the Entamoeba histolytica Gal/GalNAc Lectin Heavy Subunit

机译:VH3基因在中和人类对溶组织变形杆菌Gal / GalNAc凝集素重亚基特异性抗体中的用途

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摘要

A combinatorial human immunoglobulin gene library was constructed from peripheral lymphocytes of an asymptomatic Entamoeba histolytica cyst passer and screened for the production of Fab antibody to the parasite. One of the Fab clones, CP33, recognized the 260-kDa galactose- and N-acetyl-d-galactosamine (Gal/GalNAc)-specific lectin of E. histolytica. By shuffling the heavy and light chains of CP33 with the heavy and light chains of two libraries derived from the cyst passer and a liver abscess patient, 18 additional clones were obtained. Sequence analysis of the heavy-chain genes, including CP33-H, revealed that all the nearest V-segment germ lines belonged to the VH3 family (VH3-21, VH3-30, VH3-48, and VH3-53), but the levels of homology were only 85 to 95%. The closest D-segment germ line was D2-2 or D6-6, and for the J-segment the closest germ line was JH4b or JH6b. On the other hand, all the light-chain genes, including CP33-L, belonged to the Vκ1 family, in which the closest Vκ germ line gene was 02/012 or L5, with the Jκ1, Jκ2, Jκ4, or Jκ5 segment. CP33 and three other Fabs obtained by light-chain shuffling were purified and analyzed further. All of these Fabs recognized the cysteine-rich domain of the 170-kDa heavy subunit of the Gal/GalNAc lectin. Preincubation of E. histolytica trophozoites with these Fabs significantly inhibited amebic adherence to Chinese hamster ovary cells and also inhibited erythrophagocytosis. The ability of the neutralizing antibodies to block erythrophagocytosis for the first time implicates the lectin in phagocytosis and VH3 antibodies in defense against parasitic infections. These results demonstrate the utility of a combinatorial human immunoglobulin gene library for identifying and characterizing neutralizing antibodies from humans with amebiasis.
机译:从无症状的解组织变形虫包囊囊传代者的外周淋巴细胞构建了组合的人免疫球蛋白基因文库,并筛选了针对该寄生虫的Fab抗体的产生。 Fab克隆之一CP33识别溶组织性大肠杆菌的260 kDa半乳糖和N-乙酰基-d-半乳糖胺(Gal / GalNAc)特异性凝集素。通过将CP33的重链和轻链与来自囊肿传球者和肝脓肿患者的两个文库的重链和轻链进行改组,获得了18个其他克隆。对包括CP33-H在内的重链基因进行的序列分析显示,所有最近的V段种系都属于VH3家族(VH3-21,VH3-30,VH3-48和VH3-53),但是同源性水平仅为85%至95%。最接近的D段种系是D2-2或D6-6,对于J段,最接近的种系是JH4b或JH6b。另一方面,包括CP33-L在内的所有轻链基因均属于Vκ1家族,其中最接近的Vκ种系基因为02/012或L5,具有Jκ1,Jκ2,Jκ4或Jκ5区段。纯化并进一步分析通过轻链改组获得的CP33和其他三个Fab。所有这些Fab都识别出Gal / GalNAc凝集素的170kDa重亚基的富含半胱氨酸的结构域。用这些Fabs预先培养溶组织大肠杆菌滋养体可显着抑制阿米巴对中国仓鼠卵巢细胞的粘附,也可抑制红细胞吞噬作用。中和抗体首次阻止红细胞吞噬的能力暗示了凝集素参与吞噬作用,而VH3抗体则可以抵抗寄生虫感染。这些结果证明了组合的人免疫球蛋白基因文库用于鉴定和表征来自患有阿米巴病的人的中和抗体的实用性。

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