cGAS-mediated control of blood-stage malaria promotes Plasmodium-specific germinal center responses
William O. Hahn, Noah S. Butler, Scott E. Lindner, Holly M. Akilesh, D. Noah Sather, Stefan H.I. Kappe, Jessica A. Hamerman, Michael Gale Jr., W. Conrad Liles, Marion Pepper
William O. Hahn, Noah S. Butler, Scott E. Lindner, Holly M. Akilesh, D. Noah Sather, Stefan H.I. Kappe, Jessica A. Hamerman, Michael Gale Jr., W. Conrad Liles, Marion Pepper
View: Text | PDF
Research Article Immunology Infectious disease

cGAS-mediated control of blood-stage malaria promotes Plasmodium-specific germinal center responses

Abstract

Sensing of pathogens by host pattern recognition receptors is essential for activating the immune response during infection. We used a nonlethal murine model of malaria (Plasmodium yoelii 17XNL) to assess the contribution of the pattern recognition receptor cyclic GMP-AMP synthase (cGAS) to the development of humoral immunity. Despite previous reports suggesting a critical, intrinsic role for cGAS in early B cell responses, cGAS-deficient (cGAS–/–) mice had no defect in the early expansion or differentiation of Plasmodium-specific B cells. As the infection proceeded, however, cGAS–/– mice exhibited higher parasite burdens and aberrant germinal center and memory B cell formation when compared with littermate controls. Antimalarial drugs were used to further demonstrate that the disrupted humoral response was not B cell intrinsic but instead was a secondary effect of a loss of parasite control. These findings therefore demonstrate that cGAS-mediated innate-sensing contributes to parasite control but is not intrinsically required for the development of humoral immunity. Our findings highlight the need to consider the indirect effects of pathogen burden in investigations examining how the innate immune system affects the adaptive immune response.

Authors

William O. Hahn, Noah S. Butler, Scott E. Lindner, Holly M. Akilesh, D. Noah Sather, Stefan H.I. Kappe, Jessica A. Hamerman, Michael Gale Jr., W. Conrad Liles, Marion Pepper

×

Figure 6

Prolonged reduction in germinal center response is associated with reduced memory B cell formation in cGAS–/– mice.

Options: View larger image (or click on image) Download as PowerPoint
Prolonged reduction in germinal center response is associated with reduc...
(A) Spleen sections were stained with antibodies against PNA, B220, and CD4. Scale bar: 1,000 μm (first and third images); 100 μm (second and fourth images). (B) Quantification of MSP1+ B cells subsets 22 days after infection with Plasmodium yoelii 17XNL. Error bars represent SD. *P > 0.05, ***P < 0.001, ****P < 0.0001, by unpaired Student’s t test. (C and D) Quantification of serum levels of MSP1-specific IgG2c and IgM 22 days after infection. Data represent 7 biological replicates from 3 pooled experiments. Statistical analysis was performed using the unpaired Student’s t test. Error bars represent SD. **P < 0.01, ***P < 0.001. (E) Mean fluorescent intensity of CD73 on MSP1-specific memory B cells that are CD38+/GL7 22 days after infection. Representative data are shown representative of 2 separate experiments. The geometric mean intensity (GMI) of cGAS–/– mice was 600 ± 151 as compared with versus 1,763 ± 112 in WT controls. P < 0.001 by unpaired Student’s t test. Error bars represent SD. *P < 0.05.