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Optimal immunization cocktails can promote induction of broadly neutralizing Abs against highly mutable pathogens.


ABSTRACT: Strategies to elicit Abs that can neutralize diverse strains of a highly mutable pathogen are likely to result in a potent vaccine. Broadly neutralizing Abs (bnAbs) against HIV have been isolated from patients, proving that the human immune system can evolve them. Using computer simulations and theory, we study immunization with diverse mixtures of variant antigens (Ags). Our results show that particular choices for the number of variant Ags and the mutational distances separating them maximize the probability of inducing bnAbs. The variant Ags represent potentially conflicting selection forces that can frustrate the Darwinian evolutionary process of affinity maturation. An intermediate level of frustration maximizes the chance of evolving bnAbs. A simple model makes vivid the origin of this principle of optimal frustration. Our results, combined with past studies, suggest that an appropriately chosen permutation of immunization with an optimally designed mixture (using the principles that we describe) and sequential immunization with variant Ags that are separated by relatively large mutational distances may best promote the evolution of bnAbs.

SUBMITTER: Shaffer JS 

PROVIDER: S-EPMC5111661 | biostudies-literature | 2016 Nov

REPOSITORIES: biostudies-literature

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Optimal immunization cocktails can promote induction of broadly neutralizing Abs against highly mutable pathogens.

Shaffer J Scott JS   Moore Penny L PL   Kardar Mehran M   Chakraborty Arup K AK  

Proceedings of the National Academy of Sciences of the United States of America 20161024 45


Strategies to elicit Abs that can neutralize diverse strains of a highly mutable pathogen are likely to result in a potent vaccine. Broadly neutralizing Abs (bnAbs) against HIV have been isolated from patients, proving that the human immune system can evolve them. Using computer simulations and theory, we study immunization with diverse mixtures of variant antigens (Ags). Our results show that particular choices for the number of variant Ags and the mutational distances separating them maximize  ...[more]

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