Spatially regulated protease activity in lymph nodes renders B cell follicles a sanctuary for retention of intact antigens

Author:

Aung Aereas,Cui Ang,Soleimany Ava P.ORCID,Bukenya Maurice,Lee Heya,Cottrell Christopher A.ORCID,Silva Murillo,Kirkpatrick Jesse D.,Gregory Justin R.,Amlashi Parastoo,Remba Tanaka,Froehle Leah M.,Xiao Shuhao,Abraham Wuhbet,Adams Josetta,Suh Heikyung,Huyett Phillip,Kwon Douglas S.,Hacohen Nir,Schief William R.,Bhatia Sangeeta N.,Irvine Darrell J.

Abstract

SUMMARYThe structural integrity of vaccine antigens is critical, as antigen degradation in vivo could eliminate neutralizing epitopes and create competing B cell responses against irrelevant breakdown products. Using FRET imaging and imaging zymography, we found that protease activity and antigen breakdown are spatially heterogeneous in lymph nodes. Following protein immunization, antigens are rapidly degraded in the subcapsular sinus, paracortex, and interfollicular regions of the tissue. By contrast, the follicles and follicular dendritic cell (FDC) networks exhibit low protease activity and antigen degradation rates. Immunization regimens targeting antigen rapidly to FDCs led to germinal centers (GCs) where responses to intact antigen were highly dominant, while traditional bolus immunizations led to weaker GC responses where more GC B cells bound to breakdown products than intact antigen. Thus, spatially-compartmentalized antigen proteolysis impacts humoral immunity and can be exploited to enhance vaccine-induced production of antibody responses against key pathogen structural epitopes.

Publisher

Cold Spring Harbor Laboratory

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