Literature DB >> 25164014

Promoting thiol expression increases the durability of antitumor T-cell functions.

Pravin Kesarwani1, Amir A Al-Khami1, Gina Scurti2, Krishnamurthy Thyagarajan1, Navtej Kaur1, Shahid Husain3, Quan Fang1, Osama S Naga1, Patricia Simms2, Gyda Beeson4, Christina Voelkel-Johnson5, Elizabeth Garrett-Mayer6, Craig C Beeson4, Michael I Nishimura2, Shikhar Mehrotra1.   

Abstract

Ex vivo-expanded CD8(+) T cells used for adoptive immunotherapy generally acquire an effector memory-like phenotype (TEM cells). With regard to therapeutic applications, two undesired features of this phenotype in vivo are limited persistence and reduced antitumor efficacy, relative to CD8(+) T cells with a central memory-like phenotype (TCM cells). Furthermore, there is incomplete knowledge about all the differences between TEM and TCM cells that may influence tumor treatment outcomes. Given that TCM cells survive relatively longer in oxidative tumor microenvironments, we investigated the hypothesis that TCM cells possess relatively greater antioxidative capacity than TEM cells. Here, we report that TCM cells exhibit a relative increase compared with TEM cells in the expression of cell surface thiols, a key target of cellular redox controls, along with other antioxidant molecules. Increased expression of redox regulators in TCM cells inversely correlated with the generation of reactive oxygen and nitrogen species, proliferative capacity, and glycolytic enzyme levels. Notably, T-cell receptor-transduced T cells pretreated with thiol donors, such as N-acetyl cysteine or rapamycin, upregulated thiol levels and antioxidant genes. A comparison of antitumor CD8(+) T-cell populations on the basis of surface thiol expression showed that thiol-high cells persisted longer in vivo and exerted superior tumor control. Our results suggest that higher levels of reduced cell surface thiols are a key characteristic of T cells that can control tumor growth and that profiling this biomarker may have benefits to adoptive T-cell immunotherapy protocols. ©2014 American Association for Cancer Research.

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Year:  2014        PMID: 25164014      PMCID: PMC4216764          DOI: 10.1158/0008-5472.CAN-14-1084

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  49 in total

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3.  Thiols and the immune system: effect of N-acetylcysteine on T cell system in human subjects.

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Journal:  Methods Enzymol       Date:  1995       Impact factor: 1.600

4.  Mammalian target of rapamycin up-regulation of pyruvate kinase isoenzyme type M2 is critical for aerobic glycolysis and tumor growth.

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Journal:  Proc Natl Acad Sci U S A       Date:  2011-02-15       Impact factor: 11.205

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6.  Lymphocyte surface thiol levels.

Authors:  Bita Sahaf; Kartoosh Heydari; Leonard A Herzenberg; Leonore A Herzenberg
Journal:  Proc Natl Acad Sci U S A       Date:  2003-03-17       Impact factor: 11.205

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  19 in total

1.  Anti-oxidant capacity and anti-tumor T cell function: A direct correlation.

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2.  Thioredoxin-1 improves the immunometabolic phenotype of antitumor T cells.

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3.  Efficacy of Adoptive T-cell Therapy Is Improved by Treatment with the Antioxidant N-Acetyl Cysteine, Which Limits Activation-Induced T-cell Death.

Authors:  Matthew J Scheffel; Gina Scurti; Patricia Simms; Elizabeth Garrett-Mayer; Shikhar Mehrotra; Michael I Nishimura; Christina Voelkel-Johnson
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7.  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.

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8.  IL-15 activates mTOR and primes stress-activated gene expression leading to prolonged antitumor capacity of NK cells.

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9.  Lack of p53 Augments Antitumor Functions in Cytolytic T Cells.

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10.  Impact of glutathione peroxidase 4 on cell proliferation, angiogenesis and cytokine production in hepatocellular carcinoma.

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Journal:  Oncotarget       Date:  2018-01-22
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