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用大肠杆菌志贺毒素1(VT1)-B亚基和霍乱毒素无毒突变体进行鼻腔免疫可引发血清中和抗体。

Nasal immunization with E. coli verotoxin 1 (VT1)-B subunit and a nontoxic mutant of cholera toxin elicits serum neutralizing antibodies.

作者信息

Byun Y, Ohmura M, Fujihashi K, Yamamoto S, McGhee J R, Udaka S, Kiyono H, Takeda Y, Kohsaka T, Yuki Y

机构信息

JCR Biopharmaceuticals Incorporated, , San Diego, CA 92121-1194, USA.

出版信息

Vaccine. 2001 Feb 28;19(15-16):2061-70. doi: 10.1016/s0264-410x(00)00411-4.

Abstract

Escherichia coli O157:H7 produces two forms of verotoxin (VT), VT1 and VT2, which cause hemorrhagic colitis with development, in some cases, of hemolytic uremic syndrome. These toxins consist of an enzymatically active A subunit and pentamers of B subunit responsible for their binding to host cells. We used the secretion-expression system of Bacillus brevis to produce recombinant VT1B and VT2B. The secreted B subunits were purified and sequenced to verify their structure. Receptor-binding showed that rVT1B but not rVT2B bound to Gb3-receptor. When mice were nasally immunized with rVT1B or rVT2B together with a nontoxic mutant of cholera toxin (mCT) or native cholera toxin (nCT) as adjuvants, serum IgG and mucosal IgA antibody responses to VT1B were induced. The VT1B-specific antibodies prevented VT1B binding to its Gb3 receptor. In contrast, poor serum and no mucosal VT2B-specific antibodies but brisk CTB-specific antibody responses were induced by nasal immunization with rVT2B in the presence of mCT or nCT. These results show that nasal immunization with rVTB and mCT as a nontoxic mucosal adjuvant is an effective regimen for the induction of VT1B but not VT2B antibody responses which inhibit VT1B binding to Gb3 receptor.

摘要

大肠杆菌O157:H7产生两种形式的志贺毒素(VT),即VT1和VT2,它们可导致出血性结肠炎,在某些情况下还会发展为溶血尿毒综合征。这些毒素由具有酶活性的A亚基和负责与宿主细胞结合的B亚基五聚体组成。我们利用短短芽孢杆菌的分泌表达系统来生产重组VT1B和VT2B。对分泌的B亚基进行纯化和测序以验证其结构。受体结合实验表明,rVT1B能与Gb3受体结合,而rVT2B不能。当用rVT1B或rVT2B与霍乱毒素无毒突变体(mCT)或天然霍乱毒素(nCT)作为佐剂对小鼠进行鼻腔免疫时,可诱导出针对VT1B的血清IgG和黏膜IgA抗体反应。VT1B特异性抗体可阻止VT1B与其Gb3受体结合。相比之下,在mCT或nCT存在的情况下,用rVT2B进行鼻腔免疫诱导出的血清VT2B特异性抗体较少且无黏膜VT2B特异性抗体,但CTB特异性抗体反应活跃。这些结果表明,以rVTB和mCT作为无毒黏膜佐剂进行鼻腔免疫是诱导抑制VT1B与Gb3受体结合的VT1B抗体反应的有效方案,但对VT2B抗体反应无效。

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