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Vaccination with a structure-based stabilized version of malarial antigen Pfs48/45 elicits ultra-potent transmission-blocking antibody responses

Immunity. 2022-08; 
Brandon McLeod, Moustafa T Mabrouk, Kazutoyo Miura, Rashmi Ravichandran, Sally Kephart, Sophia Hailemariam, Thao P Pham, Anthony Semesi, Iga Kucharska, Prasun Kundu, Wei-Chiao Huang, Max Johnson, Alyssa Blackstone, Deleah Pettie, Michael Murphy, John C Kraft, Elizabeth M Leaf, Yang Jiao, Marga van de Vegte-Bolmer, Geert-Jan van Gemert, Jordache Ramjith, C Richter King, Randall S MacGill, Yimin Wu, Kelly K Lee, Matthijs M Jore, Neil P King, Jonathan F Lovell, Jean-Philippe Julien
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Catalog Peptides … Pfs48/45-6C-8GS-I53-50A fusions were synthesized and cloned by Genscript into pCMV with an N-terminal secrecon signal peptide and a C-terminal hexa-histidine tag. … Get A Quote

摘要

Malaria transmission-blocking vaccines (TBVs) aim to elicit human antibodies that inhibit sporogonic development of Plasmodium falciparum in mosquitoes, thereby preventing onward transmission. Pfs48/45 is a leading clinical TBV candidate antigen and is recognized by the most potent transmission-blocking monoclonal antibody (mAb) yet described; still, clinical development of Pfs48/45 antigens has been hindered, largely by its poor biochemical characteristics. Here, we used structure-based computational approaches to design Pfs48/45 antigens stabilized in the conformation recognized by the most potently inhibitory mAb, achieving >25°C higher thermostability compared with the wild-type protein. Antibodies elicite... More

关键词

antibodies, malaria, structure-based immunogen design