2021
DOI: 10.3390/v13122512
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Why the HIV Reservoir Never Runs Dry: Clonal Expansion and the Characteristics of HIV-Infected Cells Challenge Strategies to Cure and Control HIV Infection

Abstract: Antiretroviral therapy (ART) effectively reduces cycles of viral replication but does not target proviral populations in cells that persist for prolonged periods and that can undergo clonal expansion. Consequently, chronic human immunodeficiency virus (HIV) infection is sustained during ART by a reservoir of long-lived latently infected cells and their progeny. This proviral landscape undergoes change over time on ART. One of the forces driving change in the landscape is the clonal expansion of infected CD4 T … Show more

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Cited by 29 publications
(17 citation statements)
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“…In addition, clonal expansion directed towards diverse antigens including CMV, flu, EBV rather than passive expansion could represent an important aspect in reservoir maintenance. Depending on efficiency of translocation, viral replication, innate immune mechanisms and CD8+CTL function, variable CD4 clonal expansion could be envisaged, with different levels of involvement of NK cells to control the renovating reservoir ( 64 ).…”
Section: Discussionmentioning
confidence: 99%
“…In addition, clonal expansion directed towards diverse antigens including CMV, flu, EBV rather than passive expansion could represent an important aspect in reservoir maintenance. Depending on efficiency of translocation, viral replication, innate immune mechanisms and CD8+CTL function, variable CD4 clonal expansion could be envisaged, with different levels of involvement of NK cells to control the renovating reservoir ( 64 ).…”
Section: Discussionmentioning
confidence: 99%
“…Such variants can integrate as proviral DNA, thus seeding the viral reservoir [5,6]. Proliferation of CD4 T-cells harbouring integrated virus, either homeostatic or as a result of antigenic stimulation, is thought to maintain the size of the HIV reservoir through many years of virologically suppressive ART [7][8][9][10]. Archived RAMs can re-emerge if virus production resumes, facilitated by lapses in adherence or treatment interruption, retaining potential clinical significance long term.…”
Section: Dynamics Of Hiv Drug Resistancementioning
confidence: 99%
“…These include the viral cytopathic effect, immune clearance, and clonal expansion of latent HIV‐1‐infected CD4+ T cells 25,26 . The precise mechanism(s) by which latent HIV‐1‐infected cell clonal expansion occurs are not completely understood, but are thought to include general immune activation, antigen driven expansion and contraction of infected CD4+ T cell clones, homeostatic proliferation, and HIV‐1 integration site‐dependent provirus‐driven clonal expansion 4,11,19,27–33 …”
Section: Introductionmentioning
confidence: 99%
“…25,26 The precise mechanism(s) by which latent HIV-1infected cell clonal expansion occurs are not completely understood, but are thought to include general immune activation, antigen driven expansion and contraction of infected CD4+ T cell clones, homeostatic proliferation, and HIV-1 integration site-dependent provirus-driven clonal expansion. 4,11,19,[27][28][29][30][31][32][33] Although ART suppresses HIV-1 replication, improves immune function, reduces comorbidities, and has led to significant improvements in both longevity and quality of life in PLWH, it does not completely reverse the significant loss in virus-specific immune functions observed in PLWH, 34 nor does it eliminate the preexisting HIV-1 reservoir. 24 Additionally, ART presents challenges such as adherence to drug regimens, the emergence of resistant viruses, and cumulative ART toxicity.…”
Section: Introductionmentioning
confidence: 99%