4.6 Article

Antibody and memory B cell responses to the dengue virus NS1 antigen in individuals with varying severity of past infection

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IMMUNOLOGY
卷 -, 期 -, 页码 -

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WILEY
DOI: 10.1111/imm.13651

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antibodies; B-cell ELISpots; dengue; dengue fever; disease severity; neutralizing antibodies; NS1 antigen

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To understand the role of NS1-specific antibodies in disease pathogenesis, the levels of neutralizing antibodies, NS1-antibodies, IgG antibody subclasses, and NS1-specific memory B-cell responses were compared in individuals with different severities of dengue. The results showed that individuals with past severe dengue had higher levels of neutralizing antibodies and NS1-antibodies, as well as stronger antibody responses to DENV1, 2, and 4. The study also found that individuals with past dengue had broadly cross-reactive B-cell responses to multiple DENV serotypes. These findings are important for further understanding the functionality of NS1-specific antibodies and the antibody repertoire associated with protection against severe disease.
To further understand the role of NS1-specific antibodies (Abs) in disease pathogenesis, we compared neutralizing antibody levels (Nabs), NS1-Ab levels, IgG antibody subclass profiles and NS1-specific memory B-cell responses (Bmems) in individuals, with varying severity of past dengue. Nabs (Neut50 titres) were assessed using the Foci Reduction Neutralization Test (FRNT) and in-house ELISAs were used to assess NS1-Abs and NS1-Ab subclasses for all four DENV serotypes in individuals with past DF (n = 22), those with past DHF (n = 14) and seronegative (SN) individuals (n = 7). B-cell ELISpot assays were used to assess NS1-specific Bmem responses. 15/22 (68.18%) individuals with past DF and 9/14 (64.29%) individuals with past DHF had heterotypic infections. Neut50 titres were found to be significantly higher for DENV1 than DENV2 (p = 0.0006) and DENV4 (p = 0.0127), in those with past DHF, whereas there was no significant difference seen in titres for different DENV serotypes in those with past DF. Overall NS1-Ab to all serotypes and NS1-specific IgG1 responses for DENV1, 2 and 4 serotypes were significantly higher in those with past DHF than individuals with past DF. Those with past DHF also had higher IgG1 than IgG3 for DENV1 and DENV3, whereas no differences were seen in those with past DF. Over 50% of those with past DF or DHF had NS1-specific Bmem responses to >2 DENV serotypes. There was no difference in the frequency of Bmem responses to any of the DENV serotypes between individuals with past DF and DHF. Although the frequency of Bmem responses to DENV1 correlated with DENV1-specific NS1-Abs levels (Spearman r = 0.35, p = 0.02), there was no correlation with other DENV serotypes. We found that those with past DF had broadly cross-reactive Nabs, while those with past DHF had higher NS1-Ab responses possibly with a different functionality profile than those with past DF. Therefore, it would be important to further evaluate the functionality of NS1-specific antibody and Bmem responses to find out the type of antibody repertoire that is associated with protection against severe disease.

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