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首页> 外文期刊>Infection and immunity >Cloning and Sequence Analysis of a Highly Polymorphic Cryptosporidium parvum Gene Encoding a 60-Kilodalton Glycoprotein and Characterization of Its 15- and 45-Kilodalton Zoite Surface Antigen Products
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Cloning and Sequence Analysis of a Highly Polymorphic Cryptosporidium parvum Gene Encoding a 60-Kilodalton Glycoprotein and Characterization of Its 15- and 45-Kilodalton Zoite Surface Antigen Products

机译:编码60千达旦糖蛋白的高度多态隐孢子虫基因的克隆和序列分析及其15和45千达尔顿渗铝石表面抗原产物的表征

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The apicomplexan parasite Cryptosporidium parvum is a major cause of serious diarrheal disease in both humans and animals. No efficacious chemo- or immunotherapies have been identified for cryptosporidiosis, but certain antibodies directed against zoite surface antigens and/or proteins shed by gliding zoites have been shown to neutralize infectivity in vitro and/or to passively protect against, or ameliorate, disease in vivo. We previously used monoclonal antibody 11A5 to identify a 15-kDa surface glycoprotein that was shed behind motile sporozoites and was recognized by several lectins that neutralized parasite infectivity for cultured epithelial cells. Here we report the cloning and sequence analysis of the gene encoding this 11A5 antigen. Surprisingly, the gene encoded a 330-amino-acid, mucin-like glycoprotein that was predicted to contain an N-terminal signal peptide, a homopolymeric tract of serine residues, 36 sites of O-linked glycosylation, and a hydrophobic C-terminal peptide specifying attachment of a glycosylphosphatidylinositol anchor. The single-copy gene lacked introns and was expressed during merogony to produce a 60-kDa precursor which was proteolytically cleaved to 15- and 45-kDa glycoprotein products that both localized to the surface of sporozoites and merozoites. The gp15/45/60 gene displayed a very high degree of sequence diversity among C. parvumisolates, and the numerous single-nucleotide and single-amino-acid polymorphisms defined five to six allelic classes, each characterized by additional intra-allelic sequence variation. The gp15/45/60 single-nucleotide polymorphisms will prove useful for haplotyping and fingerprinting isolates and for establishing meaningful relationships between C. parvum genotype and phenotype.
机译:apicomplexan寄生虫 Cryptosporidium parvum 是人类和动物严重腹泻病的主要原因。对于隐孢子虫病,尚未发现有效的化学疗法或免疫疗法,但已证明某些针对zoite表面抗原和/或由滑动zoite释放的蛋白质的抗体可在体外中和传染性和/或被动预防或改善体内疾病。我们以前使用单克隆抗体11A5来识别一个15 kDa的表面糖蛋白,该蛋白落在运动的子孢子后面,并被几种凝集素所识别,这些凝集素中和了寄生虫对培养的上皮细胞的感染性。在这里,我们报告编码此11A5抗原的基因的克隆和序列分析。出人意料的是,该基因编码了330个氨基酸的粘蛋白样糖蛋白,预计包含N端信号肽,丝氨酸残基的均聚物,36个O联糖基化位点和一个疏水性C端肽规定了糖基磷脂酰肌醇锚的连接。单拷贝基因缺少内含子,并在模子介导期间表达以产生60kDa的前体,该蛋白被蛋白水解切割成15-kDa和45-kDa的糖蛋白产物,这些产物均定位于子孢子和裂殖子的表面。 gp15 / 45/60基因在 C中显示出很高的序列多样性。小种分离物,以及众多的单核苷酸和单氨基酸多态性定义了五到六个等位基因类别,每个特征是额外的等位基因内部序列变异。 gp15 / 45/60单核苷酸多态性将证明对单体型和指纹图谱分离物以及在C之间建立有意义的关系非常有用。 parvum 基因型和表型。

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