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Beyond CTLA-4 and PD-1: Orphan nuclear receptor NR2F6 as T-cell s | 32486

Immunotherapy: Open Access

ISSN - 2471-9552

Beyond CTLA-4 and PD-1: Orphan nuclear receptor NR2F6 as T-cell signaling switch and emerging target in cancer immunotherapy

International Conference on Tumor & Cancer Immunology and Immunotherapy

July 28-30, 2016 Melbourne, Australia

Victoria Klepsch

Medical University Innsbruck, Austria

Scientific Tracks Abstracts: Immunother Open Acc

Abstract :

Modulation of the immune system for the treatment of primary and metastatic tumors in cancer patients has been a goal for many decades. Very recently, blockade of immune checkpoints CTLA-4 and PD-1 has emerged as promising cancer immune therapies. Even though encouraging, there is an unmet medical need as still only a very limited number of patients respond to and are potentially cured by these therapies. In contrast to cell surface checkpoints, there are cancer therapeutic targets that are located inside the immune cells and are amenable to pharmacological modulation. Based on our published and unpublished findings that genetically NR2F6-deficient mice are able to immunologically reject otherwise lethal tumor burdens; we have identified and preclinically validated the orphan nuclear receptor NR2F6 (nuclear receptor subfamily 2, group F, member 6; alias Ear2 and COUPTFIII) as a bona fide immune checkpoint. We could show that genetic ablation of NR2F6 significantly improves survival in the murine transgenic TRAMP prostate cancer model. Furthermore, NR2F6-/- mice spontaneously reject implanted tumors and develop host-protective immunological memory against tumor re-challenge. This is paralleled by increased frequencies of both CD4+ and CD8+ T-cells and higher expression levels of interleukin-2 and interferon-�³ at the tumor site. This defines NR2F6 as an intracellular and potentially also druggable immune checkpoint, where the presence of NR2F6 limits effector T-cell activation within the tumor microenvironment governing the amplitude of anti-cancer immunity, representing a promising avenue for development of alternative immune checkpoint inhibition treatment regimens.

Biography :

Victoria Klepsch has received her PhD degree from the Medical University Innsbruck. She is a Postdoctoral Fellow at the Medical University Innsbruck in Gottfried Baier’s Lab. She has published 3 papers in well-reputed journals and has been working on NR2F6 and tumor immunology since 4 years continuing investigating in depth in this nuclear receptor NR2F6 in T-cell biology and cancer immunity.

Email: victoria.klepsch@i-med.ac.at

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