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O-Specific Polysaccharide-Specific Memory B Cell Responses in Young Children,Older Children,and Adults Infected with Vibrio cholerae O1 Ogawa in Bangladesh
Authors:Amena Aktar  M. Arifur Rahman  Sadia Afrin  M. Omar Faruk  Taher Uddin  Aklima Akter  M. Israk Nur Sami  Tahirah Yasmin  Fahima Chowdhury  Ashraful I. Khan  Daniel T. Leung  Regina C. LaRocque  Richelle C. Charles  Taufiqur Rahman Bhuiyan  Anjali Mandlik  Meagan Kelly  Pavol Ková?   Peng Xu  Stephen B. Calderwood  Jason B. Harris  Firdausi Qadri  Edward T. Ryan
Abstract:Cholera caused by Vibrio cholerae O1 confers at least 3 to 10 years of protection against subsequent disease regardless of age, despite a relatively rapid fall in antibody levels in peripheral blood, suggesting that memory B cell responses may play an important role in protection. The V. cholerae O1-specific polysaccharide (OSP) component of lipopolysaccharide (LPS) is responsible for serogroup specificity, and it is unclear if young children are capable of developing memory B cell responses against OSP, a T cell-independent antigen, following cholera. To address this, we assessed OSP-specific memory B cell responses in young children (2 to 5 years, n = 11), older children (6 to 17 years, n = 21), and adults (18 to 55 years, n = 28) with cholera caused by V. cholerae O1 in Dhaka, Bangladesh. We also assessed memory B cell responses against LPS and vibriocidal responses, and plasma antibody responses against OSP, LPS, and cholera toxin B subunit (CtxB; a T cell-dependent antigen) on days 2 and 7, as well as days 30, 90, and 180 after convalescence. In all age cohorts, vibriocidal responses and plasma OSP, LPS, and CtxB-specific responses peaked on day 7 and fell toward baseline over the follow-up period. In comparison, we were able to detect OSP memory B cell responses in all age cohorts of patients with detectable responses over baseline for 90 to 180 days. Our results suggest that OSP-specific memory B cell responses can occur following cholera, even in the youngest children, and may explain in part the age-independent induction of long-term immunity following naturally acquired disease.
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