Chlamydiae are a diverse group of obligate intracellular prokaryotic pathogens that infect a wide spectrum of mammalian hosts. Paradoxically, this broad spectrum of infection and disease diversity occurs despite considerable conservation in chlamydial genome organization and structure. To better understand the genetic basis of chlamydial host tropism we have undertaken a comparative in vivo and in vitro functional genomic study of chlamydial host cell interactions. We find that chlamydiae have co-evolved specific virulence genes that function in a species-specific manner to evade IFN-gamma mediated host defense mechanisms. These findings have important implications for the design of humanized mice for the study of C. trachomatis pathogenesis, immunity, and vaccine development. We have shown that chlamydial virulence genes localize to the replication termination region of the genome. This region exhibits extensive genetic polymorphisms among strains and as such has been termed the plasticity zone (PZ). We have mapped and characterized genes within the PZ that confer host specific infection tropism and have identified the host genes targeted by these virulence factors. Specifically we have shown that human strains have maintained a functional tryptophan synthase (TS) operon that circumvents the effect of IFN-gamma mediated indoleamine 2,3-dixoygenase tryptophan deprivation in human cervical epithelial cells. The TS gene is unique to human strains and the IFN-gamma inducible IDO defense system unique to human epithelial cells; demonstrating an unambiguous biological connection supporting the coevolution of pathogen and host. Similarly, we have discovered that the genetically syntenous murine strains have evolved a completely different pathogen strategy for evading IFN-gamma mediated host specific defense in murine epithelial cells. This involves the secretion of a large cytotoxin located in the PZ, unique to murine strains, that targets and inactivates members of the murine specific IFN-gamma inducible small p47 GTPases; specifically the p47 GPTase Iigp, a G protein that functions in the intracellular trafficking of lipids to the trans-Golgi. To our knowledge this is an unprecedented finding in the field of bacterial pathogenesis because it demonstrates that a restricted complement of pathogen specific genes have evolved specifically to target host-specific IFN-gamma inducible host defense mechanisms; a pathogenetic strategy that defines host infection tropism. Future studies will focus on characterizing the molecular mechanism(s) of GTPase inactivation by the chlamydial toxin and studying the cellular and molecular basis of host resistance to chlamydial infection mediated by the murine specific GTPase gene family. This will involve biochemical assays to ascertain toxin mediated monoglycosylation or proteolytic modification of GTPases and cell biology experiments to determine the step in the chlamydial infection processes where GTPase function. Preliminary siRNA gene silencing and transfection experiments indicate that the p47 GTPase IIGP is the primary anti-chlamydial factor that inhibits growth of toxin deficient chlamydial strains. In summary, our findings show that chlamydial virulence genes have co-evolved specifically to evade IFN-gamma mediated host defense mechanisms. To our knowledge this is the first description of the molecular basis defining this unique bacterial pathogen-host relationship. These findings will allow targeted gene knock of p47 GTPases (Iigp) together with IDO IFN-gamma regulated epithelial cell expression transgenic mice to be made that will provide a novel small animal model that is """"""""humanized"""""""" in regard to chlamydial human challenge providing a relevant host for the study of C. trachomatis pathogenesis and immunity. Moreover, chlamydial PZ virulence genes represent novel targets for the development of new chlamydial anti-infectives and vaccines.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000845-07
Application #
7196651
Study Section
(LICP)
Project Start
Project End
Budget Start
Budget End
Support Year
7
Fiscal Year
2005
Total Cost
Indirect Cost
Name
Niaid Extramural Activities
Department
Type
DUNS #
City
State
Country
United States
Zip Code
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