百日咳毒素亚基的制备与表征。

G C Sheu, Y Y Wo, C H Lu
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引用次数: 0

摘要

百日咳毒素(Pertussis toxin, PT)是一种典型的百日咳a - b寡聚体外毒素,已被证明是百日咳无细胞百日咳疫苗必不可少的保护性抗原。为了研究其组分的相关功能,我们纯化了A和B低聚物进行活性研究。以插入S1编码区的表达载体pET-20b为载体,在大肠杆菌B834 (DE3)中表达了PT的A低聚物(S1亚基),并通过金属螯合柱进行了纯化。B低聚物采用单步纯化方法分离得到。单独来看,重组S1和B寡聚物在体内表现出截然不同的生物活性。S1亚基诱导白细胞促进(LP)活性,但不影响小鼠体重增加。相反,B低聚物降低小鼠体重增加,但不显示LP活性。体外实验表明,S1亚基与B寡聚物联合可增强天然PT的毒性,并在CHO细胞聚集试验和血凝试验中表现出加性毒性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Preparation and characterization of Pertussis toxin subunits.

Pertussis toxin (PT), a typical A-B oligomer exotoxin of Bordetella pertussis, has been demonstrated to be an essential protective antigen for acellular pertussis vaccine against whooping cough. In order to investigate the associated functionality ascribed to its components, we have purified A and B oligomers for the activity study. The A oligomer (S1 subunit) of PT was expressed in E. coli B834 (DE3) harboring expression vector (pET-20b) with the insert of S1 coding region and purified by metal-chelating column. The B oligomer was isolated by a single-step purification procedure. Individually, recombinant S1 and B oligomer exhibited quite distinct biological activities in vivo. S1 subunit induced leukocytosis-promoting (LP) activity, but did not affect mouse body weight-gain. On the contrary, B oligomer reduced mouse body weight-gain but did not reveal LP activity. In vitro, the combination of S1 subunit and B oligomer could enhance the toxic activities as exhibited by native PT and showed an additive toxicity in CHO cell clustering test and hemagglutination assay.

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