Literature DB >> 29396710

N-acetyl cysteine protects anti-melanoma cytotoxic T cells from exhaustion induced by rapid expansion via the downmodulation of Foxo1 in an Akt-dependent manner.

Matthew J Scheffel1, Gina Scurti2, Megan M Wyatt1, Elizabeth Garrett-Mayer3, Chrystal M Paulos1, Michael I Nishimura2, Christina Voelkel-Johnson4.   

Abstract

Therapeutic outcomes for adoptive cell transfer (ACT) therapy are constrained by the quality of the infused T cells. The rapid expansion necessary to obtain large numbers of cells results in a more terminally differentiated phenotype with decreased durability and functionality. N-acetyl cysteine (NAC) protects against activation-induced cell death (AICD) and improves anti-tumor efficacy of Pmel-1 T cells in vivo. Here, we show that these benefits of NAC can be extended to engineered T cells and significantly increases T-cell survival within the tumor microenvironment. The addition of NAC to the expansion protocol of human TIL13838I TCR-transduced T cells that are under evaluation in a Phase I clinical trial, demonstrated that findings in murine cells extend to human cells. Expansion of TIL13838I TCR-transduced T cells in NAC also increased their ability to kill target cells in vitro. Interestingly, NAC did not affect memory subsets, but diminished up-regulation of senescence (CD57) and exhaustion (PD-1) markers and significantly decreased expression of the transcription factors EOMES and Foxo1. Pharmacological inhibition of the PI3K/Akt pathway ablates the decrease in Foxo1 induced by NAC treatment of activated T cells. This suggests a model in which NAC through PI3K/Akt activation suppresses Foxo1 expression, thereby impacting its transcriptional targets EOMES, PD-1, and granzyme B. Taken together, our results indicate that NAC exerts pleiotropic effects that impact the quality of TCR-transduced T cells and suggest that the addition of NAC to current clinical protocols should be considered.

Entities:  

Keywords:  Adoptive T-cell therapy; Akt; Cell death; Foxo1; N-acetyl-cysteine; PD1

Mesh:

Substances:

Year:  2018        PMID: 29396710      PMCID: PMC5862784          DOI: 10.1007/s00262-018-2120-5

Source DB:  PubMed          Journal:  Cancer Immunol Immunother        ISSN: 0340-7004            Impact factor:   6.968


  48 in total

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Authors:  Matthew J Scheffel; Gina Scurti; Patricia Simms; Elizabeth Garrett-Mayer; Shikhar Mehrotra; Michael I Nishimura; Christina Voelkel-Johnson
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10.  Clinical and immunologic evaluation of three metastatic melanoma patients treated with autologous melanoma-reactive TCR-transduced T cells.

Authors:  Tamson Moore; Courtney Regan Wagner; Gina M Scurti; Kelli A Hutchens; Constantine Godellas; Ann Lau Clark; Elizabeth Motunrayo Kolawole; Lance M Hellman; Nishant K Singh; Fernando A Huyke; Siao-Yi Wang; Kelly M Calabrese; Heather D Embree; Rimas Orentas; Keisuke Shirai; Emilia Dellacecca; Elizabeth Garrett-Mayer; Mingli Li; Jonathan M Eby; Patrick J Stiff; Brian D Evavold; Brian M Baker; I Caroline Le Poole; Boro Dropulic; Joseph I Clark; Michael I Nishimura
Journal:  Cancer Immunol Immunother       Date:  2017-10-20       Impact factor: 6.968

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6.  N-Acetylcysteine: A potential therapeutic agent for SARS-CoV-2.

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Review 9.  Oxidative Stress in the Tumor Microenvironment and Its Relevance to Cancer Immunotherapy.

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10.  Repurposing the antioxidant and anti-inflammatory agent N-acetyl cysteine for treating COVID-19.

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