Potent AMA1-specific human monoclonal antibody against P. vivax Pre-erythrocytic and Blood Stages

Author:

Winnicki Anna C,King Christopher L,Bosch Jurgen,Malachin Alyssa N,Carias Lenore L,Skomorovska-Prokvolit Yelenna,Tham Wai-HongORCID,Dietrich Melanie H,Popovici Jean,Roobsoong Wanlapa,Beeson James G,Sattabongkot Jetsumon,Yeoh Lee M,Opi D. Herbert,Feufack-Donfack Lionel Brice,Orban Agnes,Drago Chiara L,McLaine Olivia S,Redinger Karli R,Jung Nicolai C,Baldor Lea,Kirtley Payton,Neilsen Kiersey,Aleshnick MayaORCID,Zanghi Gigliola,Rezakhani Nastaran,Vaughan Ashley M.,Wilder Brandon KORCID

Abstract

New therapeutics are necessary for preventing Plasmodium vivax malaria due to easy transmissibility and dormancy in the liver that increases the clinical burden due to recurrent relapse. We isolated 12 Pv Apical Membrane Antigen 1 (PvAMA1) specific human monoclonal antibodies from Peripheral Blood Mononuclear Cells of a Pv exposed individual. PvAMA1 is essential for sporozoite and merozoite invasion, making it a unique therapeutic target. HumAb 826827 blocked the invasion of human erythrocytes using Pv clinical isolates and inhibited sporozoite invasion of human hepatocytes in vitro (IC50 of 0.3 to 3.7 ug/mL). It also significantly reduced liver infection of chimeric FRG humHep mice in vivo. The crystal structure of rPvAMA1 bound to 826827 shows that 826827 partially occupies the highly conserved hydrophobic groove in PvAMA1 that binds its known receptor, RON2. We have isolated a potent humAb that is isolate transcendent, blocks both pre erythrocytic and blood stage infection, and could be a new therapy for Pv.

Publisher

Cold Spring Harbor Laboratory

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