Randomized, Placebo-Controlled, Double-Blind Phase 2 Trial Comparing the Reactogenicity and Immunogenicity of a Single Standard Dose to Those of a High Dose of CVD 103-HgR Live Attenuated Oral Cholera Vaccine, with Shanchol Inactivated Oral Vaccine as an Open-Label Immunologic Comparator.

Q2 Biochemistry, Genetics and Molecular Biology
Clinical and Vaccine Immunology Pub Date : 2017-12-05 Print Date: 2017-12-01 DOI:10.1128/CVI.00265-17
Samba O Sow, Milagritos D Tapia, Wilbur H Chen, Fadima C Haidara, Karen L Kotloff, Marcela F Pasetti, William C Blackwelder, Awa Traoré, Boubou Tamboura, Moussa Doumbia, Fatoumata Diallo, Flanon Coulibaly, Uma Onwuchekwa, Mamoudou Kodio, Sharon M Tennant, Mardi Reymann, Diana F Lam, Marc Gurwith, Michael Lock, Thomas Yonker, Jonathan Smith, Jakub K Simon, Myron M Levine
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引用次数: 8

Abstract

Reactive immunization with a single-dose cholera vaccine that could rapidly (within days) protect immunologically naive individuals during virgin soil epidemics, when cholera reaches immunologically naive populations that have not experienced cholera for decades, would facilitate cholera control. One dose of attenuated Vibrio cholerae O1 classical Inaba vaccine CVD 103-HgR (Vaxchora) containing ≥2 × 108 CFU induces vibriocidal antibody seroconversion (a correlate of protection) in >90% of U.S. adults. A previous CVD 103-HgR commercial formulation required ≥2 × 109 CFU to elicit high levels of seroconversion in populations in developing countries. We compared the vibriocidal responses of Malians (individuals 18 to 45 years old) randomized to ingest a single ≥2 × 108-CFU standard dose (n = 50) or a ≥2 × 109-CFU high dose (n = 50) of PaxVax CVD 103-HgR with buffer or two doses (n = 50) of Shanchol inactivated cholera vaccine (the immunologic comparator). To maintain blinding, participants were dosed twice 2 weeks apart; CVD 103-HgR recipients ingested placebo 2 weeks before or after ingesting vaccine. Seroconversion (a ≥4-fold vibriocidal titer rise) between the baseline and 14 days after CVD 103-HgR ingestion and following the first and second doses of Shanchol were the main outcomes measured. By day 14 postvaccination, the rates of seroconversion after ingestion of a single standard dose and a high dose of CVD 103-HgR were 71.7% (33/46 participants) and 83.3% (40/48 participants), respectively. The rate of seroconversion following the first dose of Shanchol, 56.0% (28/50 participants), was significantly lower than that following the high dose of CVD 103-HgR (P = 0.003). The vibriocidal geometric mean titer (GMT) of the high dose of CVD 103-HgR exceeded the GMT of the standard dose at day 14 (214 versus 95, P = 0.045) and was ∼2-fold higher than the GMT on day 7 and day 14 following the first Shanchol dose (P > 0.05). High-dose CVD 103-HgR is recommended for accelerated evaluation in developing countries to assess its efficacy and practicality in field situations. (This study has been registered at ClinicalTrials.gov under registration no. NCT02145377.).

Abstract Image

Abstract Image

随机、安慰剂对照、双盲2期试验,比较单一标准剂量与高剂量CVD 103-HgR口服霍乱减毒活疫苗的反应原性和免疫原性,并以Shanchol口服灭活疫苗作为开放标记免疫比较。
当霍乱传播到几十年来没有经历过霍乱的免疫初级人群时,单剂量霍乱疫苗的反应性免疫接种可以在未开发土壤流行期间迅速(在几天内)保护免疫初级个体,这将有助于控制霍乱。一剂含有≥2 × 108 CFU的减毒霍乱弧菌O1经典稻叶疫苗CVD 103-HgR (Vaxchora)可在>90%的美国成年人中诱导杀弧菌抗体血清转化(与保护相关)。以前的CVD 103-HgR商业化制剂需要≥2 × 109 CFU才能在发展中国家人群中引起高水平的血清转化。我们比较了随机摄入单一≥2 × 108-CFU标准剂量(n = 50)或≥2 × 109-CFU高剂量(n = 50) paxax CVD 103-HgR与缓冲剂或两剂量(n = 50) Shanchol灭活霍乱疫苗(免疫学比较物)的马里人(18至45岁)的杀弧菌反应。为了保持盲法,受试者每隔两周给药两次;CVD 103-HgR受者在接种疫苗前后2周服用安慰剂。在CVD 103-HgR摄入后基线至14天之间以及第一剂和第二剂Shanchol后的血清转化(杀弧菌滴度升高≥4倍)是测量的主要结果。在疫苗接种后第14天,摄入单一标准剂量和高剂量CVD 103-HgR后的血清转化率分别为71.7%(33/46名参与者)和83.3%(40/48名参与者)。首次给药后的血清转换率为56.0%(28/50),显著低于高剂量CVD 103-HgR后的血清转换率(P = 0.003)。高剂量CVD 103-HgR的杀弧菌几何平均滴度(GMT)在第14天超过标准剂量的GMT(214比95,P = 0.045),比第一次Shanchol剂量后第7天和第14天的GMT高约2倍(P > 0.05)。建议在发展中国家加速评价高剂量CVD 103-HgR,以评估其在实地情况下的功效和实用性。(本研究已在ClinicalTrials.gov注册,注册号为:NCT02145377)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Clinical and Vaccine Immunology
Clinical and Vaccine Immunology 医学-传染病学
CiteScore
2.88
自引率
0.00%
发文量
0
审稿时长
1.5 months
期刊介绍: Cessation. First launched as Clinical and Diagnostic Laboratory Immunology (CDLI) in 1994, CVI published articles that enhanced the understanding of the immune response in health and disease and after vaccination by showcasing discoveries in clinical, laboratory, and vaccine immunology. CVI was committed to advancing all aspects of vaccine research and immunization, including discovery of new vaccine antigens and vaccine design, development and evaluation of vaccines in animal models and in humans, characterization of immune responses and mechanisms of vaccine action, controlled challenge studies to assess vaccine efficacy, study of vaccine vectors, adjuvants, and immunomodulators, immune correlates of protection, and clinical trials.
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