Low protease activity in B cell follicles promotes retention of intact antigens after immunization

Aereas Aung(Allen Institute), Ang Cui(Broad Institute), Laura Maiorino(Allen Institute), Ava P. Amini(Microsoft (United States)), Justin R. Gregory(Allen Institute), Maurice Bukenya(Allen Institute), Yiming J. Zhang(Allen Institute), Heya Lee(Allen Institute), Christopher A. Cottrell(Scripps Research Institute), Duncan M. Morgan(Allen Institute), Murillo Silva(Allen Institute), Heikyung Suh(Allen Institute), Jesse D. Kirkpatrick(Harvard–MIT Division of Health Sciences and Technology), Parastoo Amlashi(Allen Institute), Tanaka Remba(Allen Institute), Leah Froehle(Ragon Institute of MGH, MIT and Harvard), Shuhao Xiao(Allen Institute), Wuhbet Abraham(Allen Institute), Josetta Adams(Allen Institute), J. Christopher Love(Broad Institute), Phillip Huyett(Massachusetts Eye and Ear Infirmary), Douglas S. Kwon(Ragon Institute of MGH, MIT and Harvard), Nir Hacohen(Broad Institute), William R. Schief(Scripps Research Institute), Sangeeta N. Bhatia(Broad Institute), Darrell J. Irvine(Scripps Research Institute)
Science
January 26, 2023
Cited by 96Open Access
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Abstract

The structural integrity of vaccine antigens is critical to the generation of protective antibody responses, but the impact of protease activity on vaccination in vivo is poorly understood. We characterized protease activity in lymph nodes and found that antigens were rapidly degraded in the subcapsular sinus, paracortex, and interfollicular regions, whereas low protease activity and antigen degradation rates were detected in the vicinity of follicular dendritic cells (FDCs). Correlated with these findings, immunization regimens designed to target antigen to FDCs led to germinal centers dominantly targeting intact antigen, whereas traditional immunizations led to much weaker responses that equally targeted the intact immunogen and antigen breakdown products. Thus, spatially compartmentalized antigen proteolysis affects humoral immunity and can be exploited.


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