Mechanisms involved in Helicobacter pylori-induced interleukin-8 production by a gastric cancer cell line, MKN45
10.1128/iai.65.8.3218-3224.1997
Crossref journal-article
American Society for Microbiology
Infection and Immunity (235)
Abstract

Accumulating evidence suggests an important role of interleukin-8 (IL-8) in Helicobacter pylori infection-associated chronic atrophic gastritis and peptic ulcer. We observed in this study that a gastric cancer-derived cell line, MKN45, produced a massive amount of IL-8 upon coculture with live H. pylori but not with killed H. pylori, H. pylori culture supernatants, or live H. pylori separated by a permeable membrane, indicating that IL-8 production requires a direct contact between the cells and live bacteria. Moreover, the tyrosine kinase inhibitor herbimycin but neither a protein kinase C inhibitor (staurosporine) nor a protein kinase A inhibitor (H89) inhibited IL-8 production by MKN45 cells cocultured with live bacteria, suggesting the involvement of a tyrosine kinase(s) in H. pylori-induced IL-8 production. In addition, coculture of H. pylori induced IL-8 mRNA expression in MKN45 cells and an increase in luciferase activity in cells which were transfected with a luciferase expression vector linked with a 5'-flanking region of the IL-8 gene (bp -133 to +44), indicating that the induction of IL-8 production occurred at the transcriptional level. This region contain three cis elements important for induction of IL-8 gene expression: AP-1 (-126 to -120 bp), NF-IL6 (-94 to -81 bp), and NF-kappaB (-80 to -70 bp) binding sites. Mutation of the NF-kappaB binding site abrogated completely the induction of luciferase activity, whereas that of the AP-1 site partially reduced the induction. However, mutation of the NF-IL6 binding site resulted in no decrease in the induction of luciferase activity. Moreover, specific NF-kappaB complexes were detected in the nuclear proteins extracted from MKN45 cells which were infected with H. pylori. Collectively, these results suggest that H. pylori induced the activation of NF-kappaB as well as AP-1, leading to IL-8 gene transcription.

Bibliography

Aihara, M., Tsuchimoto, D., Takizawa, H., Azuma, A., Wakebe, H., Ohmoto, Y., Imagawa, K., Kikuchi, M., Mukaida, N., & Matsushima, K. (1997). Mechanisms involved in Helicobacter pylori-induced interleukin-8 production by a gastric cancer cell line, MKN45. Infection and Immunity, 65(8), 3218–3224.

Authors 10
  1. M Aihara (first)
  2. D Tsuchimoto (additional)
  3. H Takizawa (additional)
  4. A Azuma (additional)
  5. H Wakebe (additional)
  6. Y Ohmoto (additional)
  7. K Imagawa (additional)
  8. M Kikuchi (additional)
  9. N Mukaida (additional)
  10. K Matsushima (additional)
References 0 Referenced 211

None

Dates
Type When
Created 5 years, 7 months ago (Jan. 6, 2020, 2:19 p.m.)
Deposited 3 years, 5 months ago (March 5, 2022, 4:17 a.m.)
Indexed 1 week, 2 days ago (Aug. 19, 2025, 6:03 a.m.)
Issued 28 years ago (Aug. 1, 1997)
Published 28 years ago (Aug. 1, 1997)
Published Print 28 years ago (Aug. 1, 1997)
Funders 0

None

@article{Aihara_1997, title={Mechanisms involved in Helicobacter pylori-induced interleukin-8 production by a gastric cancer cell line, MKN45}, volume={65}, ISSN={1098-5522}, url={http://dx.doi.org/10.1128/iai.65.8.3218-3224.1997}, DOI={10.1128/iai.65.8.3218-3224.1997}, number={8}, journal={Infection and Immunity}, publisher={American Society for Microbiology}, author={Aihara, M and Tsuchimoto, D and Takizawa, H and Azuma, A and Wakebe, H and Ohmoto, Y and Imagawa, K and Kikuchi, M and Mukaida, N and Matsushima, K}, year={1997}, month=aug, pages={3218–3224} }