Journal
CHEMBIOCHEM
Volume 22, Issue 18, Pages 2783-2790Publisher
WILEY-V C H VERLAG GMBH
DOI: 10.1002/cbic.202100249
Keywords
antimicrobial; bacterial pathogenesis; glycobiology; Helicobacter pylori; host-pathogen interactions; innate immunity; iron homeostasis; lactoferrin; toxin secretion; virulence
Funding
- Office of Medical Research, Department of Veterans Affairs [IK2BX001701]
- National Institutes of Health [R01 HD090061]
- NIH [GM05551, T32 HL007411-36S1, P30DK058404]
- Childhood Infections Research Program [T32 HL007411-36S1, T32-AI095202, 2T32AI112541-06, K08AI151100, R35GM133602]
- National Science Foundation [1547757, 1400969]
- Vanderbilt Institute for Clinical and Translational Research program - National Center for Research Resources [UL1RR024975-01]
- National Center for Advancing Translational Sciences [2UL1TR000445-06, 5UL1TR002243-03]
- Division Of Human Resource Development
- Direct For Education and Human Resources [1400969] Funding Source: National Science Foundation
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Chronic infection with Helicobacter pylori increases the risk of gastric diseases, including gastric cancer, with strains encoding the cag T4SS system being associated with more serious disease outcomes. The presence of nutrient iron can modulate the activity of the T4SS and biogenesis of T4SS pili, with lactoferrin exerting antimicrobial activity against H. pylori under iron-limited conditions. Additionally, culturing H. pylori with holo-lactoferrin prior to co-culture with gastric epithelial cells can lead to repression of the cag T4SS activity and decreased biogenesis of T4SS pili.
Chronic infection with Helicobacter pylori increases risk of gastric diseases including gastric cancer. Despite development of a robust immune response, H. pylori persists in the gastric niche. Progression of gastric inflammation to serious disease outcomes is associated with infection with H. pylori strains which encode the cag Type IV Secretion System (cag T4SS). The cag T4SS is responsible for translocating the oncogenic protein CagA into host cells and inducing pro-inflammatory and carcinogenic signaling cascades. Our previous work demonstrated that nutrient iron modulates the activity of the T4SS and biogenesis of T4SS pili. In response to H. pylori infection, the host produces a variety of antimicrobial molecules, including the iron-binding glycoprotein, lactoferrin. Our work shows that apo-lactoferrin exerts antimicrobial activity against H. pylori under iron-limited conditions, while holo-lactoferrin enhances bacterial growth. Culturing H. pylori in the presence of holo-lactoferrin prior to co-culture with gastric epithelial cells, results in repression of the cag T4SS activity. Concomitantly, a decrease in biogenesis of cag T4SS pili at the host-pathogen interface was observed under these culture conditions by high-resolution electron microscopy analyses. Taken together, these results indicate that acquisition of alternate sources of nutrient iron plays a role in regulating the pro-inflammatory activity of a bacterial secretion system and present novel therapeutic targets for the treatment of H. pylori-related disease.
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