CD73 promotes colitis‑associated tumorigenesis in mice

Liu, Xuan-hui; Wu, Xianrui; Lan, Nan; Zheng, Xiaobin; Zhou, Chang; Hu, Tuo; Chen, Yu‑Feng; Cai, Zerong; Lan, Ping

doi:10.3892/ol.2020.11670

Cited by 9 publications

(11 citation statements)

References 49 publications

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“…These findings suggest that transplantation of CD73 + cells could lead to tumor formation. However, the promotion of colitis-associated tumorigenesis by CD73 reported by Liu et al was observed in a chronic inflammatory model generated following three cycles of treatment with azoxymethane, a genotoxic colonic carcinogen, and DSS administration for 3 weeks (Liu et al, 2020), which is different from the acute colitis model used in the present study. Moreover, transplanted MSCs disappear after temporary engraftment (Kean et al, 2013), but we will further investigate whether CD73 + cell spheroids remain at the injured site for a long time using longitudinal analysis, considering the potential clinical application of MSC transplantation.…”

Section: Secretory Factors Of Cd73 + Cell Spheroids Induce Alteration...contrasting

confidence: 70%

“…Inhibition of CD73 activity or gene silencing in tumor cells is reported to attenuate tumorigenesis (Jin et al , 2010; Stagg et al , 2010). Additionally, CD73 is highly expressed in solid tumors and is reported to facilitate colitis-associated tumorigenesis (Liu et al , 2020; Roh et al , 2020). These findings suggest that transplantation of CD73 + cells could lead to tumor formation.…”

Section: Discussionmentioning

confidence: 99%

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CD73-positive cell spheroid transplantation attenuates colonic atrophy

Hisamatsu

Itakura

Mabuchi

et al. 2022

Preprint

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The incidence of inflammatory bowel diseases (IBD) is increasing worldwide. Mesenchymal stem/stromal cells (MSCs) have immunomodulatory functions and are a promising source for cell transplantation therapy for IBD. However, owing to their heterogeneous nature, their therapeutic efficacy in colitis is controversial and depends on the delivery route and form of transplanted cells. Cluster of differentiation (CD)73 is widely expressed in MSCs and used to obtain a homogeneous MSC population. Herein, we determined the optimal method for MSC transplantation using CD73+ cells in a colitis model. mRNA sequencing analysis showed that CD73+ cells exhibit downregulation of inflammatory genes and upregulation of extracellular matrix-related genes. Furthermore, three-dimensional CD73+ cell spheroids showed enhanced engraftment at the injured site through the enteral route, facilitated extracellular matrix remodeling, and downregulated inflammatory gene expression in fibroblasts, leading to attenuation of colonic atrophy. Therefore, the interaction between intestinal fibroblasts and exogenous MSCs via tissue remodeling is one mechanism that can be exploited for colitis prevention. Our results highlight that transplantation of homogeneous cell populations with well-characterized properties is beneficial for IBD treatment.

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Section: Secretory Factors Of Cd73 + Cell Spheroids Induce Alteration...contrasting

confidence: 70%

Section: Discussionmentioning

confidence: 99%

CD73-positive cell spheroid transplantation attenuates colonic atrophy

Hisamatsu

Itakura

Mabuchi

et al. 2022

Preprint

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“…Considering elevated purinergic signaling levels in colon cancer samples, we strongly suppose that purinergic ecto-enzymes can be responsible for a similar antiinflammatory/immunosuppressive role in colorectal tumorigenesis (X.-H. Liu et al 2020). Given their immunosuppressive powers, it would not be surprising to see that these proteins are highly expressed in the colorectal tumor microenvironment (Liu et al 2012).…”

Section: Discussionmentioning

confidence: 99%

“…While some studies associate stromal CD73 expression with higher tumorigenic potential in colorectal cancer (Wu et In CRC studies with the cell lines, tumor cell specific CD73 expression was found to be essential for tumor growth in vitro and in vivo (Wu et al 2016). However, in a colitis associated cancer model, use of CD73 specific inhibitor reduced the tumor burden (Liu et al 2020). On the contrary, another report suggested that tumor cell specific CD73 expression is dispensable for colorectal tumor growth while stroma specific (mesenchymal cells) CD73 expression was essential for CD73-driven tumor growth (Yu et al 2020).…”

Section: Discussionmentioning

confidence: 99%

Characterization of Differential Expression Patterns of the Extracellular Purinergic Enzymes in Colorectal Cancer

Göktuna

2022

Trakya University Journal of Natural Sciences

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Objective: The aim of this study is to characterize tumor cell specific expression of purinergic ecto-enzymes CD39 and CD73 and to associate prognostic significance of these expression patterns in colorectal cancer (CRC) patients. Methods: Gene expression of the target genes in various CRC cell lines were assessed via WB and RT-PCR. Additionally, tumor vs stromal cell expression of the target genes was analyzed from publicly available patient expression datasets. Finally, the correlation between CD39 and CD73 expression with patient prognosis was analyzed via TCGA datasets. Results: In CRC cell lines CD39 found to be not expressed at all while CD73 was expressed extensively in most cell lines via WB and RT-CR analyses. Patient microarray expression data confirmed the results from CRC cells lines that CD39 expression was very low in epithelial/tumor cells relative to other stromal cell types yet CD73 was expressed abundantly in every cell type within patient tumor samples. Interestingly, CD39 expression in patient tumors was correlated with favorable prognosis while CD73 expression was associated with worse prognosis. Conclusion: Although CD39 and CD73 are related enzymes involved in extracellular purinergic signaling, their expression patterns in tumor cells and prognostic effects in patients show opposing outcomes. Therefore, better insights in understanding the functional involvement of purinergic ecto-enzymes in colorectal tumor development is needed via further mechanistical studies.

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“…In addition, concentrations of N-acetylaspartate produced by ovarian cancer cells were found to increase in parallel with cancer progression and correlated with, the polarization of macrophages towards the M2-like phenotype [156]. Non-specific stimulation of ARs by the agonist NECA upregulated the expression of NAT8L RNA in a colitis-associated tumorigenesis mouse model [157]. Because CD73 inhibitor conversely downregulated NAT8L expression, the observations were ascribed to AR modulation.…”

Section: Prospective Targets Of Adenosinergic Therapymentioning

confidence: 96%

Current Adenosinergic Therapies: What Do Cancer Cells Stand to Gain and Lose?

Kotulová

Hajdúch

Džubák

2021

IJMS

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A key objective in immuno-oncology is to reactivate the dormant immune system and increase tumour immunogenicity. Adenosine is an omnipresent purine that is formed in response to stress stimuli in order to restore physiological balance, mainly via anti-inflammatory, tissue-protective, and anti-nociceptive mechanisms. Adenosine overproduction occurs in all stages of tumorigenesis, from the initial inflammation/local tissue damage to the precancerous niche and the developed tumour, making the adenosinergic pathway an attractive but challenging therapeutic target. Many current efforts in immuno-oncology are focused on restoring immunosurveillance, largely by blocking adenosine-producing enzymes in the tumour microenvironment (TME) and adenosine receptors on immune cells either alone or combined with chemotherapy and/or immunotherapy. However, the effects of adenosinergic immunotherapy are not restricted to immune cells; other cells in the TME including cancer and stromal cells are also affected. Here we summarise recent advancements in the understanding of the tumour adenosinergic system and highlight the impact of current and prospective immunomodulatory therapies on other cell types within the TME, focusing on adenosine receptors in tumour cells. In addition, we evaluate the structure- and context-related limitations of targeting this pathway and highlight avenues that could possibly be exploited in future adenosinergic therapies.

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CD73 promotes colitis‑associated tumorigenesis in mice

Cited by 9 publications

References 49 publications

CD73-positive cell spheroid transplantation attenuates colonic atrophy

CD73-positive cell spheroid transplantation attenuates colonic atrophy

Characterization of Differential Expression Patterns of the Extracellular Purinergic Enzymes in Colorectal Cancer

Current Adenosinergic Therapies: What Do Cancer Cells Stand to Gain and Lose?

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