Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae

Vibrio cholerae infection provides long-lasting protective immunity, while oral, inactivated cholera vaccines (OCV) result in more-limited protection. To identify characteristics of the innate immune response that may distinguish natural V. cholerae infection from OCV, we stimulated differentiated,...

Descripción completa

Detalles Bibliográficos
Autores principales: Weil, Ana A., Ellis, Crystal N., Debela, Meti D., Bhuiyan, Taufiqur R., Rashu, Rasheduzzaman, Bourque, Daniel L., Khan, Ashraful I., Chowdhury, Fahima, LaRocque, Regina C., Charles, Richelle C., Ryan, Edward T., Calderwood, Stephen B., Qadri, Firdausi, Harris, Jason B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6706466/
https://www.ncbi.nlm.nih.gov/pubmed/31434744
http://dx.doi.org/10.1128/mSphere.00206-19
_version_ 1783445708591857664
author Weil, Ana A.
Ellis, Crystal N.
Debela, Meti D.
Bhuiyan, Taufiqur R.
Rashu, Rasheduzzaman
Bourque, Daniel L.
Khan, Ashraful I.
Chowdhury, Fahima
LaRocque, Regina C.
Charles, Richelle C.
Ryan, Edward T.
Calderwood, Stephen B.
Qadri, Firdausi
Harris, Jason B.
author_facet Weil, Ana A.
Ellis, Crystal N.
Debela, Meti D.
Bhuiyan, Taufiqur R.
Rashu, Rasheduzzaman
Bourque, Daniel L.
Khan, Ashraful I.
Chowdhury, Fahima
LaRocque, Regina C.
Charles, Richelle C.
Ryan, Edward T.
Calderwood, Stephen B.
Qadri, Firdausi
Harris, Jason B.
author_sort Weil, Ana A.
collection PubMed
description Vibrio cholerae infection provides long-lasting protective immunity, while oral, inactivated cholera vaccines (OCV) result in more-limited protection. To identify characteristics of the innate immune response that may distinguish natural V. cholerae infection from OCV, we stimulated differentiated, macrophage-like THP-1 cells with live versus heat-inactivated V. cholerae with and without endogenous or exogenous cholera holotoxin (CT). Interleukin 23A gene (IL23A) expression was higher in cells exposed to live V. cholerae than in cells exposed to inactivated organisms (mean change, 38-fold; 95% confidence interval [95% CI], 4.0 to 42; P < 0.01). IL-23 secretion was also higher in cells exposed to live V. cholerae than in cells exposed to inactivated V. cholerae (mean change, 5.6-fold; 95% CI, 4.4 to 11; P < 0.001). This increase in IL-23 secretion was more marked than for other key innate immune cytokines (e.g., IL-1β and IL-6) and dependent on exposure to the combination of both live V. cholerae and CT. While IL-23 secretion was reduced following stimulation with either heat-inactivated wild-type V. cholerae or a live isogenic ctxAB mutant of V. cholerae, the addition of exogenous CT restored IL-23 secretion in combination with the live isogenic ctxAB mutant V. cholerae, but not when it was paired with stimulation by heat-inactivated V. cholerae. The posttranslational regulation of IL-23 under these conditions was dependent on the activity of the cysteine protease cathepsin B. In humans, IL-23 promotes the differentiation of Th17 cells to T follicular helper cells, which maintain and support long-term memory B cell generation after infection. Based on these findings, the stimulation of IL-23 production may be a determinant of protective immunity following V. cholerae infection. IMPORTANCE An episode of cholera provides better protection against reinfection than oral cholera vaccines, and the reasons for this are still under study. To better understand this, we compared the immune responses of human cells exposed to live Vibrio cholerae with those of cells exposed to heat-killed V. cholerae (similar to the contents of oral cholera vaccines). We also compared the effects of active cholera toxin and the inactive cholera toxin B subunit (which is included in some cholera vaccines). One key immune signaling molecule, IL-23, was uniquely produced in response to the combination of live bacteria and active cholera holotoxin. Stimulation with V. cholerae that did not produce the active toxin or was killed did not produce an IL-23 response. The stimulation of IL-23 production by cholera toxin-producing V. cholerae may be important in conferring long-term immunity after cholera.
format Online
Article
Text
id pubmed-6706466
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher American Society for Microbiology
record_format MEDLINE/PubMed
spelling pubmed-67064662019-08-29 Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae Weil, Ana A. Ellis, Crystal N. Debela, Meti D. Bhuiyan, Taufiqur R. Rashu, Rasheduzzaman Bourque, Daniel L. Khan, Ashraful I. Chowdhury, Fahima LaRocque, Regina C. Charles, Richelle C. Ryan, Edward T. Calderwood, Stephen B. Qadri, Firdausi Harris, Jason B. mSphere Research Article Vibrio cholerae infection provides long-lasting protective immunity, while oral, inactivated cholera vaccines (OCV) result in more-limited protection. To identify characteristics of the innate immune response that may distinguish natural V. cholerae infection from OCV, we stimulated differentiated, macrophage-like THP-1 cells with live versus heat-inactivated V. cholerae with and without endogenous or exogenous cholera holotoxin (CT). Interleukin 23A gene (IL23A) expression was higher in cells exposed to live V. cholerae than in cells exposed to inactivated organisms (mean change, 38-fold; 95% confidence interval [95% CI], 4.0 to 42; P < 0.01). IL-23 secretion was also higher in cells exposed to live V. cholerae than in cells exposed to inactivated V. cholerae (mean change, 5.6-fold; 95% CI, 4.4 to 11; P < 0.001). This increase in IL-23 secretion was more marked than for other key innate immune cytokines (e.g., IL-1β and IL-6) and dependent on exposure to the combination of both live V. cholerae and CT. While IL-23 secretion was reduced following stimulation with either heat-inactivated wild-type V. cholerae or a live isogenic ctxAB mutant of V. cholerae, the addition of exogenous CT restored IL-23 secretion in combination with the live isogenic ctxAB mutant V. cholerae, but not when it was paired with stimulation by heat-inactivated V. cholerae. The posttranslational regulation of IL-23 under these conditions was dependent on the activity of the cysteine protease cathepsin B. In humans, IL-23 promotes the differentiation of Th17 cells to T follicular helper cells, which maintain and support long-term memory B cell generation after infection. Based on these findings, the stimulation of IL-23 production may be a determinant of protective immunity following V. cholerae infection. IMPORTANCE An episode of cholera provides better protection against reinfection than oral cholera vaccines, and the reasons for this are still under study. To better understand this, we compared the immune responses of human cells exposed to live Vibrio cholerae with those of cells exposed to heat-killed V. cholerae (similar to the contents of oral cholera vaccines). We also compared the effects of active cholera toxin and the inactive cholera toxin B subunit (which is included in some cholera vaccines). One key immune signaling molecule, IL-23, was uniquely produced in response to the combination of live bacteria and active cholera holotoxin. Stimulation with V. cholerae that did not produce the active toxin or was killed did not produce an IL-23 response. The stimulation of IL-23 production by cholera toxin-producing V. cholerae may be important in conferring long-term immunity after cholera. American Society for Microbiology 2019-08-21 /pmc/articles/PMC6706466/ /pubmed/31434744 http://dx.doi.org/10.1128/mSphere.00206-19 Text en Copyright © 2019 Weil et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Weil, Ana A.
Ellis, Crystal N.
Debela, Meti D.
Bhuiyan, Taufiqur R.
Rashu, Rasheduzzaman
Bourque, Daniel L.
Khan, Ashraful I.
Chowdhury, Fahima
LaRocque, Regina C.
Charles, Richelle C.
Ryan, Edward T.
Calderwood, Stephen B.
Qadri, Firdausi
Harris, Jason B.
Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae
title Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae
title_full Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae
title_fullStr Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae
title_full_unstemmed Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae
title_short Posttranslational Regulation of IL-23 Production Distinguishes the Innate Immune Responses to Live Toxigenic versus Heat-Inactivated Vibrio cholerae
title_sort posttranslational regulation of il-23 production distinguishes the innate immune responses to live toxigenic versus heat-inactivated vibrio cholerae
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6706466/
https://www.ncbi.nlm.nih.gov/pubmed/31434744
http://dx.doi.org/10.1128/mSphere.00206-19
work_keys_str_mv AT weilanaa posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT elliscrystaln posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT debelametid posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT bhuiyantaufiqurr posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT rashurasheduzzaman posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT bourquedaniell posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT khanashrafuli posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT chowdhuryfahima posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT larocquereginac posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT charlesrichellec posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT ryanedwardt posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT calderwoodstephenb posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT qadrifirdausi posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae
AT harrisjasonb posttranslationalregulationofil23productiondistinguishestheinnateimmuneresponsestolivetoxigenicversusheatinactivatedvibriocholerae

Ejemplares similares