Automated Genome-Wide Visual Profiling of Cellular Proteins Involved in HIV Infection

Author:

Genovesio Auguste1,Kwon Yong-Jun12,Windisch Marc P.1,Kim Nam Youl1,Choi Seo Yeon1,Kim Hi Chul1,Jung Sungyong1,Mammano Fabrizio3,Perrin Virginie3,Boese Annette S.1,Casartelli Nicoletta3,Schwartz Olivier3,Nehrbass Ulf1,Emans Neil1

Affiliation:

1. Institut Pasteur-Korea, Gyeonggi-do, Korea

2. Department of Biochemistry, College of Science, Yonsei University, Seoul, South Korea

3. Institut Pasteur, Paris, France

Abstract

Recent genome-wide RNAi screens have identified >842 human genes that affect the human immunodeficiency virus (HIV) cycle. The list of genes implicated in infection differs between screens, and there is minimal overlap. A reason for this variance is the interdependence of HIV infection and host cell function, producing a multitude of indirect or pleiotropic cellular effects affecting the viral infection during RNAi screening. To overcome this, the authors devised a 15-dimensional phenotypic profile to define the viral infection block induced by CD4 silencing in HeLa cells. They demonstrate that this phenotypic profile excludes nonspecific, RNAi-based side effects and viral replication defects mediated by silencing of housekeeping genes. To achieve statistical robustness, the authors used automatically annotated RNAi arrays for seven independent genome-wide RNAi screens. This identified 56 host genes, which reliably reproduced CD4-like phenotypes upon HIV infection. The factors include 11 known HIV interactors and 45 factors previously not associated with HIV infection. As proof of concept, the authors confirmed that silencing of PAK1, Ku70, and RNAseH2A impaired HIV replication in Jurkat cells. In summary, multidimensional, visual profiling can identify genes required for HIV infection.

Publisher

Elsevier BV

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