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Intracellular Expression of CTB in Vibrio cholerae Strains in Laboratory Culture Conditions

Authors
Choi, HunseokSon, SeonghyeonLee, DonghyunBae, JonghyunSeo, EunyoungKim, Dong WookKim, Eun Jin
Issue Date
Jun-2023
Publisher
한국미생물·생명공학회
Keywords
Cholera; cholera toxin (CT); cholera toxin B subunit (CTB); vaccine; Vibrio cholerae
Citation
Journal of Microbiology and Biotechnology, v.33, no.6, pp.736 - 744
Indexed
SCIE
SCOPUS
KCI
Journal Title
Journal of Microbiology and Biotechnology
Volume
33
Number
6
Start Page
736
End Page
744
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/187394
DOI
10.4014/jmb.2302.02014
ISSN
1017-7825
Abstract
The introduction of the toxT-139F allele triggers the expression of TCP (toxin co-regulated pilus) and CT (cholera toxin) under simple laboratory culture conditions in most Vibrio cholerae strains. Such V. cholerae strains, especially strains that have been used in OCVs (oral cholera vaccines), can induce antibody responses against TCP in animal models. However, CT produced in these V. cholerae strains is secreted into the culture medium. In this study, V. cholerae strains that can express intracellular CTB under the control of the toxT-139F allele have been constructed for potential application in OCVs. First, we constructed a recombinant plasmid directly linking the ctxAB promoter to ctxB without ctxA and confirmed CTB expression from the plasmid in V. cholerae containing the toxT-139F allele. We constructed another recombinant plasmid to express NtrCTB, from which 14 internal amino acids-from the 7th to the 20th amino acid-of the leader peptide of CTB have been omitted, and we found that NtrCTB remained in the cells. Based on those results, we constructed V. cholerae strains in which chromosomal ctxAB is replaced by ntrctxB or ntrctxB-dimer. Both NtrCTB and NtrCTB-dimer remained in the bacterial cells, and 60% of the NtrCTB-dimer in the bacterial cells was maintained in a soluble form. To develop improved OCVs, these strains could be tested to see whether they induce immune responses against CTB in animal models.
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