Immunofocusing humoral immunity potentiates the functional efficacy of the AnAPN1 malaria transmission-blocking vaccine antigen

Author:

Bender Nicole G.ORCID,Khare Prachi,Martinez Juan,Tweedell Rebecca E.,Nyasembe Vincent O.,López-Gutiérrez BorjaORCID,Tripathi AbhaiORCID,Miller Dustin,Hamerly TimothyORCID,Vela Eric M.,Davis Ryan R.ORCID,Howard Randall F.,Nsango Sandrine,Cobb Ronald R.,Harbers Matthias,Dinglasan Rhoel R.ORCID

Abstract

AbstractMalaria transmission-blocking vaccines (TBVs) prevent the completion of the developmental lifecycle of malarial parasites within the mosquito vector, effectively blocking subsequent infections. The mosquito midgut protein Anopheline alanyl aminopeptidase N (AnAPN1) is the leading, mosquito-based TBV antigen. Structure-function studies identified two Class II epitopes that can induce potent transmission-blocking (T-B) antibodies, informing the design of the next-generation AnAPN1. Here, we functionally screened new immunogens and down-selected to the UF6b construct that has two glycine-linked copies of the T-B epitopes. We then established a process for manufacturing UF6b and evaluated in outbred female CD1 mice the immunogenicity of the preclinical product with the human-safe adjuvant Glucopyranosyl Lipid Adjuvant in a liposomal formulation with saponin QS21 (GLA-LSQ). UF6b:GLA-LSQ effectively immunofocused the humoral response to one of the key T-B epitopes resulting in potent T-B activity, underscoring UF6b as a prime TBV candidate to aid in malaria elimination and eradication efforts.

Funder

Global Health Innovative Technology Fund (GHIT FUND), Japan

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Infectious Diseases,Pharmacology,Immunology

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