Francisella inhibits STAT1-mediated signaling in macrophages and prevents activation of antigen-specific T cells

doi:10.1093/intimm/dxn119

International Immunology Advance Access originally published online on November 11, 2008
International Immunology 2009 21(1):19-28; doi:10.1093/intimm/dxn119

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Francisella inhibits STAT1-mediated signaling in macrophages and prevents activation of antigen-specific T cells

Kimberly M. Roth¹, John S. Gunn²^,3, William Lafuse³ and Abhay R. Satoskar¹^,2^,3

¹ Department of Microbiology
² Center for Microbial Interface Biology
³ Department of Molecular Virology, Immunology and Medical Genetics, Ohio State University, Columbus, OH, USA

Correspondence to: A. R. Satoskar; E-mail: satoskar.2{at}osu.edu

Signal transducer and activator of transcription-1 (STAT1) signalingmediate most biological functions of IFN ${alpha}$ , IFNβ and IFN ${gamma}$ although recent studies indicate that IFN ${gamma}$ can alter expressionof several genes via a STAT1-independent pathway. STAT1 is criticalfor immunity against a variety of intracellular pathogens andsome studies show that pathogens evade host immunity by interferingwith STAT1 signaling. Here, we have investigated the role ofSTAT1 in host defense against pulmonary Francisella novicidainfection using STAT1–/– mice. In addition, we examinedthe effect of F. novicida on STAT1 signaling in macrophagesand on their ability to activate antigen-specific T cells. Bothwild-type (WT) and STAT1–/– BALB/c mice were susceptibleto aerosol challenge with 10³ F. novicida and displayed 100%mortality. However, STAT1–/– mice developed moresevere pneumonia, liver pathology and succumbed to infectionfaster than WT mice. The lungs, liver and hearts from F. novicida-infectedSTAT1–/– mice also contained more bacteria thanWT mice at the time of death. In vitro studies showed that F.novicida suppressed IFN ${gamma}$ R ${alpha}$ (alpha subunit of IFN ${gamma}$ receptor) andMHC class II expression, down-regulated IFN ${gamma}$ -induced STAT1 activationand reduced nuclear binding of STAT1 in RAW264.7 macrophages.Furthermore, F. novicida-infected BMDM loaded with ovalbumin(OVA) were less efficient in activating OVA-specific CD4+ Tcells in vitro. These findings demonstrate that STAT1-mediatedsignaling participates in the host defense against pulmonaryF. novicida infection but it is not sufficient to prevent mortalityassociated with this infection. Moreover, our results show thatF. novicida attenuates STAT1-mediated IFN ${gamma}$ signaling in macrophagesand impairs their ability to activate antigen-specific CD4+T cells.

Keywords: Francisella novicida, IFN ${gamma}$ , STAT1

Transmitting editor: C. Terhorst

Received 1 May 2008, accepted 4 October 2008.

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