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Plasmodium falciparum-specific IgM B cells dominate in children, expand with malaria, and produce functional IgM

J Exp Med. 2021-04; 
Christine S Hopp, Padmapriya Sekar, Ababacar Diouf, Kazutoyo Miura, Kristin Boswell, Jeff Skinner, Christopher M Tipton, Mary E Peterson, Michael J Chambers, Sarah Andrews, Jinghua Lu, Joshua Tan, Shanping Li, Safiatou Doumbo, Kassoum Kayentao, Aissata Ongoiba, Boubacar Traore, Silvia Portugal, Peter D Sun, Carole Long, Richard A Koup, Eric O Long, Adrian B McDermott, Peter D Crompton
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DNA Sequencing PCR products were Sanger sequenced by GenScript, and sequences were analyzed using IMGT/V-QUEST (Giudicelli et al., 2011). Ig heavy and light chain sequences were synthesized and cloned by GenScript into IgG1, κ, or λ expression vectors Get A Quote

摘要

IgG antibodies play a role in malaria immunity, but whether and how IgM protects from malaria and the biology of Plasmodium falciparum (Pf)-specific IgM B cells is unclear. In a Mali cohort spanning infants to adults, we conducted longitudinal analyses of Pf- and influenza-specific B cells. We found that Pf-specific memory B cells (MBCs) are disproportionally IgM+ and only gradually shift to IgG+ with age, in contrast to influenza-specific MBCs that are predominantly IgG+ from infancy to adulthood. B cell receptor analysis showed Pf-specific IgM MBCs are somatically hypermutated at levels comparable to influenza-specific IgG B cells. During acute malaria, Pf-specific IgM B cells expand and upregulate activation... More

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