Vaccine elicitation and structural basis for antibody protection against alphaviruses

Alphaviruses are RNA viruses that represent emerging public health threats. To identify protective antibodies, we immunized macaques with a mixture of western, eastern, and Venezuelan equine encephalitis virus-like particles (VLPs), a regimen that protects against aerosol challenge with all three viruses. Single- and triple-virus-specific antibodies were isolated, and we identified 21 unique binding groups. Cryo-EM structures revealed that broad VLP binding inversely correlated with sequence and conformational variability. One triple-specific antibody, SKT05, bound proximal to the fusion peptide and neutralized all three Env-pseudotyped encephalitic alphaviruses by using different symmetry elements for recognition across VLPs. Neutralization in other assays (e.g., chimeric Sindbis virus) yielded variable results. SKT05 bound backbone atoms of sequence-diverse residues, enabling broad recognition despite sequence variability; accordingly, SKT05 protected mice against Venezuelan equine encephalitis virus, chikungunya virus, and Ross River virus challenges. Thus, a single vaccine-elicited antibody can protect in vivo against a broad range of alphaviruses. [Display omitted] •Trivalent EEV VLP vaccine elicits antibodies with broad alphavirus activity•mAb SKT05 protects against arthritogenic and encephalitic alphavirus infection•Backbone contacts of sequence-diverse residues enable broad SKT05 recognition•Vaccinated macaques can be used to generate clinically relevant reagents Vaccine-elicited antibodies in non-human primates show a wide range of specificities against encephalitic and arthritogenic alphaviruses, extending to very broad recognition and providing insights into both antiviral immunity and vaccination strategies for alphavirus-driven diseases.