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首页> 外文期刊>Molecular Immunology >Characterization of Escherichia coli K1 colominic acid-specific murine antibodies that are cross-protective against Neisseria meningitidis groups B, C, and Y
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Characterization of Escherichia coli K1 colominic acid-specific murine antibodies that are cross-protective against Neisseria meningitidis groups B, C, and Y

机译:对脑膜炎奈瑟氏球菌B,C和Y交叉保护的大肠杆菌K1 colominic酸特异性鼠抗体的特征

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摘要

The capsular polysaccharide (PS) of Neisseria meningitidis serogroup B (NMGB) is α(2-8)-linked N-acetylneuraminic acid (Neu5Ac), which is almost identical to the O-acetylated colominic acid (CA) of Escherichia coli K1 Although E. coli K1 has long been known to elicit cross-protective antibodies against NMGB, limited information on these highly cross-reactive antibodies is available.In the present study, six new monoclonal antibodies (mAbs) specific to both E. coli K1 CA and NMGB PS were produced by immunizing Balb/c mice with E. coli K1, and their serological and molecular properties were characterized, together with 12 previously reported hybridoma mAbs.Among the bactericidal mAbs against NMGB, both HmenB5 and HmenB18, which are genetically identical though of different mouse origins, were able to kill serogroup C and Y meningococci.Based on SPR sensograms, the binding affinity of HmenB18 for PS was suggested to be associated with at least two different binding forces: the polyanionicity of Neu5Ac and an interaction with the O-acetyl groups of Neu5Ac.Molecular analysis showed that similar to most mAbs presenting a few restricted V region germline genes, the V region genes of HmenB18 were 979% and 986% identical to the closest IGHV1-1401 and IGLV15-10301 germline gene alleles, respectively, and V-D-J editing in this mAb generated an unusually long VH-CDR3 sequence (17 amino acid residues), containing one basic arginine, two hydrophobic isoleucine residues and a 'YAMDY' motif.Models of the mAb combining sites demonstrate that most of the mAbs exhibited a wide, shallow groove with a high overall positive charge, as seen in mAb735, which is specific for a polyanionic helical epitope. In contrast, the combining site of HmenB18 was shown to be wide but to present a relatively weak positive charge, consistent with the extensive recognition by HmenB18 of the various structural epitopes formed with the Neu5Ac residue and its O-acetylation.
机译:脑膜炎奈瑟氏球菌B血清群(NMGB)的荚膜多糖(PS)是与α(2-8)连接的N-乙酰神经氨酸(Neu5Ac),与大肠杆菌K1的O-乙酰化殖民地酸(CA)几乎相同长期以来,已知大肠杆菌K1会引发针对NMGB的交叉保护抗体,但有关这些高度交叉反应的抗体的信息却很少。在本研究中,针对大肠杆菌K1 CA和大肠杆菌K1 CA通过用大肠杆菌K1免疫Balb / c小鼠产生NMGB PS,并对其血清学和分子特性以及之前报道的12种杂交瘤mAb进行了特征分析。根据SPR感应图,HmenB18对PS的结合亲和力至少与两种不同的结合力有关:聚阴离子分子分析表明,与大多数展示少数V区种系限制性基因的mAb相似,HmenB18的V区基因与最接近的IGHV1 979%和986%相同。 1401和IGLV15-10301生殖系基因等位基因分别在该mAb中编辑,产生了异常长的VH-CDR3序列(17个氨基酸残基),其中包含一个碱性精氨酸,两个疏水异亮氨酸残基和一个'YAMDY'基序。 mAb结合位点表明,大多数mAb表现出宽而浅的凹槽,带有高的整体正电荷,如mAb735中所见,mAb735对聚阴离子螺旋表位具有特异性。相比之下,HmenB18的结合位点显示宽,但呈现相对较弱的正电荷,这与HmenB18对由Neu5Ac残基形成的各种结构表位及其O-乙酰化的广泛识别相一致。

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