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首页> 外文期刊>Infection and immunity >Primary structure of the variable region of monoclonal antibody 2B10, capable of inducing anti-idiotypic antibodies that recognize the C-terminal region of MSA-1 of Plasmodium falciparum.
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Primary structure of the variable region of monoclonal antibody 2B10, capable of inducing anti-idiotypic antibodies that recognize the C-terminal region of MSA-1 of Plasmodium falciparum.

机译:单克隆抗体2B10可变区的一级结构,能够诱导识别恶性疟原虫MSA-1 C端区域的抗独特型抗体。

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摘要

Previously, we reported on the properties of a monoclonal antibody, 2B10, which has the same determinant on the human erythrocyte as MSA-1 of Plasmodium falciparum (FCR3 strain); the binding of both ligands to erythrocyte receptors was totally sialic acid dependent. In this work, rabbit anti-2B10 idiopathic antibodies were generated. The anti-idiotypic antibodies recognized both the erythrocyte binding site of 2B10 and the C-terminal region of MSA-1 (amino acids 1047 to 1640); they were able to inhibit 2B10 and MSA-1 binding to erythrocytes and partially prevent P. falciparum merozoites from invading erythrocytes. The utility of 2B10 in the study of the interaction between MSA-1 and human erythrocytes prompted us to determine the nucleotide and deduced amino acid sequences of its VH and VL regions. The data show that the 2B10 VH region is part of the J558 family and is especially homologous to BALB/c anti-nitrophenyl monoclonal antibody 21.1.43; the VL region belongs to the VK1 subgroup and comes from the same genomic locus as (NZB x W)F1 anti-DNA and C57BL anti-dextran monoclonal antibodies BXW-14 and 42.48.12.2, respectively. Most of the differences among the VH and VL segments are located in CDR1 and -3. The binding site of 2B10 contains both negatively and positively charged amino acid residues. The amino acid sequences of the 2B10 VH region and a region of MSA-1 from the Wellcome strain of P. falciparum (amino acids 1002 to 1115) share 43% similarity, and the amino acid sequences between the 2B10 VL region and another segment of the same MSA-1 (amino acids 1247 to 1394) share 48% similarity. We conclude that the interactions between erythrocyte receptors and their ligands, 2B10 and MSA-1, are related and that the C-terminal region of MSA-1 is the erythrocyte binding domain.
机译:先前,我们报道了单克隆抗体2B10的特性,该抗体在人红细胞上具有与恶性疟原虫(FCR3株)的MSA-1相同的决定因素;两种配体与红细胞受体的结合完全依赖唾液酸。在这项工作中,产生了兔抗2B10特发性抗体。抗独特型抗体既识别2B10的红细胞结合位点,又识别MSA-1的C端区域(氨基酸1047至1640)。它们能够抑制2B10和MSA-1与红细胞的结合,并部分阻止恶性疟原虫裂殖子入侵红细胞。 2B10在研究MSA-1与人类红细胞之间的相互作用中的实用性促使我们确定其VH和VL区的核苷酸和推导的氨基酸序列。数据显示2B10 VH区是J558家族的一部分,并且与BALB / c抗硝基苯基单克隆抗体21.1.43特别同源; VL区属于VK1亚组,分别与(NZB x W)F1抗DNA和C57BL抗右旋糖酐单克隆抗体BXW-14和42.48.12.2来自相同的基因组位点。 VH和VL段之间的大多数差异位于CDR1和-3中。 2B10的结合位点包含带负电荷和带正电荷的氨基酸残基。恶性疟原虫的Wellcome菌株的2B10 VH区和MSA-1区的氨基酸序列(氨基酸1002至1115)具有43%的相似性,并且2B10 VL区与该区的另一个片段之间的氨基酸序列相同的MSA-1(氨基酸1247至1394)具有48%的相似性。我们得出结论,红细胞受体与其配体2B10和MSA-1之间的相互作用是相关的,并且MSA-1的C端区域是红细胞结合域。

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