αv Integrins regulate germinal center B cell responses through noncanonical autophagy
Fiona Raso, … , Adam Lacy-Hulbert, Mridu Acharya
Fiona Raso, … , Adam Lacy-Hulbert, Mridu Acharya
Published July 12, 2018
Citation Information: J Clin Invest. 2018;128(9):4163-4178. https://doi.org/10.1172/JCI99597.
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Research Article Immunology

αv Integrins regulate germinal center B cell responses through noncanonical autophagy

Abstract

Germinal centers (GCs) are major sites of clonal B cell expansion and generation of long-lived, high-affinity antibody responses to pathogens. Signaling through TLRs on B cells promotes many aspects of GC B cell responses, including affinity maturation, class switching, and differentiation into long-lived memory and plasma cells. A major challenge for effective vaccination is identifying strategies to specifically promote GC B cell responses. Here, we have identified a mechanism of regulation of GC B cell TLR signaling, mediated by αv integrins and noncanonical autophagy. Using B cell–specific αv-KO mice, we show that loss of αv-mediated TLR regulation increased GC B cell expansion, somatic hypermutation, class switching, and generation of long-lived plasma cells after immunization with virus-like particles (VLPs) or antigens associated with TLR ligand adjuvants. Furthermore, targeting αv-mediated regulation increased the magnitude and breadth of antibody responses to influenza virus vaccination. These data therefore identify a mechanism of regulation of GC B cells that can be targeted to enhance antibody responses to vaccination.

Authors

Fiona Raso, Sara Sagadiev, Samuel Du, Emily Gage, Tanvi Arkatkar, Genita Metzler, Lynda M. Stuart, Mark T. Orr, David J. Rawlings, Shaun W. Jackson, Adam Lacy-Hulbert, Mridu Acharya

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Figure 6

Increased antibody production in αv-CD19 mice.

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Increased antibody production in αv-CD19 mice. (A–B) Serum anti-VLP anti...
(AB) Serum anti-VLP antibody titers in control and αv-CD19 mice immunized with 2 μg VLPs containing ssRNA measured 14 days after immunization (A) or over a time course from preimmunization (pre) to 35 days (B). VLP-specific Abs were not detected (ND) in preimmunization bleeds. (C) Serum anti-NP IgM, IgG, IgG1, and Ig2c titers in control and αv-CD19 mice immunized with NP-CG (50 μg) combined with TLR7 ligand imiquimod-SE (10 μg). (D) Serum anti-NP IgG1 and IgG2c antibody titers in control and αv-CD19 mice immunized with NP-CG (50 μg) combined with LPS (5 μg). All data points represent individual mice with mean shown. P values of less than 0.05 are shown (Mann-Whitney-Wilcoxon test). *P < 0.05; **P < 0.005. Samples below the level of detection are indicated as not detected. Similar results were seen in 3 independent experiments.