| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2035152 | Cell | 2015 | 12 Pages |
•HIV expression persists even when primary cells transition from activated to resting•Tat positive-feedback circuitry drives this autonomy from cell-state relaxation•Orthogonal activation of Tat shows that the circuitry suffices for autonomous latency
SummaryBiological circuits can be controlled by two general schemes: environmental sensing or autonomous programs. For viruses such as HIV, the prevailing hypothesis is that latent infection is controlled by cellular state (i.e., environment), with latency simply an epiphenomenon of infected cells transitioning from an activated to resting state. However, we find that HIV expression persists despite the activated-to-resting cellular transition. Mathematical modeling indicates that HIV’s Tat positive-feedback circuitry enables this persistence and strongly controls latency. To overcome the inherent crosstalk between viral circuitry and cellular activation and to directly test this hypothesis, we synthetically decouple viral dependence on cellular environment from viral transcription. These circuits enable control of viral transcription without cellular activation and show that Tat feedback is sufficient to regulate latency independent of cellular activation. Overall, synthetic reconstruction demonstrates that a largely autonomous, viral-encoded program underlies HIV latency—potentially explaining why cell-targeted latency-reversing agents exhibit incomplete penetrance.
Graphical AbstractFigure optionsDownload full-size imageDownload high-quality image (228 K)Download as PowerPoint slide
