Ipr1 Gene Mediates Innate Immunity to Tuberculosis

Overview

Journal Nature

Specialty Science

Date 2005 Apr 9

PMID 15815631

Citations 243

Authors

Hui Pan

Bo-Shiun Yan

Mauricio Rojas

Yuriy V Shebzukhov

Hongwei Zhou

Lester Kobzik

Darren E Higgins

Mark J Daly

Barry R Bloom

Igor Kramnik

Affiliations

Soon will be listed here.

Abstract

An estimated eight million people are infected each year with the pathogen Mycobacterium tuberculosis, and more than two million die annually. Yet only about 10% of those infected develop tuberculosis. Genetic variation within host populations is known to be significant in humans and animals, but the nature of genetic control of host resistance to tuberculosis remains poorly understood. Previously we mapped a new genetic locus on mouse chromosome 1, designated sst1 (for supersusceptibility to tuberculosis 1). Here we show that this locus mediates innate immunity in sst1 congenic mouse strains and identify a candidate gene, Intracellular pathogen resistance 1 (Ipr1), within the sst1 locus. The Ipr1 gene is upregulated in the sst1 resistant macrophages after activation and infection, but it is not expressed in the sst1 susceptible macrophages. Expression of the Ipr1 transgene in the sst1 susceptible macrophages limits the multiplication not only of M. tuberculosis but also of Listeria monocytogenes and switches a cell death pathway of the infected macrophages from necrosis to apoptosis. Our data indicate that the Ipr1 gene product might have a previously undocumented function in integrating signals generated by intracellular pathogens with mechanisms controlling innate immunity, cell death and pathogenesis.

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