Insight in miRNome of Long-Term Non-Progressors and Elite Controllers Exposes Potential RNAi Role in Restraining HIV-1 Infection

Ayala-Suárez, Rubén; Díez-Fuertes, Francisco; Calonge, Esther; Tarazona, Humberto Erick De La Torre; Alda, M Gracia-Ruiz de; Capa, Laura; Alcamı́, José

doi:10.3390/jcm9082452

Cited by 11 publications

(9 citation statements)

References 89 publications

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“…Several studies have shown that PBMCs from ECs have a miRNA repertoire that is distinct from that of HIV-1 ART-naïve progressors, and such a difference may in part explain the control of viral infection in ECs ( Witwer et al., 2012 ; Reynoso et al., 2014 ; Ayala-Suárez et al., 2020 ). In this context, we assessed the levels of miRNA-103 and CCR5 mRNA in CD4 + T cells from ECs and ART-naïve progressors and found that CCR5 mRNA in CD4 + T cells obtained from ECs was significantly decreased when compared to that in CD4 + T cells from ART-naïve progressors, in line with recently published results ( Claireaux et al., 2022 ; Gonzalo-Gil et al., 2019 ; Meijerink et al., 2014 ).…”

Section: Discussionmentioning

confidence: 99%

“…Previous meta-analyses of genetic studies showed a genome-wide significant association between the CCR5 locus and viral load, highlighting the impact of CCR5 expression limitation on HIV-1 replication and control ( McLaren et al., 2015 ). Indeed, it has been shown that PBMCs from ART-naïve progressors may have less total miRNAs than cells from ECs ( Ayala-Suárez et al., 2020 ). As well, viral infection can have an impact on miRNA expression ( Bennasser et al., 2005 ; Triboulet et al., 2007 ) as viral proteins such as Tat and Vpr have been reported to act as RNA silencing suppressors ( Casey Klockow et al., 2013 ; Cojo et al., 2017 ).…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

MiRNA-103 downmodulates CCR5 expression reducing human immunodeficiency virus type-1 entry and impacting latency establishment in CD4+ T cells

Bellini¹,

Lodge²,

Pham³

et al. 2022

iScience

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

MiRNA-103 downmodulates CCR5 expression reducing human immunodeficiency virus type-1 entry and impacting latency establishment in CD4+ T cells

Bellini¹,

Lodge²,

Pham³

et al. 2022

iScience

View full text Add to dashboard Cite

“…Another interesting strategy consists of restoring the killing capacity of cells by miRNA modulation. Therefore, the involvement of miRNAs in CD8 + T cells cytotoxicity has also been investigated (29)(30)(31)(32)(33)(34)(35). However, to our knowledge, no attempts have been made to restore the killing capacity of cells by miRNA modulation.…”

Section: Discussionmentioning

confidence: 99%

Selective miRNA inhibition in CD8+ cytotoxic T lymphocytes enhances HIV-1 specific cytotoxic responses

et al. 2022

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miRNAs dictate relevant virus-host interactions, offering new avenues for interventions to achieve an HIV remission. We aimed to enhance HIV-specific cytotoxic responses—a hallmark of natural HIV control— by miRNA modulation in T cells. We recruited 12 participants six elite controllers and six patients with chronic HIV infection on long-term antiretroviral therapy ("progressors"). Elite controllers exhibited stronger HIV-specific cytotoxic responses than the progressors, and their CD8+T cells showed a miRNA (hsa-miR-10a-5p) significantly downregulated. When we transfected ex vivo CD8+ T cells from progressors with a synthetic miR-10a-5p inhibitor, miR-10a-5p levels decreased in 4 out of 6 progressors, correlating with an increase in HIV-specific cytotoxic responses. The effects of miR-10a-5p inhibition on HIV-specific CTL responses were modest, short-lived, and occurred before day seven after modulation. IL-4 and TNF-α levels strongly correlated with HIV-specific cytotoxic capacity. Thus, inhibition of miR-10a-5p enhanced HIV-specific CD8+ T cell capacity in progressors. Our pilot study proves the concept that miRNA modulation is a feasible strategy to combat HIV persistence by enhancing specific cytotoxic immune responses, which will inform new approaches for achieving an antiretroviral therapy-free HIV remission.

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“…Additionally, it is debated that whether host RNA interference (RNAi) contributes to immune responses against HIV-1. Nevertheless, several miRNAs are differentially regulated in HIV-1 elite controllers as compared to typical progressor patients, suggesting that HIV-1 interferes with host RNAi ( 95 ). HIV-1 manipulates host RNAi mechanisms through its RNA elements such as RRE (Rev Response Element) and TAR (Trans Activation Response) as well as Rev and Tat proteins.…”

Section: Discussionmentioning

confidence: 99%

Dodging the Host Interferon-Stimulated Gene Mediated Innate Immunity by HIV-1: A Brief Update on Intrinsic Mechanisms and Counter-Mechanisms

2021

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Host restriction factors affect different phases of a viral life cycle, contributing to innate immunity as the first line of defense against viruses, including HIV-1. These restriction factors are constitutively expressed, but triggered upon infection by interferons. Both pre-integration and post-integration events of the HIV-1 life cycle appear to play distinct roles in the induction of interferon-stimulated genes (ISGs), many of which encode antiviral restriction factors. However, HIV-1 counteracts the mechanisms mediated by these restriction factors through its encoded components. Here, we review the recent findings of pathways that lead to the induction of ISGs, and the mechanisms employed by the restriction factors such as IFITMs, APOBEC3s, MX2, and ISG15 in preventing HIV-1 replication. We also reflect on the current understanding of the counter-mechanisms employed by HIV-1 to evade innate immune responses and overcome host restriction factors. Overall, this mini-review provides recent insights into the HIV-1-host cross talk bridging the understanding between intracellular immunity and research avenues in the field of therapeutic interventions against HIV-1.

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Insight in miRNome of Long-Term Non-Progressors and Elite Controllers Exposes Potential RNAi Role in Restraining HIV-1 Infection

Cited by 11 publications

References 89 publications

MiRNA-103 downmodulates CCR5 expression reducing human immunodeficiency virus type-1 entry and impacting latency establishment in CD4+ T cells

MiRNA-103 downmodulates CCR5 expression reducing human immunodeficiency virus type-1 entry and impacting latency establishment in CD4+ T cells

Selective miRNA inhibition in CD8+ cytotoxic T lymphocytes enhances HIV-1 specific cytotoxic responses

Dodging the Host Interferon-Stimulated Gene Mediated Innate Immunity by HIV-1: A Brief Update on Intrinsic Mechanisms and Counter-Mechanisms

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