鉴定坏死分枝杆菌白细胞毒素蛋白上的线性 B 细胞表位。

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-07-25 DOI:10.1016/j.anaerobe.2024.102884
Jiawei Xiao , Siwen Yu , Kai Jiang , Xianjing He , Lan Bi , Pengyu Zhao , Tianshuo Wang , Ning Yang , Donghua Guo
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引用次数: 0

摘要

目的:坏死杆菌可导致人类患上莱米埃尔综合征,动物患上一系列疾病,包括烂脚病和肝脓肿。坏死杆菌释放的主要毒力因子是白细胞毒素,已被证明与疾病的严重程度密切相关。白细胞毒素通常被用作亚单位疫苗的关键抗原。因此,有必要鉴定 F. necrophorum 白细胞毒素的 B 细胞表位:在这项研究中,我们利用淋巴细胞杂交瘤技术开发出了一种针对F. necrophorum白细胞毒素蛋白的单克隆抗体(mAb)3D7。利用白细胞毒素截短重组蛋白和肽,通过Western印迹、ELISA和点印迹,并通过SWISS-MODEL同源建模和PyMOL可视化,鉴定了3D7 mAb识别的B细胞表位:结果:经鉴定,3D7 mAb 属于具有 κ 链轻链的 IgG1 亚类。它与天然白细胞毒素具有反应性。结果表明,3D7 mAb 能识别 F. necrophorum 白细胞毒素蛋白的 B 细胞表位 I2168SSFGVGV2175(EP-3D7)。序列对比分析表明,EP-3D7 在 F. necrophorum 菌株中高度保守,但在其他细菌中保守程度较低,这表明了 EP-3D7 的特异性。EP-3D7以β折叠的方式存在于白细胞毒素蛋白的表面:总之,这些结果确定了 EP-3D7 是 F. necrophorum 白细胞毒素的保守抗原表位。结论:这些结果确立了 EP-3D7 作为 F. necrophorum 白细胞毒素的保守抗原表位,它对疫苗和 F. necrophorum 表位诊断试剂的开发可能很有价值。
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Identification of linear B cell epitopes on the leukotoxin protein of Fusobacterium necrophorum

Objective

Fusobacterium necrophorum can casuse Lemierre's syndrome in humans and a range of illnesses, including foot rot and liver abscesses, in animals. The main virulence factor released by F. necrophorum is leukotoxin, which has been shown to have a strong correlation with the severity of the disease. Leukotoxin is commonly employed as the key antigen in the formulation of subunit vaccines. Therefore, identification of the B-cell epitope of F. necrophorum leukotoxin is necessary.

Methods

In this research, we utilized lymphocyte hybridoma technology to develop a monoclonal antibody (mAb), 3D7, targeting the F. necrophorum leukotoxin protein. Identification of B-cell epitopes recognized by 3D7 mAb was achieved through Western blot, ELISA and dot blots using leukotoxin-truncated recombinant proteins and peptides, and through SWISS-MODEL homology modeling and PyMOL visualization.

Results

The 3D7 mAb was identified as belonging to the IgG1 subclass with a κ-chain light chain. It demonstrated reactivity with the natural leukotoxin. The results showed that the 3D7 mAb recognizes a B-cell epitope of the F. necrophorum leukotoxin protein, I2168SSFGVGV2175 (EP-3D7). Sequence comparison analysis showed that EP-3D7 was highly conserved in F. necrophorum strains, but less conserved in other bacteria, indicating the specificity of EP-3D7. EP-3D7 is present on the surface of leukotoxin proteins in a β-folded manner.

Conclusions

In summary, these results establish EP-3D7 as a conserved antigenic epitope of F. necrophorum leukotoxin. It could be valuable in the development of vaccines and diagnostic reagents for F. necrophorum epitopes.
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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