Cell
Volume 140, Issue 5, 5 March 2010, Pages 731-743
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Genome-wide Analysis of the Host Intracellular Network that Regulates Survival of Mycobacterium tuberculosis

https://doi.org/10.1016/j.cell.2010.02.012Get rights and content
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Summary

We performed a genome-wide siRNA screen to identify host factors that regulated pathogen load in human macrophages infected with a virulent strain of Mycobacterium tuberculosis. Iterative rounds of confirmation, followed by validation, identified 275 such molecules that were all found to functionally associate with each other through a dense network of interactions. This network then yielded to a molecular description of the host cell functional modules that were both engaged and perturbed by the pathogen. Importantly, a subscreen against a panel of field isolates revealed that the molecular composition of the host interface varied with both genotype and the phenotypic properties of the pathogen. An analysis of these differences, however, permitted identification of those host factors that were invariantly involved, regardless of the diversification in adaptive mechanisms employed by the pathogen. Interestingly, these factors were found to predominantly function through the regulation of autophagy.

Highlights

► A genome-wide siRNA screen identified host factors regulating M. tuberculosis infection ► These factors define various functional modules of the host human macrophage ► A core set of regulatory factors were identified with a panel of Mtb field isolates ► These core host cell factors predominantly function in the regulation of autophagy

HUMDISEASE
MICROBIO
SYSBIO

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