4.5 Article

Increased sensitivity to tryptophan bioavailability is a positive adaptation by the human strains of Chlamydia pneumoniae

Journal

MOLECULAR MICROBIOLOGY
Volume 93, Issue 4, Pages 797-813

Publisher

WILEY-BLACKWELL
DOI: 10.1111/mmi.12701

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Funding

  1. NHMRC

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One of the most significant activities induced by interferon-gamma against intracellular pathogens is the induction of IDO (indoleamine 2,3-dioxygenase) expression, which subsequently results in the depletion of tryptophan. We tested the hypothesis that human strains of Chlamydia pneumoniae are more sensitive to tryptophan limitation than animal C. pneumoniae strains. The human strains were significantly more sensitive to IFN-gamma than the animal strains in a lung epithelia cell model (BEAS-2B), with exposure to 1 U ml(-1) IFN-gamma resulting in complete loss of infectious yield of human strains, compared to the animal strains where reductions in infectious progeny were around 3.5-4.0 log. Strikingly, the IFN-gamma induced loss of ability to form infectious progeny production was completely rescued by removal of the IFN-gamma and addition of exogenous tryptophan for the human strains, but not the animal strains. In fact, a human heart strain was more capable of entering a non-infectious, viable persistent stage when exposed to IFN-gamma and was also more effectively rescued, compared to a human respiratory strain. Exquisite susceptibility to IFN-gamma, specifically due to tryptophan availability appears to be a core adaptation of the human C. pneumoniae strains, which may reflect the chronic nature of their infections in this host.

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