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通过重组技术制备的霍乱弧菌O1缺失突变体的志愿者研究。

Volunteer studies of deletion mutants of Vibrio cholerae O1 prepared by recombinant techniques.

作者信息

Levine M M, Kaper J B, Herrington D, Losonsky G, Morris J G, Clements M L, Black R E, Tall B, Hall R

机构信息

Department of Medicine, University of Maryland, School of Medicine, Baltimore 21201.

出版信息

Infect Immun. 1988 Jan;56(1):161-7. doi: 10.1128/iai.56.1.161-167.1988.

Abstract

Vibrio cholerae O1 A-B- vaccine strain JBK 70 and A-B+ CVD 101 prepared by recombinant DNA techniques from pathogenic EI Tor Inaba N16961 and classical Ogawa 395, respectively, were fed to 38 volunteers in single doses of 10(4) to 10(10). Although severe diarrhea did not occur in any vaccine, more than one-half developed mild diarrhea. These attenuated strains colonized well and elicited prominent vibriocidal and antitoxic (CVD 101) antibody responses. Recipients of a single dose of JBK 70 were significantly protected when challenged with 10(6) wild-type N16961. Diarrhea occurred in 7 of 8 controls but in only 1 of 10 vaccines (P less than 0.003, 89% vaccine efficacy), demonstrating the potency of immune mechanisms that do not involve cholera antitoxin. Further derivatives were prepared to explore the pathogenesis of the residual diarrhea, considering that either intestinal colonization by the vaccine itself or accessory toxins might be responsible. CVD 102, an auxotrophic mutant of CVD 101, did not cause diarrhea but colonized poorly and elicited feeble immune responses. Derivatives of JBK 70 and CVD 101 (CVD 104 and 105) deleted of genes encoding the EI Tor hemolysin still caused mild diarrhea. Genetically engineered strains can be colonizing, highly immunogenic, and protective single-dose oral vaccines, but they must be further attenuated before they can be considered for use as public health tools.

摘要

分别通过重组DNA技术从致病性埃尔托型稻叶株N16961和古典小川型395制备的霍乱弧菌O1 A - B - 疫苗株JBK 70和A - B + CVD 101,以10⁴至10¹⁰的单剂量喂给38名志愿者。虽然任何一种疫苗都未出现严重腹泻,但超过一半的人出现了轻度腹泻。这些减毒株定植良好,并引发了显著的杀弧菌和抗毒素(CVD 101)抗体反应。单剂量JBK 70的接受者在用10⁶野生型N16961攻击时得到了显著保护。8名对照中有7人出现腹泻,而10名疫苗接种者中只有1人出现腹泻(P小于0.003,疫苗效力为89%),证明了不涉及霍乱抗毒素的免疫机制的效力。考虑到疫苗本身的肠道定植或辅助毒素可能是造成残留腹泻的原因,制备了进一步的衍生物以探索残留腹泻的发病机制。CVD 102是CVD 101的营养缺陷型突变体,不引起腹泻,但定植能力差且引发的免疫反应微弱。缺失编码埃尔托溶血素基因的JBK 70和CVD 101的衍生物(CVD 104和105)仍会引起轻度腹泻。基因工程菌株可以是定植性、高免疫原性和保护性的单剂量口服疫苗,但在被考虑用作公共卫生工具之前,它们必须进一步减毒。

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本文引用的文献

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Duration of infection-derived immunity to cholera.霍乱感染后免疫的持续时间。
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Endemic cholera in rural Bangladesh, 1966-1980.1966 - 1980年孟加拉国农村的地方性霍乱
Am J Epidemiol. 1982 Dec;116(6):959-70. doi: 10.1093/oxfordjournals.aje.a113498.
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Infect Immun. 1983 Jun;40(3):1083-91. doi: 10.1128/iai.40.3.1083-1091.1983.

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