Inflammatory cytokines IL-17 and TNF-α up-regulate PD-L1 expression in human prostate and colon cancer cells

Wang, Xun; Yang, Lu; Huang, Feng; Zhang, Qiuyang; Liu, Sen; Ma, Lin; You, Zongbing

doi:10.1016/j.imlet.2017.02.006

Cited by 259 publications

(207 citation statements)

References 40 publications

Supporting

Mentioning

198

Contrasting

Unclassified

Order By: Relevance

“…In addition, IL-17 upregulated PD-L1 protein expression in both cell lines. 20 Although still speculative, TNF>, IL-17, and other cytokines that are dysregulated in obesity constitute possible links with EC expression of PD-L1. A link between obesity and immune evasion by PD-L1-mediated suppression of cytotoxic CD8+ T cells is also of interest in cancers other than EC for which there is epidemiological association with obesity.…”

Section: G00001mentioning

confidence: 99%

Programmed Death Ligand 1 Expression Among 700 Consecutive Endometrial Cancers: Strong Association With Mismatch Repair Protein Deficiency

Joehlin‐Price

Rhoades

et al. 2018

Int J Gynecol Cancer

View full text Add to dashboard Cite

show abstract

Section: G00001mentioning

confidence: 99%

Programmed Death Ligand 1 Expression Among 700 Consecutive Endometrial Cancers: Strong Association With Mismatch Repair Protein Deficiency

Joehlin‐Price

Rhoades

et al. 2018

Int J Gynecol Cancer

View full text Add to dashboard Cite

show abstract

“…This postulate is based on the observations that PD-L1 expression in tumor cells is induced by IFN-γ (Cheng et al, 2007; Dondero et al, 2016; Iwai et al, 2002; Muhlbauer et al, 2006), and IFN-γ signaling is dependent on sphingolipid metabolism (Bajwa et al, 2017; Ottenlinger et al, 2016; Seo, Alexander, & Hahm, 2011; Wakita, Nishimura, Tokura, Furukawa, & Takigawa, 1996). Furthermore, Akt- (Abdelhamed, Ogura, Yokoyama, Saiki, & Hayakawa, 2016; Atefi et al, 2014; Dong et al, 2016; Lastwika et al, 2016; Song et al, 2013; Yang et al, 2017; Zhao et al, 2017), NF-kB- (Gowrishankar et al, 2015), and TNFα- (Wang et al, 2017) signaling induce PD-L1 expression, and all of these pathways are regulated by sphingolipid signaling. Therefore, manipulation of tumor immunology using SK inhibitors is an unexplored potential new approach to improved cancer therapy.…”

Section: Sphingosine Kinases As Targets For Anticancer Drugsmentioning

confidence: 99%

Targeting Sphingosine Kinases for the Treatment of Cancer

Lewis

Voelkel‐Johnson

Smith

2018

Advances in Cancer Research

View full text Add to dashboard Cite

Sphingosine kinases (SK1 and SK2) are key, druggable targets within the sphingolipid metabolism pathway that promote tumor growth and pathologic inflammation. A variety of isozyme-selective and dual inhibitors of SK1 and SK2 have been described in the literature, and at least one compound has reached clinical testing in cancer patients. In this chapter, we will review the rationale for targeting SKs and summarize the preclinical and emerging clinical data for ABC294640 as the first-in-class selective inhibitor of SK2.

show abstract

“…In general, testosterone is considered as an anti-inflammatory while estrogens are more proinflammatory, but several studies show shared effects on immune cells between hormones (indicated in red). References not cited in text: androgens on T helper cells (Sutherland et al 2005, Hepworth et al 2010, Fijak et al 2011, Andersson et al 2015, Wang et al 2017b) and on DCs (Koh et al 2009, Corrales et al 2012; estrogens on T helper cells (Correale et al 1998, Maret et al 2003, Lélu et al 2011, Morse & McNeel 2012, Chen et al 2015 and on DCs (Zhang et al 2004 linked to patient outcomes (Ylitalo et al 2016, Strömvall et al 2017, emphasizing the importance of understanding this biology. The receptor and non-receptor-mediated effects of steroids on innate immune cells have been widely studied in experimental animal models as well as in clinical studies of many diseases (Trigunaite et al 2015, Roved et al 2017.…”

Section: Sex Steroids and The Immune Tumor Microenvironment Effect Ofmentioning

confidence: 99%

Sex steroids in the tumor microenvironment and prostate cancer progression

Boibessot¹,

Toren²

2018

Endocrine-Related Cancer

View full text Add to dashboard Cite

Prostate cancer is uniquely dependent on androgens. Despite years of research on the relationship between androgens and prostate cancer, many questions remain as to the biological effects of androgens and other sex steroids during prostate cancer progression. This article reviews the clinical and basic research on the influence of sex steroids such as androgens, estrogens and progesterone within the prostate tumor microenvironment on the progression of prostate cancer. We review clinical studies to date evaluating serum sex steroids as prognostic biomarkers and discuss their respective biological effects within the prostate tumor microenvironment. We also review the link between genomic alterations and sex steroid levels within prostate tumors. Finally, we highlight the links between sex steroid levels and the function of the immune system within the tumor microenvironment. As the context of treatment of lethal prostate cancer evolves over time, an understanding of this underlying biology remains central to developing optimal treatment approaches.

show abstract

Inflammatory cytokines IL-17 and TNF-α up-regulate PD-L1 expression in human prostate and colon cancer cells

Cited by 259 publications

References 40 publications

Programmed Death Ligand 1 Expression Among 700 Consecutive Endometrial Cancers: Strong Association With Mismatch Repair Protein Deficiency

Programmed Death Ligand 1 Expression Among 700 Consecutive Endometrial Cancers: Strong Association With Mismatch Repair Protein Deficiency

Targeting Sphingosine Kinases for the Treatment of Cancer

Sex steroids in the tumor microenvironment and prostate cancer progression

Contact Info

Product

Resources

About