Daniel Bunis scite author profile

SUMMARY Targeted HIV cure strategies require definition of the mechanisms that maintain the virus. Here, we tracked HIV replication and the persistence of infected CD4 T cells in individuals with natural virologic control by sequencing viruses, T cell receptor genes, HIV integration sites and cellular transcriptomes. Our results revealed three mechanisms of HIV persistence operating within distinct anatomic and functional compartments. In lymph node, we detected viruses with genetic and transcriptional attributes of active replication in both T follicular helper (TFH) cells and non-TFH memory cells. In blood, we detected inducible proviruses of archival origin among highly differentiated, clonally expanded cells. Linking the lymph node and blood was a small population of circulating cells harboring inducible proviruses of recent origin. Thus, HIV replication in lymphoid tissue, clonal expansion of infected cells, and recirculation of recently infected cells act together to maintain the virus in HIV controllers despite effective antiviral immunity.

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dittoSeq: universal user-friendly single-cell and bulk RNA sequencing visualization toolkit

Bunis

Andrews

Fragiadakis³

et al. 2020

149

114

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Summary A visualization suite for major forms of bulk and single-cell RNAseq data in R. dittoSeq is color blindness-friendly by default, robustly documented to power ease-of-use and allows highly customizable generation of both daily-use and publication-quality figures. Availability and implementation dittoSeq is an R package available through Bioconductor via an open source MIT license. Supplementary information Supplementary data are available at Bioinformatics online.

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Single-Cell Mapping of Progressive Fetal-to-Adult Transition in Human Naive T Cells

et al. 2021

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Daniel Bunis

Multiple Origins of Virus Persistence during Natural Control of HIV Infection

dittoSeq: universal user-friendly single-cell and bulk RNA sequencing visualization toolkit

Single-Cell Mapping of Progressive Fetal-to-Adult Transition in Human Naive T Cells

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