‘Affinity escape’: Novel SARS-CoV-2 variants may escape immunity by raising the RBD-ACE2 affinity high enough to outcompete the avidity of neutralizing antibodies.
SARS-CoV-2 has proven to be a rapidly evolving RNA virus with steadily emerging new viral variants. Several of them show enhanced infectivity and/or escape from neutralization by monoclonal antibodies (mAbs), and some were termed variants of concern (VoC).
Extended escape from protective antibodies is well described in virology as so-called serotype formation1. Serotypes avoid recognition by previously generated anti-viral antibodies because they differ in neutralizing epitopes due to viral mutation and selection. Typical examples of such serotype-forming viruses are Polio and Dengue viruses, forming 3 and 4 distinct and stable serotypes, respectively1.
For the Beta and Gamma variants of SARS-CoV-2, it has recently been shown that the E484K mutation within the receptor binding domain (RBD) of the spike protein strongly reduces recognition by convalescent sera from individuals after infection with the original Wuhan strain2,3. While this observation suggests development of viral serotypes, it has been difficult to make the reverse observation, i.e., to find or induce sera that neutralize variants with the E484K mutation better than the Wuhan strain3,4,5. Thus, the current data do not fully demonstrate the existence of different SARS-CoV-2 serotypes. Generally, the demonstration of mAbs capable of distinguishing distinct variants is not sufficient to declare new serotypes, as serotypes are defined by polyclonal anti-sera. In contrast, we have recently demonstrated that viral strains can escape neutralizing antibodies despite essentially preserved recognition specificity: by ways of increased receptor affinity. While RBD of the Wuhan strain binds ACE2 with an affinity of 2–10−8 M, RBD with the L452R and E484Q mutations (such as in the Delta and Kappa variants) shows a 4–5 fold higher affinity for the receptor3. This not only causes the well-known increased infectivity but also shifts the virus-receptor equilibrium to the right, i.e., the virus binds more strongly to the ACE2 receptor. Indeed, neutralizing antibodies after infection and vaccination have difficulties in competing with RBD-ACE2 binding, suggesting that neutralization is reduced despite that the epitopes of the mutated RBD maintained essentially the same specificity for these antibodies (Fig. 1). Thus, increasing receptor affinity may constitute a new pathway for viruses to escape neutralizing antibodies and may be called affinity escape6. Differences in assay setups (e.g., plate coating of ACE27 versus coating of RBD on sensor chips3) may lead to different affinities measured in specific cases. Nevertheless, it is well documented that some VoCs exhibit clearly higher affinities for ACE23,7,8,9, supporting the notion that the above-described affinity type escape is a general phenomenon of SARS-CoV-2.
Consequently, vaccine optimization should aim at inducing higher avidity antibodies, rather than altered epitope specificity as would be required for new serotypes10. Indeed, Wuhan strain-based vaccines that induce high avidity antibodies also protect from severe disease caused by prominent VoCs3. Even protection from the Omicron variant is achieved to a relatively high degree after three vaccinations11, likely because this induces high titers of antibodies with increased avidity. The latter is promoted by the well-known mechanism of antibody avidity maturation which is enhanced by booster vaccination and with time12. Interestingly, booster vaccination after a prolonged interval to the first vaccine dose resulted in enhanced antibody responses13. Importantly, a longer vaccination-infection interval was found to be associated with increased neutralization potency to Omicron after breakthrough infection14, an observation consistent with the notion that protection from variants may be favored by progressive affinity maturation during the intervals. Re-infection by VoCs and SARS-CoV-2 in general is favored by the fact that the avidity of antibodies induced by natural infection is relatively low15,16, probably related to the low capability of SARS-CoV-2 to induce neutralizing antibodies17 and the poor formation of germinal centers required for antibody avidity maturation12,18. mAb therapy of infection with viral variants is improved by co-administration of multiple neutralizing mAbs with several different relevant specificities19, reflecting the superiority of polyclonal as opposed to monoclonal antibodies and the presence of multiple neutralizing epitopes on the spike protein and its RBD20. In comparison to mAb therapy that can only be done with a low number of different antibodies, serum antibodies have the advantage of being highly polyclonal and multi-specific.
Evolutionary, novel serotypes are unlikely to emerge from viruses that are inefficient at inducing neutralizing antibodies17. Instead, such viruses may get bigger selective advantage by increasing receptor affinity. These observations imply that the current large efforts to identify correlates of protection21 should include the assessment of antibody avidity22 which is often not done23. It will be interesting to determine whether Coronaviruses are unique in this regard, or whether similar observations may be made for other viruses with well-known receptors, such as Adenoviruses.
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Acknowledgements
We thank our team members for their numerous contributions. The work was supported by the Swiss National Science Foundation (SNF grants 31003A 149925 and 310030-179459) and Inselspital Bern, Switzerland.
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M.F.B., M.O.M. and D.E.S. contributed to the conception of the work, and designed, generated, revised and finalized the manuscript and the figure.
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M.F.B. and M.O.M. own shares and/or receive salaries of Saiba GmbH which is involved in the development of a vaccine against COVID-19. D.E.S. declares no Competing Financial or Non-Financial Interests.
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Bachmann, M.F., Mohsen, M.O. & Speiser, D.E. Increased receptor affinity of SARS-CoV-2: a new immune escape mechanism. npj Vaccines 7, 56 (2022). https://doi.org/10.1038/s41541-022-00479-9
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DOI: https://doi.org/10.1038/s41541-022-00479-9
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