| Literature DB >> 31325330 |
Shira Warszawski1, Elya Dekel1, Ivan Campeotto2, Jennifer M Marshall3, Katherine E Wright4, Oliver Lyth4, Orli Knop1, Neta Regev-Rudzki1, Matthew K Higgins2, Simon J Draper3, Jake Baum4, Sarel J Fleishman1.
Abstract
Many human pathogens use host cell-surface receptors to attach and invade cells. Often, the host-pathogen interaction affinity is low, presenting opportunities to block invasion using a soluble, high-affinity mimic of the host protein. The Plasmodium falciparum reticulocyte-binding protein homolog 5 (RH5) provides an exciting candidate for mimicry: it is highly conserved and its moderate affinity binding to the human receptor basigin (KD ≥1 μM) is an essential step in erythrocyte invasion by this malaria parasite. We used deep mutational scanning of a soluble fragment of human basigin to systematically characterize point mutations that enhance basigin affinity for RH5 and then used Rosetta to design a variant within the sequence space of affinity-enhancing mutations. The resulting seven-mutation design exhibited 1900-fold higher affinity (KD approximately 1 nM) for RH5 with a very slow binding off rate (0.23 h-1 ) and reduced the effective Plasmodium growth-inhibitory concentration by at least 10-fold compared to human basigin. The design provides a favorable starting point for engineering on-rate improvements that are likely to be essential to reach therapeutically effective growth inhibition.Entities:
Keywords: zzm321990Plasmodium falciparum; Rosetta; deep sequencing; high-affinity design; host-pathogen interactions
Year: 2019 PMID: 31325330 PMCID: PMC6904230 DOI: 10.1002/prot.25786
Source DB: PubMed Journal: Proteins ISSN: 0887-3585