Katz scite author profile

Antitumor T cells are subject to multiple mechanisms of negative regulation1–3. Recent findings that innate lymphoid cells (ILCs) regulate adaptive T cell responses4–6 led us to examine the regulatory potential of ILCs in the context of cancer. We identified a unique ILC population that inhibits tumor-infiltrating lymphocytes (TILs) from high-grade serous tumors, defined their suppressive capacity in vitro, and performed a comprehensive analysis of their phenotype. Notably, the presence of this CD56+CD3− population in TIL cultures was associated with reduced T cell numbers, and further functional studies demonstrated that this population suppressed TIL expansion and altered TIL cytokine production. Transcriptome analysis and phenotypic characterization determined that regulatory CD56+CD3− cells exhibit low cytotoxic activity, produce IL-22, and have an expression profile that overlaps with those of natural killer (NK) cells and other ILCs. NKp46 was highly expressed by these cells, and addition of anti-NKp46 antibodies to TIL cultures abrogated the ability of these regulatory ILCs to suppress T cell expansion. Notably, the presence of these regulatory ILCs in TIL cultures corresponded with a striking reduction in the time to disease recurrence. These studies demonstrate that a previously uncharacterized ILC population regulates the activity and expansion of tumor-associated T cells.

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Wide area cluster monitoring with Ganglia

Sacerdoti

Katz

Massie

et al. 2003

119

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Indoor survey of moulds and prevalence of mould atopy in Israel

Katz

Verleger

Barr

et al. 1999

Clin Experimental Allergy

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Katz

Gastro‐oesophageal reflux associated with nocturnal gastric acid breakthrough on proton pump inhibitors

A distinct innate lymphoid cell population regulates tumor-associated T cells

Wide area cluster monitoring with Ganglia

Indoor survey of moulds and prevalence of mould atopy in Israel

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