c-Src and c-Abl kinases control hierarchic phosphorylation and function of the CagA effector protein in Western and East Asian Helicobacter pylori strains
Doreen Mueller, … , Adam Smolka, Steffen Backert
Doreen Mueller, … , Adam Smolka, Steffen Backert
Published March 1, 2012
Citation Information: J Clin Invest. 2012;122(4):1553-1566. https://doi.org/10.1172/JCI61143.
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Research Article

c-Src and c-Abl kinases control hierarchic phosphorylation and function of the CagA effector protein in Western and East Asian Helicobacter pylori strains

Abstract

Many bacterial pathogens inject into host cells effector proteins that are substrates for host tyrosine kinases such as Src and Abl family kinases. Phosphorylated effectors eventually subvert host cell signaling, aiding disease development. In the case of the gastric pathogen Helicobacter pylori, which is a major risk factor for the development of gastric cancer, the only known effector protein injected into host cells is the oncoprotein CagA. Here, we followed the hierarchic tyrosine phosphorylation of H. pylori CagA as a model system to study early effector phosphorylation processes. Translocated CagA is phosphorylated on Glu-Pro-Ile-Tyr-Ala (EPIYA) motifs EPIYA-A, EPIYA-B, and EPIYA-C in Western strains of H. pylori and EPIYA-A, EPIYA-B, and EPIYA-D in East Asian strains. We found that c-Src only phosphorylated EPIYA-C and EPIYA-D, whereas c-Abl phosphorylated EPIYA-A, EPIYA-B, EPIYA-C, and EPIYA-D. Further analysis revealed that CagA molecules were phosphorylated on 1 or 2 EPIYA motifs, but never simultaneously on 3 motifs. Furthermore, none of the phosphorylated EPIYA motifs alone was sufficient for inducing AGS cell scattering and elongation. The preferred combination of phosphorylated EPIYA motifs in Western strains was EPIYA-A and EPIYA-C, either across 2 CagA molecules or simultaneously on 1. Our study thus identifies a tightly regulated hierarchic phosphorylation model for CagA starting at EPIYA-C/D, followed by phosphorylation of EPIYA-A or EPIYA-B. These results provide insight for clinical H. pylori typing and clarify the role of phosphorylated bacterial effector proteins in pathogenesis.

Authors

Doreen Mueller, Nicole Tegtmeyer, Sabine Brandt, Yoshio Yamaoka, Eimear De Poire, Dionyssios Sgouras, Silja Wessler, Javier Torres, Adam Smolka, Steffen Backert

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Figure 7

Clinical Western H. pylori strains expressing CagA EPIYA-AC, but not EPIYA-AB or EPIYA-BC, induce profound AGS cell elongation.

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Clinical Western H. pylori strains expressing CagA EPIYA-AC, but not EPI...
(A) AGS cells were infected for 4 hours with strains expressing the combinations EPIYA-AB, EPIYA-BC, EPIYA-AC, and EPIYA-ABC (control). See Supplemental Figure 8 for specific EPIYA motifs and flanking sequences. CagA phosphorylation was examined using α–PY-CagA and α-CagA antibodies (arrows). The asterisk in the lower panel indicates antibody cross-reactivity with an unknown phosphorylated host cell protein. (B) Quantification of CagA phosphorylation signals using the luminescence image analyzer. (C) The number of elongated cells in each experiment was quantitated in triplicate in 10 different 0.25-mm2 fields. *P ≤ 0.01; **P ≤ 0.001.