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合成的低毒性胞壁酰二肽和单磷酰脂质A在诱导针对恶性疟原虫主要裂殖子表面蛋白gp195的生长抑制性抗体方面可替代弗氏完全佐剂。

Synthetic low-toxicity muramyl dipeptide and monophosphoryl lipid A replace Freund complete adjuvant in inducing growth-inhibitory antibodies to the Plasmodium falciparum major merozoite surface protein, gp195.

作者信息

Hui G S, Tam L Q, Chang S P, Case S E, Hashiro C, Siddiqui W A, Shiba T, Kusumoto S, Kotani S

机构信息

Department of Tropical Medicine, School of Medicine, University of Hawaii, Honolulu 96816.

出版信息

Infect Immun. 1991 May;59(5):1585-91. doi: 10.1128/iai.59.5.1585-1591.1991.

Abstract

The Plasmodium falciparum major merozoite surface protein (gp195) is a protective antigen against lethal malaria. However, increasing evidence indicates that the efficacy of a malaria vaccine will require a strong adjuvant that is safe for human use. We compared the efficacies of two low-toxicity synthetic immunomodulators, B30-MDP (a lipophilic muramyl dipeptide derivative) and LA-15-PH (a synthetic equivalent of monophosphoryl lipid A), with that of Freund complete adjuvant (FCA) in eliciting an antibody response to gp195. Rabbits were immunized with native gp195 and B30-MDP, LA-15-PH, or the two in combination, with liposomes as the vehicle. Aluminum hydroxide and FCA were used as reference adjuvants. Results showed that adjuvant formulations based on B30-MDP alone or in combination with LA-15-PH induced high antibody titers to gp195, as compared with FCA. LA-15-PH alone was less effective. Aluminum hydroxide induced significantly lower antibody titers. The functional activity of the rabbit anti-gp195 antibodies induced by different adjuvants was evaluated in an in vitro parasite growth inhibition assay previously shown to correlate with anti-gp195 immunity in the Aotus monkey model. All rabbits immunized with B30-MDP-LA-15-PH and two of three rabbits immunized with B30-MDP alone produced sera that strongly inhibited parasite growth. The degree of growth inhibition was similar to that with FCA. The antibody titers of the rabbits receiving B30-MDP-LA-15-PH strongly correlated with the degree of in vitro growth inhibition. Our findings provided strong evidence that adjuvant formulations based on synthetic B30-MDP and LA-15-PH can replace FCA as adjuvants in stimulating protective immunity specific for gp195.

摘要

恶性疟原虫主要裂殖子表面蛋白(gp195)是一种抗致死性疟疾的保护性抗原。然而,越来越多的证据表明,疟疾疫苗的有效性需要一种对人类使用安全的强效佐剂。我们比较了两种低毒性合成免疫调节剂B30 - MDP(一种亲脂性胞壁酰二肽衍生物)和LA - 15 - PH(单磷酰脂质A的合成类似物)与弗氏完全佐剂(FCA)在引发针对gp195的抗体反应方面的效果。用天然gp195和B30 - MDP、LA - 15 - PH或二者组合对兔子进行免疫,以脂质体作为载体。氢氧化铝和FCA用作参考佐剂。结果表明,与FCA相比,基于单独的B30 - MDP或与LA - 15 - PH组合的佐剂配方诱导出了针对gp195的高抗体滴度。单独使用LA - 15 - PH效果较差。氢氧化铝诱导的抗体滴度明显较低。在先前显示与夜猴模型中抗gp195免疫相关的体外寄生虫生长抑制试验中,评估了不同佐剂诱导的兔抗gp195抗体的功能活性。所有用B30 - MDP - LA - 15 - PH免疫的兔子以及三只单独用B30 - MDP免疫的兔子中的两只产生了强烈抑制寄生虫生长的血清。生长抑制程度与FCA相似。接受B30 - MDP - LA - 15 - PH的兔子的抗体滴度与体外生长抑制程度密切相关。我们的研究结果提供了有力证据,表明基于合成的B30 - MDP和LA - 15 - PH的佐剂配方可以替代FCA作为刺激针对gp195的保护性免疫的佐剂。

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