Issue 3, 2018

Nanoparticle binding attenuates the pathobiology of gastric cancer-associated Helicobacter pylori

Abstract

Enteric bacteria may cause severe diseases, including gastric cancer-associated Helicobacter pylori. Their infection paths overlap with the oro-gastrointestinal uptake route for nanoparticles, increasingly occurring during environmental or consumer/medical exposure. By comprehensive independent analytical methods, such as live cell fluorescence, electron as well as atomic force microscopy and elemental analysis, we show that a wide array of nanoparticles (NPs) but not microparticles form complexes with H. pylori and enteric pathogens without the need for specific functionalization. The NP-assembly that occurred rapidly was not influenced by variations in physiological temperature, though affected by the NPs’ physico-chemical characteristics. Improved binding was observed for small NPs with a negative surface charge, whereas binding could be reduced by surface ‘stealth’ modifications. Employing human gastric epithelial cells and 3D-organoid models of the stomach, we show that NP-coating did not inhibit H. pylori's cellular attachment. However, even the assembly of non-bactericidal silica NPs attenuated H. pylori infection by reducing CagA phosphorylation, cytoskeletal rearrangement, and IL-8 secretion. Here we demonstrate that NP binding to enteric bacteria may impact their pathobiology which could be further exploited to rationally modulate the (patho)biology of microbes by nanomaterials.

Graphical abstract: Nanoparticle binding attenuates the pathobiology of gastric cancer-associated Helicobacter pylori

Associated articles

Supplementary files

Article information

Article type
Paper
Submitted
04 Sep 2017
Accepted
04 Dec 2017
First published
05 Dec 2017

Nanoscale, 2018,10, 1453-1463

Nanoparticle binding attenuates the pathobiology of gastric cancer-associated Helicobacter pylori

D. Westmeier, G. Posselt, A. Hahlbrock, S. Bartfeld, C. Vallet, C. Abfalter, D. Docter, S. K. Knauer, S. Wessler and R. H. Stauber, Nanoscale, 2018, 10, 1453 DOI: 10.1039/C7NR06573F

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