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使用来自黑猩猩的配子体评估候选Pvs25疫苗的传播阻断活性。

Assessment of transmission-blocking activity of candidate Pvs25 vaccine using gametocytes from chimpanzees.

作者信息

Collins William E, Barnwell John W, Sullivan Joann S, Nace Douglas, Williams Tyrone, Bounngaseng Amy, Roberts Jacquelin, Strobert Elizabeth, McClure Harold, Saul Allan, Long Carole A

机构信息

Malaria Branch, Division of Parasitic Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, USA.

出版信息

Am J Trop Med Hyg. 2006 Feb;74(2):215-21.

Abstract

Macaca mulatta monkeys were immunized with the candidate transmission-blocking vaccine against Plasmodium vivax, Pvs25, combined with alum or Montanide ISA 720. Efficacy was measured by combining post-immunization sera with gametocytes obtained from infections induced in chimpanzees using membrane-feeding techniques. The results indicate that immunization of M. mulatta monkeys with Pvs25 and Montanide ISA 720 was more effective than with alum in efficacy and resulted in the maintenance of a lasting transmission-blocking immunity to P. vivax. This was evident two weeks after the second immunization, and more strongly demonstrable 62 and 152 days after the second immunization. This transmission-blocking activity was strongly reinforced by a third immunization given 181 days after the primary immunization, as measured three weeks later by indirect membrane feeding. The use of gametocytes of P. vivax derived from infections induced in chimpanzees can contribute to the selection of appropriate constructs, formulations, and immunization regimens for the development of effective transmission-blocking vaccines.

摘要

将恒河猴用针对间日疟原虫的候选传播阻断疫苗Pvs25与明矾或Montanide ISA 720联合免疫。通过将免疫后的血清与使用膜饲技术在黑猩猩中诱导感染所获得的配子体相结合来测定效力。结果表明,用Pvs25和Montanide ISA 720免疫恒河猴在效力上比用明矾更有效,并导致对间日疟原虫维持持久的传播阻断免疫力。这在第二次免疫后两周就很明显,在第二次免疫后62天和152天更明显。如在初次免疫181天后进行第三次免疫,三周后通过间接膜饲法测定,这种传播阻断活性得到了强烈增强。使用源自黑猩猩感染诱导产生的间日疟原虫配子体有助于为开发有效的传播阻断疫苗选择合适的构建体、制剂和免疫方案。

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