High frequency of memory stem cells with a distinct gene signature in HIV patients with treatment interruption

Author:

Sachdeva Meenakshi1ORCID,Sharma Aman2,Arora Sunil K.13ORCID

Affiliation:

1. Department of Translational and Regenerative medicine Post Graduate Institute of Medical Education and Research (PGIMER) Chandigarh India

2. Department of Internal Medicine Post Graduate Institute of Medical Education and Research (PGIMER) Chandigarh India

3. Department of Immunopathology Post Graduate Institute of Medical Education and Research (PGIMER) Chandigarh India

Abstract

AbstractReservoirs of HIV remain a major obstacle to the complete eradication of virus despite regular anti‐retroviral therapy (ART). Memory stem cells (Tscm), one of the major reservoirs, are relatively less studied owing to their presence in lower numbers and inaccessible anatomical locations. We have evaluated the molecular characteristics of Tscms in patients with ART interruption (n = 15) versus patients on uninterrupted ART (n = 12) using flow cytometry. RNA sequencing was done in the sorted Tscms to study the differential gene expression. Patients with ART interruption had significantly lower baseline CD4+T‐cell counts and high viral loads as compared to patients on ART. The former group had significantly higher frequency of CD4+ and CD8+Tscms with a higher expression of PD‐1 on CD8+Tscms. The transcriptome profile of Tscm was significantly different among the patient groups. The main pathways were cellular and metabolic pathways, cellular development pathways, cell differentiation and negative regulation of cellular migratory pathways. An increased yet dysfunctional CD8+ memory stem cells describe HIV‐1‐infected patients with break‐in ART and a distinct transcriptional signature of CD4+ Tscm as compared to those of patients on ART. A more detailed understanding of the biology and dynamics of Tscm in future studies is warranted. Strategies to improve the functionality of the CD8+ Tscm will help these patients to tackle the outburst of viral replication that occurs after the cessation of therapy.

Publisher

Wiley

Subject

Immunology,General Medicine

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