Nataliya Prokhnevska scite author profile

In response to viral infection, CD8+ T cells undergo expansion and differentiate into distinct classes of effector cells. After clearance of the virus, a small population of long-lived memory cells persists. Comprehensive studies have defined the protein-coding transcriptional changes associated with this process. Here we expand on this prior work by performing RNA-sequencing to identify changes in long noncoding RNA (lncRNA) expression in human and mouse CD8+ T cells responding to viral infection. We identify hundreds of unannotated lncRNAs and show that expression profiles of both known and novel lncRNAs are sufficient to define naive, effector, and memory CD8+ T cell subsets, implying that they may be involved in fate decisions during antigen-driven differentiation. Additionally, in comparing mouse and human lncRNA expression, we find that lncRNAs with conserved sequence undergo similar changes in expression in the two species, suggesting an evolutionarily conserved role for lncRNAs during CD8+ T cell differentiation.

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The requirement for immune infiltration and organization in the tumor microenvironment for successful immunotherapy in prostate cancer

Jansen

Prokhnevska

2019

Urologic Oncology: Seminars and Original Investigations

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Nataliya Prokhnevska

An intra-tumoral niche maintains and differentiates stem-like CD8 T cells

Functional HPV-specific PD-1+ stem-like CD8 T cells in head and neck cancer

CD8+ T cell activation in cancer comprises an initial activation phase in lymph nodes followed by effector differentiation within the tumor

Expression of novel long noncoding RNAs defines virus-specific effector and memory CD8+ T cells

The requirement for immune infiltration and organization in the tumor microenvironment for successful immunotherapy in prostate cancer

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