Downregulation of <i>MALAT1</i> is a hallmark of tissue and peripheral proliferative T cells in COVID-19

Dey, Shoumit; Ashwin, Helen; Milross, Luke; Hunter, Bethany; Majó, Joaquim; Filby, Andrew; Fisher, Andrew J.; Kaye, Paul M.; Lagos, Dimitrios

doi:10.1093/cei/uxad034

Cited by 6 publications

(4 citation statements)

References 76 publications

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“…The effect of Malat1 on myeloid cell populations in the TME in vivo led us to investigate T-cell infiltration and function within the immune landscape because the T-cell response is paramount for the efficacy of immunomodulation therapies. A recent study in COVID-19 patients found that decreased Malat1 expression in T cells was linked to increased proliferative capabilities ( 54 ). However, there is little known about the effect Malat1 inhibition has on T-cell infiltration and function in cancer.…”

Section: Discussionmentioning

confidence: 99%

Targeted Inhibition of lncRNA Malat1 Alters the Tumor Immune Microenvironment in Preclinical Syngeneic Mouse Models of Triple-Negative Breast Cancer

Adewunmi,

Shen,

Zhang

et al. 2023

Cancer Immunology Research

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Long non-coding RNAs (lncRNA) play an important role in gene regulation in both normal tissues and cancer. Targeting lncRNAs is a promising therapeutic approach that has become feasible through the development of gapmer antisense oligonucleotides (ASOs). Metastasis-associated lung adenocarcinoma transcript (Malat1) is an abundant lncRNA whose expression is upregulated in several cancers. While Malat1 increases the migratory and invasive properties of tumor cells, its role in the tumor microenvironment (TME) is still not well defined. We explored the connection between Malat1 and the tumor immune microenvironment (TIME) using several immune competent preclinical syngeneic Tp53-null triple-negative breast cancer (TNBC) mouse models that mimic the heterogeneity and immunosuppressive TME found in human breast cancer. Using a Malat1 ASO we were able to knockdown Malat1 RNA expression resulting in a delay in primary tumor growth, decreased proliferation and increased apoptosis. Additionally, immunophenotyping of tumor-infiltrating lymphocytes (TILs) revealed that Malat1 inhibition altered the TIME, with a decrease in immunosuppressive tumor-associated macrophages (TAMs) and myeloid-derived suppressor cells (MDSCs) as well as an increase in cytotoxic CD8+ T cells. Malat1 depletion in tumor cells, TAMs, and MDSCs decreased immunosuppressive cytokine/chemokine secretion while Malat1 inhibition in T cells increased inflammatory secretions and T-cell proliferation. Combination of a Malat1 ASO with chemotherapy or immune checkpoint blockade (ICB) improved the treatment responses in a preclinical model. These studies highlight the immunostimulatory effects of Malat1 inhibition in TNBC, the benefit of a Malat1 ASO therapeutic, and its potential use in combination with chemotherapies and immunotherapies.

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Section: Discussionmentioning

confidence: 99%

Targeted Inhibition of lncRNA Malat1 Alters the Tumor Immune Microenvironment in Preclinical Syngeneic Mouse Models of Triple-Negative Breast Cancer

Adewunmi,

Shen,

Zhang

et al. 2023

Cancer Immunology Research

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“…Next, we identi ed three effector Treg clusters among CCR7 low cells expressing HLA-A, CD74, and IL32, respectively. An additional Treg cluster was de ned by high MALAT1 expression, which is associated with the cell cycle phase and Treg proliferation 29,30 . Lastly, we identi ed a subset of Tregs expressing Humanin genes MTRNRL28 and MTRNRL12.…”

Section: Single-cell Rna-seq Identi Es Treg Subsets In Gdm and Health...mentioning

confidence: 99%

Single-cell transcriptomics reveals markers of regulatory T cell dysfunction in Gestational Diabetes Mellitus

Shangaris,

Mensah,

Efthimiou

et al. 2024

Preprint

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Gestational diabetes mellitus (GDM) is a common pregnancy complication associated with hyperglycaemia, chronic inflammation and adverse health outcomes. Regulatory T cells (Tregs) are thought to contribute to GDM due to their role in suppressing inflammation. However, it remains unclear whether specific Treg subsets are impaired in patients with GDM. To investigate transcriptional variation in GDM Tregs, we applied single-cell RNA sequencing to Tregs isolated from the blood of 13 healthy pregnant women and 10 patients with GDM. We identified naive and effector Treg subsets, none of which significantly differ in the proportion of cells captured from GDM and controls. We report a naive Treg subset with reduced expression of AP-1 transcription factor subunits in GDM, including JUN, FOS, and EGR1, and an effector Treg subset with increased signalling of angiogenesis marker genes. Genes dysregulated in GDM Tregs independently predicted GDM status in pseudobulk and whole blood mRNA from independent cohorts. Remarkably, TXNIP, which regulates glucose levels, emerged as the most reliable standalone predictor in bulk mRNA (minimum AUC 0.7) equivalent to using body mass index (AUC 0.72) in our cohort. This study uncovers a disrupted molecular pathway in Treg cell subsets from GDM patients and proposes a panel of genes with translational potential as early disease biomarkers.

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“…This cluster has been previously reported and suggested to include cells which are poised to rapidly respond to secondary infections by producing cytokines 42,43 . Quiescent memory cells were slightly more prevalent within NT and characterized by the expression of several long non-coding RNAs (including Malat1) 44,45 and low ribosomal gene expression. A small proportion of our CD4 TRM was naïve-like T cells expressing Ccr7, Sell and Klf2 46 .…”

Section: Cd4 Trm In the Lungs And Nt Are Heterogeneous But Th17 Cells...mentioning

confidence: 99%

Nasal tissue-resident memory CD4⁺T cells persist after influenza A virus infection and provide heterosubtypic protection

Mathew,

Gailleton,

Scharf

et al. 2024

Preprint

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CD4 tissue-resident memory T (CD4 TRM) cells are crucial adaptive immune components involved in preventing influenza A virus (IAV) infection. Despite their importance, their physiological role in the upper respiratory tract, the first site of contact with IAV, remains unclear. Here, we find that, after IAV infection, antigen-specific CD4 TRM persist in the nasal tissue (NT) compartment and play a prime role in local viral clearance. Single cell RNA sequencing analysis reveals that NT CD4 TRM are heterogeneous and transcriptionally distinct as compared to their lung counterparts. Mechanistically, we demonstrate that the CXCR6- CXCL16 axis is involved in CD4 TRM residency in the NT. Furthermore, we show that the NT of mice and humans contains a high frequency of IL-17-producing CD4 TRM that aid in local viral clearance and in reducing tissue damage. Collectively, our results support a robust physiological role for nasal tissue CD4 TRM in preventing IAV infection.

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Downregulation of MALAT1 is a hallmark of tissue and peripheral proliferative T cells in COVID-19

Cited by 6 publications

References 76 publications

Targeted Inhibition of lncRNA Malat1 Alters the Tumor Immune Microenvironment in Preclinical Syngeneic Mouse Models of Triple-Negative Breast Cancer

Targeted Inhibition of lncRNA Malat1 Alters the Tumor Immune Microenvironment in Preclinical Syngeneic Mouse Models of Triple-Negative Breast Cancer

Single-cell transcriptomics reveals markers of regulatory T cell dysfunction in Gestational Diabetes Mellitus

Nasal tissue-resident memory CD4⁺T cells persist after influenza A virus infection and provide heterosubtypic protection

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Downregulation of MALAT1 is a hallmark of tissue and peripheral proliferative T cells in COVID-19

Cited by 6 publications

References 76 publications

Targeted Inhibition of lncRNA Malat1 Alters the Tumor Immune Microenvironment in Preclinical Syngeneic Mouse Models of Triple-Negative Breast Cancer

Targeted Inhibition of lncRNA Malat1 Alters the Tumor Immune Microenvironment in Preclinical Syngeneic Mouse Models of Triple-Negative Breast Cancer

Single-cell transcriptomics reveals markers of regulatory T cell dysfunction in Gestational Diabetes Mellitus

Nasal tissue-resident memory CD4+T cells persist after influenza A virus infection and provide heterosubtypic protection

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Nasal tissue-resident memory CD4⁺T cells persist after influenza A virus infection and provide heterosubtypic protection