Migrant memory B cells secrete luminal antibody in the vagina
Ji Eun Oh,
Norifumi Iijima,
Eric Song,
Peiwen Lu,
Jonathan Klein,
Ruoyi Jiang,
Steven H. Kleinstein and
Akiko Iwasaki ()
Additional contact information
Ji Eun Oh: Yale School of Medicine
Norifumi Iijima: Yale School of Medicine
Eric Song: Yale School of Medicine
Peiwen Lu: Yale School of Medicine
Jonathan Klein: Yale School of Medicine
Ruoyi Jiang: Yale School of Medicine
Steven H. Kleinstein: Yale School of Medicine
Akiko Iwasaki: Yale School of Medicine
Nature, 2019, vol. 571, issue 7763, 122-126
Abstract:
Abstract Antibodies secreted into mucosal barriers serve to protect the host from a variety of pathogens, and are the basis for successful vaccines1. In type I mucosa (such as the intestinal tract), dimeric IgA secreted by local plasma cells is transported through polymeric immunoglobulin receptors2 and mediates robust protection against viruses3,4. However, owing to the paucity of polymeric immunoglobulin receptors and plasma cells, how and whether antibodies are delivered to the type II mucosa represented by the lumen of the lower female reproductive tract remains unclear. Here, using genital herpes infection in mice, we show that primary infection does not establish plasma cells in the lamina propria of the female reproductive tract. Instead, upon secondary challenge with herpes simplex virus 2, circulating memory B cells that enter the female reproductive tract serve as the source of rapid and robust antibody secretion into the lumen of this tract. CD4 tissue-resident memory T cells secrete interferon-γ, which induces expression of chemokines, including CXCL9 and CXCL10. Circulating memory B cells are recruited to the vaginal mucosa in a CXCR3-dependent manner, and secrete virus-specific IgG2b, IgG2c and IgA into the lumen. These results reveal that circulating memory B cells act as a rapidly inducible source of mucosal antibodies in the female reproductive tract.
Date: 2019
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DOI: 10.1038/s41586-019-1285-1
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