BACH2 promotes seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells

Hongbo Gao; Yuhao Li; Ritudwhaj Tiwari; Marilia Pinzone; Xiwen Qin; Kolin M. Clark; Sara K. Nicholson; Tony Yao; Kelly Rome; Michael Scaglione; Will Bailis; Rachel M. Presti; Irini Sereti; Naresha Saligrama; Leyao Wang; Liang Shan

doi:10.1016/j.xcrm.2025.102311

BACH2 promotes seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells

Hongbo Gao
, Yuhao Li
, Ritudwhaj Tiwari
, Marilia Pinzone
, Xiwen Qin
, Kolin M. Clark
, Sara K. Nicholson
, Tony Yao
, Kelly Rome
, Michael Scaglione
, Will Bailis
, Rachel M. Presti
, Irini Sereti
, Naresha Saligrama
, Leyao Wang
, Liang Shan^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Despite antiretroviral therapy, HIV-1 mainly persists in memory CD4+ T cells in people living with HIV-1. Most long-lived viral reservoir cells are infected by the virus near the time of therapy initiation. A better understanding of the early events in viral reservoir seeding presents opportunities for preventing latent reservoir formation. Here, we demonstrate that CD4+ T cells expressing CCR5, permissive to HIV-1 infection, are effector or terminally differentiated cells. BTB domain and CNC homolog 2 (BACH2) is expressed by a small subset of CCR5+ cells and reverses their terminal differentiation. BACH2-mediated memory differentiation is impeded due to heightened inflammation before treatment initiation. Mice with a BACH2-knockout human immune system have a reduced frequency of HIV-1 reservoir cells and do not experience virus rebound after treatment discontinuation. Our study reveals that BACH2 is essential to the seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells.

Original language	English
Article number	102311
Journal	Cell Rep. Med.
Volume	6
Issue number	9
Early online date	2025
DOIs	https://doi.org/10.1016/j.xcrm.2025.102311
Publication status	Published - 16 Sept 2025

Keywords

ART
BACH2
CCR5
CD4 T cells
HIV-1
humanized mice
memory differentiation
terminal differentiation
viral reservoirs

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.xcrm.2025.102311

Bach2-promotes-seeding-and-establishment-of-long-lived-hiv-1-reservoir-in-memory-cd4-t-cells.pdfFinal published version, 8.8 MBLicence: CC BY

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Gao, H., Li, Y., Tiwari, R., Pinzone, M., Qin, X., Clark, K. M., Nicholson, S. K., Yao, T., Rome, K., Scaglione, M., Bailis, W., Presti, R. M., Sereti, I., Saligrama, N., Wang, L., & Shan, L. (2025). BACH2 promotes seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells. Cell Rep. Med., 6(9), Article 102311. https://doi.org/10.1016/j.xcrm.2025.102311

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title = "BACH2 promotes seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells",

abstract = "Despite antiretroviral therapy, HIV-1 mainly persists in memory CD4+ T cells in people living with HIV-1. Most long-lived viral reservoir cells are infected by the virus near the time of therapy initiation. A better understanding of the early events in viral reservoir seeding presents opportunities for preventing latent reservoir formation. Here, we demonstrate that CD4+ T cells expressing CCR5, permissive to HIV-1 infection, are effector or terminally differentiated cells. BTB domain and CNC homolog 2 (BACH2) is expressed by a small subset of CCR5+ cells and reverses their terminal differentiation. BACH2-mediated memory differentiation is impeded due to heightened inflammation before treatment initiation. Mice with a BACH2-knockout human immune system have a reduced frequency of HIV-1 reservoir cells and do not experience virus rebound after treatment discontinuation. Our study reveals that BACH2 is essential to the seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells.",

keywords = "ART, BACH2, CCR5, CD4 T cells, HIV-1, humanized mice, memory differentiation, terminal differentiation, viral reservoirs",

author = "Hongbo Gao and Yuhao Li and Ritudwhaj Tiwari and Marilia Pinzone and Xiwen Qin and Clark, \{Kolin M.\} and Nicholson, \{Sara K.\} and Tony Yao and Kelly Rome and Michael Scaglione and Will Bailis and Presti, \{Rachel M.\} and Irini Sereti and Naresha Saligrama and Leyao Wang and Liang Shan",

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doi = "10.1016/j.xcrm.2025.102311",

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T1 - BACH2 promotes seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells

AU - Gao, Hongbo

AU - Li, Yuhao

AU - Tiwari, Ritudwhaj

AU - Pinzone, Marilia

AU - Qin, Xiwen

AU - Clark, Kolin M.

AU - Nicholson, Sara K.

AU - Yao, Tony

AU - Rome, Kelly

AU - Scaglione, Michael

AU - Bailis, Will

AU - Presti, Rachel M.

AU - Sereti, Irini

AU - Saligrama, Naresha

AU - Wang, Leyao

AU - Shan, Liang

PY - 2025/9/16

Y1 - 2025/9/16

N2 - Despite antiretroviral therapy, HIV-1 mainly persists in memory CD4+ T cells in people living with HIV-1. Most long-lived viral reservoir cells are infected by the virus near the time of therapy initiation. A better understanding of the early events in viral reservoir seeding presents opportunities for preventing latent reservoir formation. Here, we demonstrate that CD4+ T cells expressing CCR5, permissive to HIV-1 infection, are effector or terminally differentiated cells. BTB domain and CNC homolog 2 (BACH2) is expressed by a small subset of CCR5+ cells and reverses their terminal differentiation. BACH2-mediated memory differentiation is impeded due to heightened inflammation before treatment initiation. Mice with a BACH2-knockout human immune system have a reduced frequency of HIV-1 reservoir cells and do not experience virus rebound after treatment discontinuation. Our study reveals that BACH2 is essential to the seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells.

AB - Despite antiretroviral therapy, HIV-1 mainly persists in memory CD4+ T cells in people living with HIV-1. Most long-lived viral reservoir cells are infected by the virus near the time of therapy initiation. A better understanding of the early events in viral reservoir seeding presents opportunities for preventing latent reservoir formation. Here, we demonstrate that CD4+ T cells expressing CCR5, permissive to HIV-1 infection, are effector or terminally differentiated cells. BTB domain and CNC homolog 2 (BACH2) is expressed by a small subset of CCR5+ cells and reverses their terminal differentiation. BACH2-mediated memory differentiation is impeded due to heightened inflammation before treatment initiation. Mice with a BACH2-knockout human immune system have a reduced frequency of HIV-1 reservoir cells and do not experience virus rebound after treatment discontinuation. Our study reveals that BACH2 is essential to the seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells.

KW - ART

KW - BACH2

KW - CCR5

KW - CD4 T cells

KW - HIV-1

KW - humanized mice

KW - memory differentiation

KW - terminal differentiation

KW - viral reservoirs

UR - https://www.scopus.com/pages/publications/105014120831

U2 - 10.1016/j.xcrm.2025.102311

DO - 10.1016/j.xcrm.2025.102311

M3 - Article

C2 - 40845840

SN - 2666-3791

VL - 6

JO - Cell Rep. Med.

JF - Cell Rep. Med.

IS - 9

M1 - 102311

ER -

BACH2 promotes seeding and establishment of long-lived HIV-1 reservoir in memory CD4+ T cells

Abstract

Keywords

UN SDGs

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