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在一项关于CVD 1204和CVD 1208的1期试验中,志贺氏菌肠毒素基因的缺失进一步减弱了携带鸟嘌呤营养缺陷型的福氏志贺氏菌2a。

Deletion in the Shigella enterotoxin genes further attenuates Shigella flexneri 2a bearing guanine auxotrophy in a phase 1 trial of CVD 1204 and CVD 1208.

作者信息

Kotloff Karen L, Pasetti Marcela F, Barry Eileen M, Nataro James P, Wasserman Steven S, Sztein Marcelo B, Picking William D, Levine Myron M

机构信息

Division of Infectious Disease and Tropical Pediatrics, Department of Pediatrics, University of Maryland School of Medicine, Baltimore, Maryland 21201, USA.

出版信息

J Infect Dis. 2004 Nov 15;190(10):1745-54. doi: 10.1086/424680. Epub 2004 Oct 19.

DOI:10.1086/424680
PMID:15499528
Abstract

BACKGROUND

We created a live, attenuated, oral Shigella vaccine by constructing a lineage of guanine auxotrophs and conducted a double-blind, placebo-controlled trial to ascertain (1) the attenuation profile of Delta guaBA Shigella flexneri 2a, which harbors deletions in the guanine nucleotide synthesis pathway (CVD 1204); (2) additional attenuation conferred by deletions in set and sen genes encoding Shigella enterotoxins (ShETs) 1 and 2, respectively (CVD 1208); and (3) the relative immunogenicity of these constructs.

METHODS

Inpatient volunteers received a single oral dose of CVD 1204, CVD 1208 (10(7), 10(8), or 10(9) cfu), or placebo. Clinical, immunologic, and microbiologic responses were evaluated.

RESULTS

Reactogenicity occurred in 8 of 23 recipients of CVD 1204, characterized by diarrhea (30%), fever (22%), and/or dysentery (17%), but in only 1 (5%) of 21 recipients of CVD 1208 (brief fever) (P=.02, Fisher's exact test). Antilipopolysaccharide responses, as measured by antibody-secreting cell, serum, or fecal antibody levels, occurred in 67%, 71%, and 100% of recipients of CVD 1204 and in 86%, 43%, and 100% of recipients of CVD 1208 at doses of 10(7), 10(8), and 10(9) cfu, respectively.

CONCLUSIONS

We conclude that 1 or both ShETs are virulence determinants in humans; their inactivation, in combination with Delta guaBA, leads to a well-tolerated and immunogenic Shigella vaccine candidate.

摘要

背景

我们通过构建鸟嘌呤营养缺陷型谱系创建了一种减毒活口服志贺氏菌疫苗,并进行了一项双盲、安慰剂对照试验,以确定:(1)携带鸟嘌呤核苷酸合成途径缺失的福氏志贺氏菌2a(CVD 1204)的Delta guaBA的减毒特征;(2)分别编码志贺氏菌肠毒素(ShETs)1和2的set和sen基因缺失所带来的额外减毒作用(CVD 1208);以及(3)这些构建体的相对免疫原性。

方法

住院志愿者口服单剂量的CVD 1204、CVD 1208(10⁷、10⁸或10⁹cfu)或安慰剂。对临床、免疫和微生物学反应进行评估。

结果

23名接受CVD 1204的受试者中有8人出现反应原性,表现为腹泻(30%)、发热(22%)和/或痢疾(17%),但21名接受CVD 1208的受试者中只有1人(5%)出现反应原性(短暂发热)(P = 0.02,Fisher精确检验)。通过抗体分泌细胞、血清或粪便抗体水平测量的抗脂多糖反应,在接受CVD 1204的受试者中分别有67%、71%和100%出现,在接受CVD 1208的受试者中,剂量为10⁷、10⁸和10⁹cfu时分别有86%、43%和100%出现。

结论

我们得出结论,1种或2种ShETs都是人类的毒力决定因素;它们的失活与Delta guaBA相结合,产生了一种耐受性良好且具有免疫原性的志贺氏菌候选疫苗。

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