Cargando…
The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection
BACKGROUND: Chlamydia trachomatis infection results in reproductive damage in some women. The process and factors involved in this immunopathology are not well understood. This study aimed to investigate the role of primary human cellular responses to chlamydial stress response proteases and chlamyd...
| Autores principales: | , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
BioMed Central
2013
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4225670/ https://www.ncbi.nlm.nih.gov/pubmed/24238294 http://dx.doi.org/10.1186/1471-2172-14-50 |
| _version_ | 1782343550263885824 |
|---|---|
| author | Cunningham, Kelly Stansfield, Scott H Patel, Pooja Menon, Shruti Kienzle, Vivian Allan, John A Huston, Wilhelmina M |
| author_facet | Cunningham, Kelly Stansfield, Scott H Patel, Pooja Menon, Shruti Kienzle, Vivian Allan, John A Huston, Wilhelmina M |
| author_sort | Cunningham, Kelly |
| collection | PubMed |
| description | BACKGROUND: Chlamydia trachomatis infection results in reproductive damage in some women. The process and factors involved in this immunopathology are not well understood. This study aimed to investigate the role of primary human cellular responses to chlamydial stress response proteases and chlamydial infection to further identify the immune processes involved in serious disease sequelae. RESULTS: Laboratory cell cultures and primary human reproductive epithelial cultures produced IL-6 in response to chlamydial stress response proteases (CtHtrA and CtTsp), UV inactivated Chlamydia, and live Chlamydia. The magnitude of the IL-6 response varied considerably (up to 1000 pg ml(-1)) across different primary human reproductive cultures. Thus different levels of IL-6 production by reproductive epithelia may be a determinant in disease outcome. Interestingly, co-culture models with either THP-1 cells or autologous primary human PBMC generally resulted in increased levels of IL-6, except in the case of live Chlamydia where the level of IL-6 was decreased compared to the epithelial cell culture only, suggesting this pathway may be able to be modulated by live Chlamydia. PBMC responses to the stress response proteases (CtTsp and CtHtrA) did not significantly vary for the different participant cohorts. Therefore, these proteases may possess conserved innate PAMPs. MAP kinases appeared to be involved in this IL-6 induction from human cells. Finally, we also demonstrated that IL-6 was induced by these proteins and Chlamydia from mouse primary reproductive cell cultures (BALB/C mice) and mouse laboratory cell models. CONCLUSIONS: We have demonstrated that IL-6 may be a key factor for the chlamydial disease outcome in humans, given that primary human reproductive epithelial cell culture showed considerable variation in IL-6 response to Chlamydia or chlamydial proteins, and that the presence of live Chlamydia (but not UV killed) during co-culture resulted in a reduced IL-6 response suggesting this response may be moderated by the presence of the organism. |
| format | Online Article Text |
| id | pubmed-4225670 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2013 |
| publisher | BioMed Central |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-42256702014-11-11 The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection Cunningham, Kelly Stansfield, Scott H Patel, Pooja Menon, Shruti Kienzle, Vivian Allan, John A Huston, Wilhelmina M BMC Immunol Research Article BACKGROUND: Chlamydia trachomatis infection results in reproductive damage in some women. The process and factors involved in this immunopathology are not well understood. This study aimed to investigate the role of primary human cellular responses to chlamydial stress response proteases and chlamydial infection to further identify the immune processes involved in serious disease sequelae. RESULTS: Laboratory cell cultures and primary human reproductive epithelial cultures produced IL-6 in response to chlamydial stress response proteases (CtHtrA and CtTsp), UV inactivated Chlamydia, and live Chlamydia. The magnitude of the IL-6 response varied considerably (up to 1000 pg ml(-1)) across different primary human reproductive cultures. Thus different levels of IL-6 production by reproductive epithelia may be a determinant in disease outcome. Interestingly, co-culture models with either THP-1 cells or autologous primary human PBMC generally resulted in increased levels of IL-6, except in the case of live Chlamydia where the level of IL-6 was decreased compared to the epithelial cell culture only, suggesting this pathway may be able to be modulated by live Chlamydia. PBMC responses to the stress response proteases (CtTsp and CtHtrA) did not significantly vary for the different participant cohorts. Therefore, these proteases may possess conserved innate PAMPs. MAP kinases appeared to be involved in this IL-6 induction from human cells. Finally, we also demonstrated that IL-6 was induced by these proteins and Chlamydia from mouse primary reproductive cell cultures (BALB/C mice) and mouse laboratory cell models. CONCLUSIONS: We have demonstrated that IL-6 may be a key factor for the chlamydial disease outcome in humans, given that primary human reproductive epithelial cell culture showed considerable variation in IL-6 response to Chlamydia or chlamydial proteins, and that the presence of live Chlamydia (but not UV killed) during co-culture resulted in a reduced IL-6 response suggesting this response may be moderated by the presence of the organism. BioMed Central 2013-11-15 /pmc/articles/PMC4225670/ /pubmed/24238294 http://dx.doi.org/10.1186/1471-2172-14-50 Text en Copyright © 2013 Cunningham et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. |
| spellingShingle | Research Article Cunningham, Kelly Stansfield, Scott H Patel, Pooja Menon, Shruti Kienzle, Vivian Allan, John A Huston, Wilhelmina M The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| title | The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| title_full | The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| title_fullStr | The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| title_full_unstemmed | The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| title_short | The IL-6 response to Chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| title_sort | il-6 response to chlamydia from primary reproductive epithelial cells is highly variable and may be involved in differential susceptibility to the immunopathological consequences of chlamydial infection |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4225670/ https://www.ncbi.nlm.nih.gov/pubmed/24238294 http://dx.doi.org/10.1186/1471-2172-14-50 |
| work_keys_str_mv | AT cunninghamkelly theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT stansfieldscotth theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT patelpooja theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT menonshruti theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT kienzlevivian theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT allanjohna theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT hustonwilhelminam theil6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT cunninghamkelly il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT stansfieldscotth il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT patelpooja il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT menonshruti il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT kienzlevivian il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT allanjohna il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection AT hustonwilhelminam il6responsetochlamydiafromprimaryreproductiveepithelialcellsishighlyvariableandmaybeinvolvedindifferentialsusceptibilitytotheimmunopathologicalconsequencesofchlamydialinfection |